ALBERT

Description: Bone remodeling is a natural process that enables growth and maintenance of the skeleton. It involves the deposition of mineralized matrix by osteoblasts and resorption by osteoclasts. Several cancers that metastasize to bone negatively perturb the remodeling process through a series of interactions with osteoclasts, and osteoblasts. These interactions have been described as the “vicious cycle” of cancer metastasis in bone. Due to the inaccessibility of the skeletal tissue it is difficult to study this system in vivo . In contrast, standard tissue culture lacks sufficient complexity. We have developed a specialized three-dimensional culture system that permits growth of a non-vascularized, multiple-cell-layer of mineralized osteoblastic tissue from pre-osteoblasts. In this study, the essential properties of bone remodeling were created in vitro by co-culturing the mineralized collagenous osteoblastic tissue with actively resorbing osteoclasts followed by reinfusion with proliferating pre-osteoblasts. Cell-cell and cell-matrix interactions were determined by confocal microscopy as well as by assays for cell specific cytokines and growth factors. Osteoclasts, differentiated in the presence of osteoblasts, led to degradation of the collagen-rich extracellular matrix. Further addition of metastatic breast cancer cells to the co-culture mimicked the vicious cycle; i.e. there was a further reduction in osteoblastic tissue thickness, an increase in osteoclastogenesis, chemotaxis of cancer cells to osteoclasts and formation of cancer cells into large colonies. The resulting model system permits detailed study of fundamental osteobiological and osteopathological processes in a manner that will enhance development of therapeutic interventions to skeletal diseases. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: The reactions of As 2 O 3 , SbCl 3 , and (BiO) 2 CO 3 with oleum (65 % SO 3 ) yielded single crystals of As(S 2 O 7 )(HS 2 O 7 ) [monoclinic, P 2 1 / c , Z = 4, a = 16.549(1), b = 6.6743(5), c = 9.9498(6) Å, β = 102.672(8)°, V = 1072.672(8) Å 3 ], Sb 2 (SO 4 ) 2 (S 2 O 7 ) [monoclinic, P 2 1 / n , Z = 4, a = 9.1586(2), b = 6.9981(2), c = 17.7956(4) Å, β = 100.9690(8)°, V = 1119.73(5) Å 3 ], and Bi 2 (S 2 O 7 ) 3 [triclinic, P , Z = 2, a = 6.5734(1), b = 10.1954(2), c = 11.5121(2) Å, α = 90.996(1)°, β = 96.976(1)°, γ = 94.870(1)°, V = 762.75(2) Å 3 ]. As(S 2 O 7 )(HS 2 O 7 ) shows the arsenic atoms in a trigonal pyramidal coordination of the oxygen atoms of one chelating S 2 O 7 2– and one monodentate HS 2 O 7 – group. The distinct As(S 2 O 7 )(HS 2 O 7 ) molecules are connected with each other by hydrogen bonds to form layers. Sb 2 (SO 4 ) 2 (S 2 O 7 ) shows the Sb 3+ cations in a seesaw-type coordination of oxygen atoms from both anions. In Bi 2 (S 2 O 7 ) 3 the Bi 3+ cations are in a square prismatic oxygen coordination of disulfate units. The antimony and the bismuth compounds exhibit complex three-dimensionally linked structures. The syntheses and the crystal structures, as well as the thermal decomposition of Sb 2 (SO 4 ) 2 (S 2 O 7 ) are presented.

Description: Silver acetate AgOAc reacts with dry liquid ammonia under the formation of colorless needle-shaped crystals of diammine silver(I) acetate [Ag(NH 3 ) 2 ]OAc ( 1 ). The compound crystallizes in the monoclinic space group P 2 1 / c with a = 8.0205(2), b = 12.4161(3), c = 6.0938(2) Å, β = 107.741(4)°, and V = 577.98(3) Å 3 at 123 K with Z = 4. The crystal structure shows the presence of almost linear [Ag(NH 3 ) 2 ] + cations, which are arranged in a corrugated chain of equidistant silver atoms. The Ag–Ag distance is 3.1089(11) Å, which falls in the range of “argentophilic” interactions. After warming to room temperature and removal of the solvent, compound 1 was found unchanged as evidenced by powder X-ray diffraction, thermogravimetric and mass-spectrometric analysis, as well as IR and Raman spectroscopy.

Description: A series of chalcogenidoantimonates, namely [Zn(NH 3 ) 6 ](Sb III 4 S 7 ) ( 1 ), [Zn(NH 3 ) 6 ]{Zn(NH 3 ) 3 Sb V S 4 } 2 · NH 3 ( 2 ), [Mn(NH 3 ) 6 ](Sb III Se 2 ) 2 ( 3 ) and [Zn(NH 3 ) 4 ]{Zn(NH 3 )Sb III Se 3 } 2 · 3NH 3 ( 4 ) are synthesized by solvothermal technique in liquid ammonia at 50 °C from elemental zinc or manganese, antimony and sulfur or selenium. 1 (space group P ) and 2 ( P ) crystallize centrosymmetrically, whereas 3 ( Pna 2 1 ) and 4 ( P 2 1 ) represent polar structures. All compounds contain discrete cationic [Zn(NH 3 ) 4 ] 2+ , [Zn(NH 3 ) 6 ] 2+ , and [Mn(NH 3 ) 6 ] 2+ ammine complexes. In the anionic structure parts, corner-connected trigonal-pyramidal SbS 3 and SbSe 3 are the characteristic building units. 1 and 4 contain 2D polymeric anions, in the latter case with Zn 2+ cations incorporated in a selenidoantimonate(III) network. The polymeric anion in the structure of 3 is a helical chain. 2 is a molecular compound and contains dinuclear anions [S 3 Sb–S–Zn(NH 3 ) 3 ] 2– with Sb V . Raman measurements show the Sb–Ch valence vibrations in the expected region between 250–370 cm –1 for 1 and at 212 cm –1 for 4 . According to the reflectance spectrum 4 is a semiconductor with an optical band gap of 2.05(5) eV.

Description: Cervical carcinoma represents the paradigm of virus-induced cancers, where virtually all cervical cancers come from previous “high-risk” HPV infection. The persistent expression of the HPV viral oncoproteins E6 and E7 is responsible for the reprogramming of fundamental cellular functions in the host cell, thus generating a noticeable, yet only partially explored, imbalance in protein molecular networks and cell signaling pathways. Eighty-eight cellular factors, identified as HPV direct or surrogate targets, were chosen and monitored in a retrospective analysis for their mRNA expression in HPV-induced cervical lesions, from dysplasia to cancer. Real-time quantitative PCR (qPCR) was performed by using formalin-fixed, paraffin embedded archival samples. Gene expression analysis identified 40 genes significantly modulated in LSIL, HSIL and squamous cervical carcinoma. Interestingly, among these, the expression level of a panel of four genes, TOP2A, CTNNB1, PFKM and GSN, was able to distinguish between normal tissues and cervical carcinomas. Immunohistochemistry was also done to assess protein expression of two genes among those up-regulated during the transition between dysplasia and carcinoma, namely E2F1 and CDC25A, and their correlation with clinical parameters. Besides the possibility of significantly enhancing the use of some of these factors in diagnostic or prognostic procedures, these data clearly outline specific pathways, and thus key biological processes, altered in cervical dysplasia and carcinoma. Deeper insight on how these molecular mechanisms work may help widen the spectrum of novel innovative approaches to these virus-induced cell pathologies. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: Cellular pathways are numerous and are highly integrated in function in the control of cellular systems. They collectively regulate cell division, proliferation, survival and apoptosis of cells and mutagenesis of key genes that control these pathways can initiate neoplastic transformations. Understanding these pathways is crucial to future therapeutic and preventive strategies of the disease. Ovarian cancers are of three major types; epithelial, germ-cell and stromal. However, ovarian cancers of epithelial origin, arising from the mesothelium, are the predominant form. Of the subtypes of ovarian cancer, the high-grade serous tumors are fatal, with low survival rate due to late detection and poor response to treatments. Close examination of preserved ovarian tissues and in vitro studies have provided insights into the mechanistic changes occurring in cells mediated by a few key genes. This review will focus on pathways and key genes of the pathways that are mutated or have aberrant functions in the pathology of ovarian cancer. Non-genetic mechanisms that are gaining prominence in the pathology of ovarian cancer, miRNAs and epigenetics, will also be discussed in the review. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: Normal pregnancy is associated with systemic vasodilation and decreased vascular contraction, partly due to increased release of endothelium-derived vasodilator substances. Endothelin-1 (ET-1) is an endothelium-derived vasoconstrictor acting via endothelin receptor type A (ET A R) and possibly type B (ET B R) in vascular smooth muscle cells (VSMCs), with additional vasodilator effects via endothelial ET B R. However, the role of ET-1 receptor subtypes in the regulation of vascular function during pregnancy is unclear. We investigated whether the decreased vascular contraction during pregnancy reflects changes in the expression/activity of ET A R and ET B R. Contraction was measured in single aortic VSMCs isolated from virgin, mid-pregnant (mid-Preg, day 12) and late-Preg (day 19) Sprague-Dawley rats, and the mRNA expression, protein amount, tissue and cellular distribution of ET A R and ET B R were examined using RT-PCR, Western blots, immunohistochemistry and immunofluorescence. Phenylephrine (Phe, 10 −5  M), KCl (51 mM) and ET-1 (10 −6  M) caused VSMC contraction that was in late-Preg 〈 mid-Preg and virgin rats. In VSMCs treated with ET B R antagonist BQ788, ET-1 caused significant contraction that was still in late-Preg 〈 mid-Preg and virgin rats. In VSMCs treated with the ET A R antagonist BQ123, ET-1 caused a small contraction; and the ET B R agonists IRL-1620 and sarafotoxin 6c (S6c) caused similar contraction that was in late-Preg 〈 mid-Preg and virgin rats. RT-PCR revealed similar ET A R, but greater ET B R mRNA expression in pregnant vs. virgin rats. Western blots revealed similar ET A R, and greater protein amount of ET B R in endothelium-intact vessels, but reduced ET B R in endothelium-denuded vessels of pregnant vs. virgin rats. Immunohistochemistry revealed prominent ET B R staining in the intima, but reduced ET A R and ET B R in the aortic media of pregnant rats. Immunofluorescence signal for ET A R and ET B R was less in VSMCs of pregnant vs. virgin rats. The pregnancy-associated decrease in ET A R- and ET B R-mediated VSMC contraction appears to involve downregulation of ET A R and ET B R expression/activity in VSM, and may play a role in the adaptive vasodilation during pregnancy. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: Neuroregenerative medicine is an ever-growing field in which regeneration of lost cells/tissues due to a neurodegenerative disease is the ultimate goal. With the scarcity of available replacement alternatives, stem cells provide an attractive source for regenerating neural tissue. While many stem cell sources exist, including: mesenchymal stem cells (MSCs), embryonic stem cells (ESCs), and induced pluripotent stem cells (iPSCs), the limited cellular potency, technical difficulties, and ethical considerations associated with these make finding alternate sources a desirable goal. Periodontal ligament stem cells (PDLSCs) derived from the neural crest were induced into neural-like cells using a combination of epidermal growth factor (EGF) and basic fibroblast growth factor (bFGF). Morphological changes were evident in our treated group, seen under both light microscopy and scanning electron microscopy (SEM). A statistically significant increase in the expression of neuron-specific β-tubulin III and the neural stem/progenitor cell marker nestin, along with positive immunohistochemical staining for glial fibrillary acidic protein (GFAP), demonstrated the success of our treatment in inducing both neuronal and glial phenotypes. Positive staining for synaptophysin demonstrated neural connections and electrophysiological recordings indicated that when subjected to whole cell patch clamping, our treated cells displayed inward currents conducted through voltage-gated sodium (Na + ) channels. Taken together, our results indicate the success of our treatment in inducing PDLSCs to neural-like cells. The ease of sourcing and expansion, their embryologic neural crest origin, and the lack of ethical implications in their use make PDLSCs an attractive source for use in neuroregenerative medicine. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: Urotensin II (UII), a vasoactive peptide modulates renal hemodynamics. However, the physiological functions of UII in glomerular cells are unclear. In particular, whether UII alters mesangial tone remains largely unknown. The present study investigates the physiological effects of UII on intracellular Ca 2+ ([Ca 2+ ] i ) and contraction in glomerular mesangial cells (GMCs). This study also tested the hypothesis that the regulator of G-protein signaling (RGS) controls UII receptor (UTR) activity in GMCs. RT-PCR, Western immunoblotting, and immunofluorescence revealed UTR expression and localization in cultured murine GMCs. Mouse UII (mUII) stimulated [Ca 2+ ] i elevation in GMCs in the absence and presence of extracellular Ca 2+ . mUII also caused a reduction in planar GMC surface area. mUII-induced [Ca 2+ ] i elevation and contraction in GMCs were attenuated by SB 657510, a UTR antagonist, araguspongin B, an inositol 1,4,5-trisphosphate receptor antagonist, thapsigargin, a sarco/endoplasmic reticulum Ca 2+ -ATPase inhibitor, and La 3+ , a store-operated Ca 2+ channel blocker, but not nimodipine, an L-type Ca 2+ channel blocker. In situ proximity ligation assay indicated molecular proximity between endogenous RGS2 and UTR in the cells. Treatment of GMCs with mUII increased plasma membrane association of RGS2 by ∼ 2-fold. mUII also increased the interaction between RGS2 and UTR in the cells. siRNA-mediated knockdown of RGS2 in murine GMCs increased mUII-induced [Ca 2+ ] i elevation and contraction by ∼ 35 and 31%, respectively. These findings indicate that mUII induces [Ca 2+ ] i elevation and contraction in murine GMCs. Data also suggest that UTR activation stimulates RGS2 recruitment to GMC plasma membrane as a negative feedback mechanism to regulate UTR signaling. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: Poly-N-acetyllactosamine (PLN) is a unique glycan composed of repeating units of the common disaccharide (Galβ1,4-GlcNAcβ1,3) n . The expression of PLN on glycoprotein core structures minimally requires enzyme activities for β1,4-galactosyltransferase (β4GalT) and β1,3-N-acetylglucosminyltransferase (β3GnT). Because β4GalTs are ubiquitous in most cells, PLN expression is generally ascribed to the tissue-specific transcription of 8 known β3GnT genes in mice. In the olfactory epithelium (OE), β3GnT2 regulates expression of extended PLN chains that are essential for axon guidance and neuronal survival. N-glycan branching and core composition, however, can also modulate the extent of PLN modification. Here we show for the first time that the β1,6-branching glycosyltransferase GCNT2 (formerly known as IGnT) is expressed at high levels specifically in the OE and other sensory ganglia. Postnatally, GCNT2 is maintained in mature olfactory neurons that coexpress β3GnT2 and PLN. This highly specific coexpression suggests that GCNT2 and β3GnT2 function cooperatively in PLN synthesis. In support of this, β3GnT2 and GCNT2 cotransfection in HEK293T cells results in high levels of PLN expression on the cell surface and on adenylyl cyclase 3, a major carrier of PLN glycans in the OE. These data clearly suggest that GCNT2 functions in vivo together with β3GnT2 to determine PLN levels in olfactory neurons by regulating β1,6-branches that promote PLN extension. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: . Sr 2 CoOsO 6 , a new osmium based ordered semiconductor double perovskite was prepared by solid state synthesis from the respective binary oxides. Room temperature PXRD analysis shows the compound to be tetragonal [ I 4/ m ; a = 5.5503(1) Å and c = 7.9320(1) Å], whereas low temperature synchrotron data refinement has revealed a second monoclinic polymorph [ I 2/ m ; a = 5.4969(2) Å, b = 5.4979(2) Å, c = 8.0090(1) Å and γ = 90.527(1)°] with a fully ordered rocksalt arrangement of cobalt and osmium atoms over the perovskite B -sites. Heat capacity and magnetic measurements indicate that Sr 2 CoOsO 6 shows antiferromagnetic ordering below T N = 108 K followed by a second magnetic transition at T 2 = 65 K. It was shown that the change from the tetragonal to the monoclinic phase occurs at T N .

Description: . The ternary germanides RE Rh 6 Ge 4 ( RE = Y, La, Pr, Nd, Sm–Lu) were obtained by arc-melting of the elements and subsequent annealing. Single crystals were grown from bismuth fluxes. The samples were studied by X-ray diffraction on powders. The structures of five members were refined from single crystal diffraction data: LiCo 6 P 4 type, P m 2, a = 715.8(1), c = 387.33(8) pm, wR = 0.0238, 332 F 2 values for LaRh 6 Ge 4 , a = 715.0(1), c = 384.96(7) pm, wR = 0.0211, 329 F 2 values for PrRh 6 Ge 4 , a = 714.28(9), c = 382.57(6) pm, wR = 0.0136, 327 F 2 values for SmRh 6 Ge 4 , a = 714.2(1), c = 381.6(1), wR = 0.0270, 327 F 2 values for GdRh 6 Ge 4 , and a = 714.2(2), c = 379.0(1) pm, wR = 0.0273, 324 F 2 values for HoRh 6 Ge 4 with 19 variables per refinement. The RE Rh 6 Ge 4 structures have two crystallographically independent germanium sites in trigonal prismatic coordination, manifesting the close structural relationship with metal-rich phosphides. Together, the rhodium and germanium atoms build up three-dimensional [Rh 6 Ge 4 ] networks, which leave large channels for the rare earth atoms. Each rare earth atom has coordination number 20 with 12 Rh, 6 Ge, and 2 RE neighbors. Temperature dependent magnetic susceptibility measurements indicate Pauli paramagnetic behavior for YRh 6 Ge 4 , LaRh 6 Ge 4 , and LuRh 6 Ge 4 . The compounds RE Rh 6 Ge 4 ( RE = Gd–Yb) are Curie-Weiss paramagnets. Antiferromagnetic ordering was observed at 8.4(5) K (GdRh 6 Ge 4 ), 13.6(5) K (TbRh 6 Ge 4 ), 5.1(5) K (DyRh 6 Ge 4 ), and 8.9(5) K (YbRh 6 Ge 4 ). DyRh 6 Ge 4 and YbRh 6 Ge 4 show metamagnetic transitions at 2.5(5) and 45(2) kOe, respectively.

Description: Reaction of manganese(II) thiocyanate with 2-chloropyrazine leads always to the formation of a compound of composition Mn(NCS) 2 (2-chloropyrazine) 4 ( 1 - Mn/Cl ) that consists of discrete complexes, in which the manganese cation is coordinated by two terminal thiocyanato anions and four 2-chloropyrazine ligands. In contrast, with 2-methylpyrazine only an aqua complex of composition Mn(NCS) 2 (2-methylpyrazine) 2 (H 2 O) 2 ( 1 - Mn/CH 3 ) is obtained that also consists of discrete octahedrally coordinated complexes. Moreover, a few single crystals of Mn(NCS) 2 (2-chloropyrazine) 4 · Mn(NCS) 2 (2-chloropyrazine) 2 (H 2 O) 2 · 2-chloropyrazine trisolvate ( 2 - Mn/Cl ) and Mn(NCS) 2 (2-methylpyrazine) 2 (H 2 O) 2 · Mn(NCS) 2 (H 2 O) 4 ( 2 - Mn/CH 3 ) were accidently obtained but no larger amounts are available. On heating, 1 - Mn/Cl and 1 - Mn/CH 3 transforms into new compounds of composition Mn(NCS) 2 (L) 2 (L = 2-chloropyrazine) ( 4 - Mn/Cl ) and 2-methylpyrazine ( 3 - Mn/CH 3 ). Surprisingly on further heating 1 - Mn/CH 3 looses additional 2-methylpyrazine ligands and transforms into a new compound of composition Mn(NCS) 2 (2-methylpyrazine) ( 4 - Mn/CH 3 ). Compound 4 - Mn/Cl is isotypic to its cobalt(II) analog and 4 - Mn/CH 3 is isotypic to Cd(NCS) 2 (2-methylpyrazine) reported recently and therefore, both structures were refined by the Rietveld method. The crystal structures of both compounds are strongly related. They consists of dimeric units, in which each two manganese cations are linked by pairs of μ-1,3-bridging thiocyanato anions, which are further connected into layers by single μ-1, 3-bridging anionic ligands. In contrast to 4 - Mn/Cl , in 4 - Mn/CH 3 these layers are further linked into a 3D coordination network by the 2-methylpyrazine ligands. Magnetic measurements reveal that 1 - Mn/Cl , 1 - Mn/CH 3 , and 3 - Mn/CH 3 shows only Curie- or Curie-Weiss paramagnetism, whereas 4 - Mn/Cl and 4 - Mn/CH 3 shows antiferromagnetic ordering at T N = 22.9 K and at 26.5 K. The results of these investigations are compared with those obtained for related compounds.

Description: . Black platelets of Bi 39.67(7) Ru 2 Br 35.0(2) were crystallized from a melt of Bi, BiBr 3 , and Ru. In the tetragonal crystal structure [ P 4/ mbm , a = 1311.92(6) pm, c = 3018.2(4) pm at 155(5) K], cluster cations [(Bi 8 2+ )Ru 2+ (Bi 8 2+ )] are embedded in a matrix of disordered bromido-bismuthate(III) groups. A thorough analysis of the disorder in the anionic part enabled the unambiguous assignment of the cluster charge. The η 4 -coordination of the two Bi 8 2+ square antiprisms to the Ru II atom in the sandwich complex resembles the bonding of Bi 5 + and Bi 8 2+ in the clusters [(Bi 5 + )Ru + (Bi 4 Br 4 )Ru + (Bi 5 + )] and [(Bi 8 2+ )Ru + (Bi 4 Br 4 )Ru + (Bi 5 + )] as well as of Bi 4 2– in 1 ∞ [(Bi 4 2– )Ru + (Bi 4 Br 4 )Ru + ]. By combining crystal chemical considerations for all mentioned compounds and using quantum chemical calculations, a common bonding scheme for the coordination compounds of bismuth polycations and polyanions was established. The η 4 -coordinating bismuth polycations and polyanions act as six electron donors, comparable to nido -carborane ligands, Zintl anions E 9 4– and E 5 6– ( E = Si to Pb), cyclopentadienyl ligands, or the cyclobutadiene dianion. The electron count for the transition metal is 18 in all finite clusters.

Description: Spermatogenesis is a special process by which spermatogonial stem cells (SSCs) divide and differentiate to male gametes called mature spermatozoa. SSCs are the unique cells because they are adult stem cells that transmit genetic information to subsequent generations. Accumulating evidence has demonstrated that SSCs can be reprogrammed to acquire pluripotency to become embryonic stem-like cells that differentiate into all cell lineages of the three germ layers, highlighting potential important applications of SSCs for regenerative medicine. Recent studies from peers and us have made great achievements on the characterization, isolation and culture of mouse and human SSCs, which could lead to better understanding the biology of SSCs and the applications of SSCs in both reproductive and regenerative medicine. In this review, we first compared the cell identity and biochemical phenotypes between mouse SSCs and human SSCs. Notably, the cell types of mouse and human SSCs are distinct, and human SSCs share some but not all phenotypes with mouse SSCs. The approaches for isolating SSCs as well as short- and long- term culture of mouse SSCs and short-period culture of human SSCs were also discussed. We further addressed the new advances on the self-renewal of SSCs with an aim to establish the long-term culture of human SSCs which has not yet been achieved. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: . Previous attempts to synthesize and isolate (thiobisphenolate) vanadium(V) dioxido complexes had always provided their dimers containing [O=V(μ-O) 2 V=O] 2+ cores, and these also dominate the solution reactivity. Hence, the behavior of their parent monomers, which represent the major species in solution, has remained uncertain. Herein we report the development of a synthetic route that allowed for the successful isolation, spectroscopic investigation, and structural characterization of the monomer PPh 4 [ S LVO 2 ] ( 3 ) [ S L 2– = 2′2-thiobis(2, 4-di- tert -butylphenolate)]. For this purpose PPh 4 [ S LVOCl 2 ] ( 1 ) had to be accessed first in order to convert it to the ethoxido compound PPh 4 [ S LVO(OEt) 2 ] ( 2 ), which is more prone to hydrolysis. Treatment of 2 with stoichiometric amounts of water followed by immediate cooling to –30 °C led to crystals of 3 . After its dissolution NMR spectra were recorded that were identical with those obtained after dissolution of its dimer, thus confirming the monomer/dimer equilibrium postulated previously. The molecular structure of 3 revealed the absence of a V ··· S interaction, which, however, stabilizes its dimer, and thus suggested the employment of a bisphenolate ligand lacking a bridging sulfur atom to obtain an analogue, which does not undergo dimerization in solution. In Et L 2– the sulfur atom is replaced by an ethylmethine unit and indeed the corresponding complex NBu 4 [ Et LVO 2 ] ( 4 ) proved to be stable as a monomer. Investigation of its potential as a catalyst for the oxidative dehydrogenation of 9-fluorenol confirmed a much lower reactivity in comparison to dimeric complexes, which is discussed.

Description: Two complexes, cis -[MnL 2 (NCS) 2 ] ( 1 ) and cis -[ZnL 2 (NCS) 2 ] ( 2 ) with asymmetrical substituted triazole ligands [L = 3, 4-dimethyl-5-(2-pyridyl)-1, 2, 4-triazole], were synthesized and characterized by elemental analysis, UV/Vis and FT-IR spectroscopy as well as thermogravimetric analyses (TGA), powder XRD, and single-crystal X-ray diffraction. In the complexes, each L molecule adopts a chelating bidentate mode by the nitrogen atoms of pyridyl and triazole. Both complexes have a similar distorted octahedral [ M N 6 ] core ( M = Mn 2+ and Zn 2+ ) with two NCS – ions in the cis position.

Description: . The multi-shaped amorphous alloy (Ni-B) powders were prepared by complexing reduction route using sodium borohydride (NaBH 4 ) as reductant with assistance of ultrasonic wave. The selected complexants, i.e. water, ammonia, salicylic acid, and ethylene diamine tetraacetic acid (EDTA) possess sequentially escalating complexation ability. The chemical composition and shapes of the product samples obtained under different conditions were characterized by X-ray powder differaction, selected area electron diffraction, and transmission electron microscope. The influence of reaction conditions such as the types of Ni-B, temperatures, NaBH 4 concentrations, and sodium hydroxide (NaOH) content on the hydrogen generation rate of hydrolysis of NaBH 4 solution were investigated in detail. The results show that the as-prepared Ni-B powders all belong to amorphous alloy with variable element contents, and the Ni-B sample prepared from EDTA complexation, possessing the best fineness and dispersity, has the strongest catalytic activity. The mean apparent activation energy of the hydrolysis reaction is 64.90 kJ · mol –1 . The NaBH 4 concentration has little impact on hydrogen generation rate, implying that the catalytic hydrolysis of NaBH 4 solution should be the pseudo zero-order reaction. Keeping the NaOH content at below 5 % could inhibit the hydrolysis of NaBH 4 solution, but the NaOH contents from 10 % to 15 % will significantly promote the hydrolysis rate of NaBH 4 . The hydrolysis reaction mechanisms, especially the effect of NaOH content on the hydrolysis reaction were also analyzed.

Description: Angiogenin (ANG) undergoes nuclear translocation and promotes ribosomal RNA (rRNA) transcription thereby enhancing cell growth and proliferation. However, the mode of action of ANG in stimulating rRNA transcription is unclear. Here, we show that ANG enhances the formation of RNA polymerase I (Pol I) pre-initiation complex at the ribosomal DNA (rDNA) promoter. ANG binds at the upstream control element (UCE) of the promoter and enhances promoter occupancy of RNA Pol I as well as the selectivity factor SL1 components TAF I 48 and TAF I 110. We also show that ANG increases the number of actively transcribing rDNA by epigenetic activation through promoter methylation and histone modification. ANG binds to histone H3, inhibits H3K9 methylation, and activates H3K4 methylation as well as H4 acetylation at the rDNA promoter. These data suggest that one of the mechanisms by which ANG stimulates rRNA transcription is through an epigenetic activation of rDNA promoter. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: The intermetallic compounds Sr 2 Au 6.52 Zn 2.48 , Sr 2 Au 6 Zn 3 , and Sr 2 Au 6 Ga 3 were obtained by induction melting of the elements in sealed tantalum tubes. Their structures were studied by X-ray diffraction on powders and refined from single crystal diffraction data: R c , a = 844.5(2), c = 2187.7(5) pm, wR 2 = 0.0411, 936 F 2 values and 20 variables for Sr 2 Au 6.52 Zn 2.48 ; a = 841.6(2), c = 2191.5(7) pm, wR 2 = 0.0126, 587 F 2 values and 19 variables for Sr 2 Au 6 Zn 3 ; and a = 841.9(2), c = 2191.1(7) pm, wR 2 = 0.0199, 660 F 2 values and 19 variables for Sr 2 Au 6 Ga 3 . The gold substructures of Sr 2 Au 6 Zn 3 and Sr 2 Au 6 Ga 3 can be considered as diamond polytypes with 6R stacking sequences (287–304 pm Au–Au in Sr 2 Au 6 Zn 3 ). The cavities formed by this network are filled in an ordered manner by strontium atoms and Zn 3 (281 pm Zn–Zn), respectively Ga 3 (286 pm Ga–Ga) triangles in a 2:1 ratio. Consequently one can describe the Sr 2 Au 6 Zn 3 and Sr 2 Au 6 Ga 3 structures as ordered substitution variants of the Zintl phase CaIn 2 . This structural relationship is discussed on the basis of a group-subgroup Scheme. Sr 2 Au 6.52 Zn 2.48 shows Zn/Au mixing on the triangle.

Description: The templated borate, [C 9 H 14 N] · [B 5 O 6 (OH) 4 ], was synthesized under hydrothermal conditions. Single crystal X-ray diffraction techonology reveals that it crystallizes in the triclinic system, space group P (No. 2). The material was also characterized by element analysis, Fourier transform infrared spectroscopy (FTIR), powder X-ray diffraction (PXRD), thermogravimetric and differential thermal analysis (TG-DTA), and luminescence spectroscopy. The compound consisted of isolated pentaborate [B 5 O 6 (OH) 4 ] – and N -butylpyridinium cations [C 9 H 14 N] + . The [B 5 O 6 (OH) 4 ] – anions are connected together by hydrogen bonds to form a three-dimensional framework, in which [C 9 H 14 N] + cations are located in. [C 9 H 14 N] · [B 5 O 6 (OH) 4 ] exhibits tunable luminescence emission at 415–458 nm by means of heating treatment from 100 to 300 °C.

Description: Two alkylimido derivatives of hexamolybdate, (Bu 4 N) 2 [Mo 6 O 18 (≡N- o -COOCH 3 C 6 H 4 )] ( 1 ) and (Bu 4 N) 2 [Mo 6 O 18 (≡N- o -COOCH 2 CH 3 C 6 H 4 )] ( 2 ), were synthesized in high purity and good yields by the reaction of [(C 4 H 9 ) 4 N] 4 [α-Mo 8 O 26 ] and methyl anthranilate or ethyl- o -aminobenzoate hydrochloride with N , N ′-dicyclohexylcarbodiimide (DCC) as a dehydrating agent in dry acetonitrile solution, which were characterized by elemental analyses, IR, UV/Vis, and 1 H NMR spectroscopy as well as ESI-MS, and single-crystal X-ray diffraction study. Compound 1 crystallizes in the monoclinic space group P 2 1 / n with one-dimensional chain structure via intramolecular hydrogen bond. Compound 2 also crystallizes in the monoclinic space group P 2 1 / n with dimer structure by intramolecular hydrogen bonds and π–π interactions between the pairs of cluster anions.

Description: The cover picture shows the frontispieces of all articles published in this Special Issue with research reports from DFG priority program 1178 “Experimental Electron Density as Key to Understanding Chemical Interactions”, highlighting the diverse range of chemistry that is covered herein. Biological processes that determine the effects of drugs consist on a certain interaction between agent and receptor. This molecular recognition is influenced by the electron density distribution. Analysis of these processes enables the rational synthesis of drugs. Electron density measurements are moreover significant for the design of advanced materials with specific features, e.g. the development of new pigments. Thus, color, stability, and durability can be tuned by modifying the electron density. Selected substance classes used in chemical synthesis, drug design and material science were analyzed and their binding and recognition processes were studied and quantified by means of electron density measurements.

Description: . Reactions of the coordinatively unsaturated complexes [Fe 2 (μ-P R 2 )(μ-P R ′ 2 )(CO) 5 ] [ R = R ′ = t Bu ( 1 ); R = t Bu, R ′ = Cy ( 2 )] with nitric oxide in toluene at elevated temperatures were investigated. Thus, the new complexes [Fe 2 (μ-P t Bu 2 ) 2 (NO) 4 ] ( 3 ) and [Fe 2 (μ-P t Bu 2 )(μ-PCy 2 )(NO) 4 ] ( 4 ) were obtained in good yields. The molecular structure of 3 was confirmed by X-ray diffraction study. Compound 4 was also prepared from the coordinatively saturated species [Fe 2 (μ-P t Bu 2 )(μ-PCy 2 )(CO) 6 ] ( 2a ) with nitric oxide in refluxing toluene. Further closely related reactions at 60 °C with the complex 1 and [FeRu(μ-P t Bu 2 ) 2 (CO) 5 ] ( 5 ), respectively, were investigated using preliminary crystal structure determination results.

Description: Two new materials of the composition ({CH 3 (CH 2 ) 15 (CH 3 ) 2 S} + ) 2 [CoBr 4 ] 2– ( 1 ) and ({CH 3 (CH 2 ) 15 (CH 3 ) 2 S} + ) 2 [CuBr 4 ] 2– ( 2 and 3 ), of which the latter exists in two polymorphs, were synthesized. The materials display the synthetically targeted structures, comprising of layers of complex metal ions and layers of long-chain sulfonium cations. The crystal structures of the materials were determined. The interlayer distances are around 24 Å, with metal–metal distances about 8 Å. The magnetic properties of 1 were investigated, and the material is paramagnetic. ({CH 3 (CH 2 ) 15 (CH 3 ) 2 S} + ) 2 [CuBr 4 ] 2 is polymorphic. Both polymorphs crystallize with triclinic symmetry.

Description: Constitutive androstane receptor (CAR) was originally identified as xenobiotic sensor that regulates the expression of cytochrome P450 genes. However, recent studies suggest that this nuclear receptor is also involved in the regulation of energy metabolism including glucose and lipid homeostasis. This study investigated the role of CAR in the regulation of bone mass in vivo using CAR -/- mice. Endogenous mRNA expression of CAR was observed in both primary osteoblasts and osteoclast precursors. CAR -/- mice have exhibited significant increase in whole body bone mineral density (BMD) by 9.5% ( p  〈 0.01) and 5.5% (p 〈 0.05) at 10 and 15 weeks of age, respectively, compared with WT mice in males. Microcomputed tomography analysis of proximal tibia demonstrated a significant increase in trabecular bone volume (62.7%), trabecular number (54.1%) in male CAR -/- mice compared with WT mice. However, primary culture of calvarial cells exhibited no significant changes in osteogenic differentiation potential between CAR -/- and WT. In addition, the number of tartrate-resistant acid-phosphatase positive osteoclasts in the femur and serum level of CTx was not different between CAR -/- and WT mice. The higher BMD and microstructural parameters were not observed in female mice. Interestingly, serum level of testosterone in male CAR -/- mice was 2.5-fold higher compared with WT mice and the mRNA expressions of Cyp2b9 and 2b10 in the liver, which regulate testosterone metabolism, were significantly down-regulated in male CAR -/- mice. Furthermore, the difference in BMD between CAR -/- and WT mice disappeared at 8 weeks after performing orchiectomy. CAR -/- mice also exhibited significant increase in serum1,25(OH) 2 D 3 levels but Cyp 27B1 which converts 25(OH)D 3 to 1,25(OH) 2 D 3 was significantly down-regulated compared to WT mice. These results suggest that in vivo deletion of CAR resulted in higher bone mass, which appears to be a result from reduced metabolism of testosterone due to down-regulation of Cyp2b. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: Single crystals of Rb 2 H 2 P 2 O 6 · 2H 2 O could be obtained from aqueous solutions of hypodiphosphoric acid and rubidium carbonate. Its crystal structure was determined by X-ray diffraction and it crystallizes in the monoclinic space group P 2 1 / c with Z = 4. The salt-like title compound consists of [H 2 P 2 O 6 ] 2– units in staggered P 2 O 6 -skeleton conformation, Rb + cations, and H 2 O molecules, held together by intermolecular hydrogen bonds of the type O ··· O. The vibrational spectra (IR/FIR and Raman) of the rubidium salt were recorded and an assignment of the vibrational modes is proposed based on the point group C 2 h for the P 2 O 6 -skeleton of the anion. The thermal behavior of Rb 2 H 2 P 2 O 6 · 2H 2 O is dominated by a complex TG decay indicating a simultaneous H 2 O delivery coupled with a disproportionation of [H 2 P 2 O 6 ] 2– , what is also supported by Raman spectra of heated samples.

Description: Three metal coordination polymers {[Co(L) 2 (H 2 O) 2 ] 2+ · 2NO 3 – } n ( 1 ), {[Mn(L) 2 (H 2 O) 2 ] 2+ · 2Cl – · 3H 2 O} n ( 2 ), and [ZnL(ba) 2 ] n ( 3 ) [L = 3, 5-bis(imidazole-1-yl)pyridine and Hba = benzoic acid] were synthesized and structurally characterized by IR spectroscopy, elemental analysis, X-ray powder diffraction, and X-ray single crystal diffraction. Complex 1 shows a one-dimensional (1D) chain structure. Adjacent chains are connected by hydrogen bonding and nitrate groups to form a 3D network. Complex 2 features a 2D layer structure. A three-dimensional network is constructed through the cluster consisting of two chloride ions and three water molecules. Complex 3 shows a 1D zigzag chain structure that further twists together to form a 3D network. The X-ray powder diffraction patterns were compared with the simulated ones. Moreover, the luminescent properties of 1 – 3 were investigated in the solid state at room temperature, and the thermogravimetric analyses were carried out to study the thermal stability of the three complexes.

Description: . The reactions of FeCl 3 · 6H 2 O and 2-(2′-hydroxyphenyl)-2-thiazoline as a bidentate O-N donor thiazoline ligand (thoz) afford a five-coordinate Fe III complex [Fe(thoz) 2 Cl] with a distorted square pyramidal configuration. Complex [Fe(thoz) 2 Cl] was isolated as air-stable crystalline solids and fully characterized, including by single-crystal X-ray structure analysis. Complex [Fe(thoz) 2 Cl] shows very efficient reactivity in the oxidation of sulfides to their corresponding sulfoxides using urea hydrogen peroxide (UHP) as the oxidant at room temperature in air.

Description: Two copper(I) complexes of compositions [Cu(HL)I] 2 · EtOH ( 1 ) and [Cu(HL) 3 ]I · MeOH ( 2 ) were synthesized via the reactions of HL [HL = 2(4, 5-diphenyl-1 H -imidazol-2-yl)pyridine] and CuI in EtOH and MeOH, respectively, under solvothermal conditions. The complexes were characterized by X-ray single crystal diffraction, IR spectroscopy, and elemental analysis. Compounds 1 and 2 are catalytically active towards ketalization reaction, giving various ketals under mild conditions.

Description: Mineral samples from the Prasolovskoe epithermal Au-Ag deposit, Russia, were investigated via transmission electron microscopy (TEM). One component was identified as the mineral kurilite Ag 8 Te 3 Se according to the data obtained from electron diffraction (ED) and Fourier transform analyses of high resolution micrographs. Micrometer-sized grains of kurilite were found next to other noble metal chalcogenide domains like the hessite-type. The EDX microprobe analyses of the kurilite domains were determined with the chemical composition Ag 7.9 Au 0.1 Te 2.9 Se 1.0 which is consistent with kurilite doped by gold. Additionally noble metal polychalcogenidehalides (NMPH) were identified via ED. Monoclinic and tetragonal polymorphs of Ag 5 Te 2 Cl were observed for the first time in a mineral sample. One additional component, whose composition equates the kurilite-type component with regard to Ag, Au, Te, and Se but with a marginal chlorine component, crystallizes in a structure type known from synthetic NMPH, namely Ag 23 Te 12 X (X = Cl, Br). This phase as well as the phases Ag 10 Te 4 Br 3 and Ag 20 Te 10 Br 2 was found next to each other in an also investigated synthetic sample.

Description: Eight chelating resins were synthesized in high yields by supporting 2-aminomethylpyridine, 2, 2′-dipyridylamine, 1, 2-phenylenediamine and 1, 2-ethylenediamine on Merrifield and Wang resins, respectively. These resins were used both as support of reducing complexes and as alkali metal sensors. 16 stable and easy to prepare reducing complexes, derived from the chelating resins and LiBH 4 and NaBH 4 , were prepared in good yields. These complexes showed chemoselectivity to reduce aldehydes in a low molar ratio and short time reactions. The fluorescence-sensing behavior of the chelating resins for alkali metal was studied. The fluorescence response of the materials where 1, 2-phenylenediamine is supported on Merrifield and Wang resins indicate that they behave as sensors for Li + and K + , respectively.

Description: The reaction of Fe 3 (CO) 12 with (C 3 H 5 ) 2 NCS 2 K in THF at room temperature afforded a red-brown solution. Treatment of the thus-obtained solution with MeI and PhCH 2 Br afforded clusters 1 , (μ-MeS)Fe 2 (CO) 6 (μ 4 -S)Fe 2 (CO) 6 (μ-CN(C 3 H 5 ) 2 ), and 2 , (μ-PhCH 2 CO)Fe 2 (CO) 6 (μ 4 -S)Fe 2 (CO) 6 (μ-CN(C 3 H 5 ) 2 ). Their structures were unambiguously determined by X-ray crystallography. Therefore, this methodology provides a novel route for the syntheses of spiro-S Fe/S clusters with aminocarbyne ligands.

Description: This study presents the preparation of 5-azido-3-nitro-1 H -1,2,4-triazole ( 1 ) in both good yield and high purity, starting from commercially available chemicals in a three step synthesis. Furthermore, several metal and nitrogen-rich salts with sodium ( 3 ), potassium ( 4 ), cesium ( 5 ), silver ( 6 ), lead ( 7 ), ammonium ( 8 ), guanidinium ( 9 ), and aminoguanidinium ( 10 ) were prepared by simple acid-base reactions. All compounds were well characterized by various means, including vibrational (IR, Raman) and multinuclear ( 1 H, 13 C, 14 N, 15 N) NMR spectroscopy, mass spectrometry, and DSC. Additionally the structure of 7 was determined by single-crystal X-ray diffraction. The sensitivities towards various outer stimuli (impact, friction, electrostatic discharge) were determined according to BAM standards. The metal salts were tested as potential primary explosives utilizing various preliminary tests.

Description: With Sharpless' and Meldal's discovery of the immensely supportive effect that metal catalysis has on Huisgen's classical 1,3-dipolar cycloaddition, azides (RN 3 ) – long underappreciated in organic synthesis – suddenly got in the focus of attention as most crucial players in sensational ‘click chemistry'. Less noisy though with the same commitment and even a much broader scope of scientific topics and objectives, the inorganic azide chemistry has made just as great strides in the last few decades. This review (Part I) gives an introductory survey of the most important results, and informs about modern developments and general trends. Particular emphasis is placed on the recent successful approaches to highly unstable homoleptic azido metal complexes of the main group and early transition elements, as well as on the enormous structural versatility caused by the ‘flexidentate' N 3 – ligand with its unsurpassed bridging capacities. The presentation in this paper of selected compounds and reactions is meant, in a way, as a prelude to the [3+2]-cycloadditions of metal azides and related species which will be covered in-depths in Part II. A large part of the comments finally deals with applications in fields such as catalysis, high explosive performance or magnetism of metal compounds containing azide, today certainly one of the most attractive research areas world-wide.

Description: The long-chain ligand, 1-phenyl-3-methyl-4-heptanoyl-pyrazol-5-one (HL) and its zinc(II) complex ZnL 2 were synthesized. The structure and the properties of ZnL 2 were characterized by elemental analysis, IR spectroscopy, X-ray diffraction, and thermogravimetric analysis. The zinc ion is five-coordinated in a square-pyramidal environment by four oxygen atoms of the HL ligands in the equatorial plane and one water molecule in the axial position. The water molecule is directly bonded to Zn 2+ and involved in intermolecular hydrogen bonding network. The complex and its corresponding ligand were screened in vitro against some strains of the human pathogenic bacteria. The metal complex exhibits higher antibacterial activity than its corresponding ligand. The complex exhibits purple effect emission as the result of fluorescence from the intraligand emission excited state.

Description: The microporous metal-organic framework Cd 2 (ABTC)(H 2 O)(DMA) 2 · H 2 O · 3DMA ( 1 ) (H 4 ABTC = 3,3′,5,5′-azobenzenetetracarboxylic acid; DMA = N , N ′-dimethylacetamide) was prepared by solvothermal reaction and characterized. X-ray structure analysis revealed that compound 1 is a three-dimensional (3D) open framework with 2D channels. The topology is based on a PtS net, constructed of 4-connected rectangular ABTC 4– units with 4-connected tetrahedral dinuclear Cd 2 (CO 2 ) 4 (H 2 O)(DMA) 2 secondary building units (SBUs). The solid-state excitation-emission spectra showed that the strongest emission peak is at 403 nm upon excitation at λ = 287 nm.

Description: P(2-SHC 6 H 4 ) 3 ( PS 3 H 3 ) reacts with GaMe 3 (1:1) to give GaMe{P(2-SC 6 H 4 ) 2 (2-SHC 6 H 4 )-κ 3 S , S′,P } ( 1 ), which could be deprotonated with NEt 3 to give [NEt 3 H][GaMe{P(2-SC 6 H 4 ) 3 -κ 3 S , S′,P }] ( 2 ). The 1:2 reaction of E (2-SHC 6 H 4 ) 3 [ E = P ( PS 3 H 3 ), As ( AsS 3 H 3 )] with GaMe 3 gave the dinuclear complexes GaMe{ E (2-SC 6 H 4 ) 2 (2-S{GaMe 2 (THF)}C 6 H 4 )-κ 3 S , S′,E } [ E = P ( 3 ), As ( 4 )]. Serendipitous hydrolysis of 4 resulted in small amounts of the hexanuclear gallium hydroxide complex cyclo -{GaMe(μ-OH)} 6 {As(2-SC 6 H 4 ) 3 -κ S , S′,S′′ } 2 ( 5 ). Complexes 1 – 4 were fully characterized, complexes 2 – 5 also by X-ray crystallography.

Description: Topological aspects of the experimental electron density in TiB 2 reconstructed on base of the multipole model are obtained from high-resolution single-crystal X-ray diffraction data. The features of electron density are compared with quantum chemical calculations and analysed in terms of Quantum Theory of Atoms in Molecules for the interpretation of atomic interactions. In spite of some differences in the Laplacian, both experimental and calculated density confirmed two main bonding interactions. The B–B bond critical point suggests a shared-type interaction with pronounced ellipticity in the boron layer, whereas B–Ti bond critical point reveals an interaction intermediate between shared and closed-shell type. Both, theory and experiment indicate a non-structured spherical topology in the penultimate shell of Ti. Integration of the electron density over the atomic basins reveals a charge transfer of 1.1 e (experiment) and 1.4 e (theory) from titanium to boron network, respectively.

Description: The stannides Li 2 CuSn 2 and Li 2 AgSn 2 were synthesized by induction-melting (or in a muffle furnace) of the elements in sealed niobium ampoules. The new phases were characterized by powder X-ray diffraction. The structures of both stannides were investigated by X-ray diffraction on single crystals: Li 2 AuSn 2 type, I 4 1 / amd , a = 442.6(1), c = 1940.9(8) pm, wR 2 = 0.0742, 310 F 2 values for Li 2 CuSn 2 and a = 456.33(9) c = 2018.2(6) pm, wR 2 = 0.0626, 339 F 2 values for Li 2 AgSn 2 with 10 variables for each refinement. The transition metal ( T ) atoms have tetrahedral tin coordination. The T Sn 4 tetrahedra are condensed via common corners forming layers that are further condensed by Sn–Sn bonding, leading to three-dimensional [CuSn 2 ] and [AgSn 2 ] networks which leave distorted hexagonal channels for the lithium atoms. The lithium ions show considerable mobility, with activation energies of 0.29 and 0.47 eV extracted from variable temperature 7 Li solid state NMR spectra. 119 Sn Mössbauer spectra at 78 K show signals at isomer shifts of δ = 2.13(1) mm s –1 for Li 2 CuSn 2 and δ = 2.07(1) mm s –1 for Li 2 AgSn 2 . The signals show electric quadrupolar splitting because of the non spherical environment of the tin nuclei. A minor impurity of β-Sn could be identified in both spectra.

Description: The complexes [Ni 2 (L) 2 ] 2 · H 2 O ( 1 ) and [Cu 2 (L) 2 (H 2 O)] · 2CH 3 OH ( 2 ) were prepared by reaction of the chiral Schiff base ligand N -[(1 R ,2 S )-2-hydroxy-1, 2-diphenyl]-acetylacetonimine (H 2 L) with Ni II and Cu II ions, respectively, aiming to develop economically and environmentally-friendly catalysts for the hydrogenation of ketones. They have a dinuclear skeleton with axial vacant sites. The catalytic effects of the two complexes for hydrogenation of ketones were tested using dihydrogen gas as hydrogen source. They present some catalytic effects in hydrogenation of acetophenone, which has a dependence on the temperature and base used in these reactions. However, no apparent catalytic effects were found for the two complexes in hydrogenation of 4-nitroacetophenone and 4-methylacetophenone. Although the catalytic conversion in these hydrogenation reactions is low, they do represent a kind of cheap and environmentally-friendly hydrogenation catalyst.

Description: Poised to investigate the association of vanadium with physiological substrates in materials capable of exerting anticancer biological activity, pH-specific synthetic chemical reactivity between vanadium and triethyl ammonium acetate/trigonelline in aqueous and mixed organic-aqueous media led to the isolation of three new binary composite materials, namely K 2 [(MeN(+)C 5 H 4 COOH) 2 ][V 10 O 28 H 2 ] · 2H 2 O ( 1 ), [(H 2 N(+)Me 2 ) 4 ][V 10 O 28 H 2 ][Me 3 N(+)CH 2 COO(–)] 2 ( 2 ), and [(Me 3 N(+)CH 2 COOH) 4 ][V 10 O 28 H 2 ][Me 3 N(+)CH 2 COO(–)] 2 · 2H 2 O ( 3 ). 1–3 were characterized by elemental analysis, FT-IR and UV/Vis spectroscopy, Cyclic voltammetry, TGA-DTG, and X-ray crystallography. In all three compounds, the [V 10 O 28 H 2 ] 4– core unit is a common cluster assembly, with the vanadium in the +5 oxidation state. The counteracting cationic assembly in each composite material originates in the betaine starting reagent or the solvent out of which the materials crystallized. Biological activity studies of 1 and 3 in vitro in MCF-7 breast epithelial and A549 lung adenocarcinoma cell cultures show that both materials inhibit the viability of both cell lines in a dose-dependent fashion, in juxtaposition to the behavior of the betaine components present in these materials. Collectively, the herein studies a) reveal the uniquely defined synthetic methodologies and physicochemical properties of the variably assembled [V 10 O 28 H 2 ] 4– core units crystallized into the composite binary polyoxovanadate-betaine lattice structures, b) unravel the distinct cytotoxicity profile of the composite materials toward MCF-7 and A549 cells, and c) attest to their future potential as metallodrugs of pharmacological significance in anticancer activity.

Description: Testosterone exerts important effects in the heart. Cardiomyocytes are target cells for androgens, and testosterone induces rapid effects via Ca 2+ release and protein kinase activation and long-term effects via cardiomyocyte differentiation and hypertrophy. Furthermore, it stimulates metabolic effects such as increasing glucose uptake in different tissues. Cardiomyocytes preferentially consume fatty acids for ATP production, but under particular circumstances, glucose uptake is increased to optimize energy production. We studied the effects of testosterone on glucose uptake in cardiomyocytes. We found that testosterone increased uptake of the fluorescent glucose analog 2-(N-(7-nitrobenz-2-oxa-1, 3-diazol-4-yl)amino)-2-deoxyglucose and [ 3 H]2-deoxyglucose, which was blocked by the glucose transporter 4 (GLUT4) inhibitor indinavir. Testosterone stimulation in the presence of cyproterone or albumin-bound testosterone induced glucose uptake, which suggests an effect that is independent of the intracellular androgen receptor. To determine the degree of GLUT4 cell surface exposure, cardiomyocytes were transfected with the plasmid GLUT4 myc -eGFP. Subsequently, testosterone increased GLUT4 myc- GFP exposure at the plasma membrane. Inhibition of Akt by the Akt-inhibitor-VIII had no effect. However, inhibition of Ca 2+ /calmodulin protein kinase (CaMKII) (KN-93 and autocamtide-2 related inhibitory peptide II) and AMP-activated protein kinase (AMPK) (compound C and siRNA for AMPK) prevented glucose uptake induced by testosterone. Moreover, GLUT4 myc- eGFP exposure at the cell surface caused by testosterone was also abolished after CaMKII and AMPK inhibition. These results suggest that testosterone increases GLUT4-dependent glucose uptake, which is mediated by CaMKII and AMPK in cultured cardiomyocytes. Glucose uptake could represent a mechanism by which testosterone increases energy production and protein synthesis in cardiomyocytes. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: The crystal structures of the alkali aluminium thiohypodiphosphates M I AlP 2 S 6 (M I = Li, Na) are reported. NaAlP 2 S 6 crystallizes in the orthorhombic space group Fdd 2 (no. 43) with a = 8.0400(2), b = 10.9452(2), c = 20.8801(4) Å, and V = 1837.44(7) Å 3 ( Z = 8). It is isostructural with AgAlP 2 S 6 , which is consistent with the similar ionic radii of Na and Ag. In contrast, LiAlP 2 S 6 crystallizes in a different structure type which has not been observed in the large number of thiohypodiphosphates reported so far. It crystallizes in the monoclinic space group C 2/ c (no. 15) with a = 6.783(3), b = 10.365(4), c = 11.776(4) Å, β = 94.399(5)°, and V = 825.46(5) Å 3 ( Z = 4).

Description: We present the synthesis of 7-(diphenylphosphine)-indole 1 ( HPinol ) as a novel mono- and bidentate P - and N, P -ligand and its coordination chemical behaviour towards the d 6 - and d 8 -transition metals rhodium(III), palladium(II) and rhenium(I). The reaction of 1 with [Cp*RhCl 2 ] 2 in a 1:2 molar ratio leads to the formation of the P -coordinated complex [RhCl 2 ( P –( HPinol ))] ( 2 ). In the presence of the weak base NEt 3 , HCl elimination occurs by forming the neutral amido-phosphine chelated complex [RhCl( N, P –( Pinol ))] ( 3 ). The same P - and N, P -coordination is observed for palladium(II), where two ligands 1 coordinate to the metal centre forming the neutral complexes [PdCl 2 ( P – HPinol ) 2 ] ( 4 ) and [Pd( N, P – Pinol ) 2 ] ( 5 ). The reaction of Re(CO) 5 Br in the presence of NEt 3 and PPh 3 delivers the amido-phosphine complex [Re(CO) 3 PPh 3 ( N, P – Pinol )] ( 6 ). All products were characterised by multinuclear NMR spectroscopy, MS and IR spectra as well as elemental analysis. Furthermore, crystal structures of ligand 1 and all complexes 2–6 are presented.

Description: Although the role of Cbl-family proteins as key cellular regulators has been established, phenomena regulated in a Cbl-dependent fashion are multiple and the mechanisms mediating the effects of Cbl proteins are diverse. This finding makes it important to consider different phenomena affected by functions of Cbl proteins individually. Among effects of Cbl on various biological functions there are many cases of regulation of cellular phenomena related to cytoskeletal rearrangements, such as cell adhesion, motility and invasion. Some of these regulatory functions are mediated by adaptor-type interactions of Cbl, especially by Cbl-dependent modulation of phosphatidyl-inositol-3' kinase (PI3K), while others are caused by Cbl-dependent ubiquitylation of various cytoskeletal and regulatory proteins, identified and unidentified. The role of Cbl in regulation of cytoskeleton-dependent cellular functions is discussed in this review. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: In the course of investigations relating to magnesia oxysulfate cement the basic magnesium salt hydrate 3Mg(OH) 2 · MgSO 4 · 8H 2 O (3–1–8 phase) was found as a metastable phase in the system Mg(OH) 2 -MgSO 4 -H 2 O at room temperature (the 5–1–2 phase is the stable phase) and was characterized by thermal analysis, Raman spectroscopy, and X-ray powder diffraction. The complex crystal structure of the 3–1–8 phase was determined from high resolution laboratory X-ray powder diffraction data [space group C 2/ c , Z = 4, a = 7.8956(1) Å, b = 9.8302(2) Å, c = 20.1769(2) Å, β = 96.2147(16)°, and V = 1556.84(4) Å 3 ]. In the crystal structure of the 3–1–8 phase, parallel double chains of edge-linked distorted Mg(OH 2 ) 2 (OH) 4 octahedra run along [–110] and [110] direction forming a pattern of crossed rods. Isolated SO 4 tetrahedra and interstitial water molecules separate the stacks of parallel double chains.

Description: Widespread changes in gene expression underlie B cell development and activation, yet our knowledge of which chromatin-remodeling factors are essential is limited. Here, we demonstrate that the BRG1 catalytic subunit of SWI/SNF complexes was dispensable for murine B cell development but played an important, albeit selective, role during activation. Although BRG1 was dispensable for CD69 induction and differentiation into plasma cells based on the ability of mutant B cells to undergo hypertrophy and secrete IgM antibodies, it was required for robust cell proliferation in response to activation. Accordingly, BRG1 was required for only ∼100 genes to be expressed at normal levels in naïve B cells but 〉1,000 genes during their activation. BRG1 upregulated 5-fold more genes than it downregulated, and the toll-like receptor pathway and JAK/STAT cytokine-signaling pathways were particularly dependent on BRG1. The importance of BRG1 in B cell activation was underscored by the occurrence of opportunistic Pasteurella infections in conditionally mutant mice. B cell activation has long served as a model of inducible gene expression, and the results presented here identify BRG1 as a chromatin-remodeling factor that upregulates the transcriptome of B cells during their activation to promote rapid cell proliferation and to mount an effective immune response. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: The cover picture shows the synthesis and the molecular structure of a zwitterionic [4.3.0]-bicyclic aluminum-phosphorus compound with annulated C 3 P 2 and Al 2 C 2 PH heterocycles and a 3c-2e Al–H–Al bond. Treatment of the dialkynylphosphine Mes–P(–C=C–CMe 3 ) 2 ( 1 ) with diethylaluminum hydride ( 2 ) in an equimolar ratio afforded a mixture of compounds, in which a [3.2.0]-bicyclic compound 3 with annulated fourmembered AlC 2 P and five-membered P 2 C 3 heterocycles could be identified by NMR spectroscopy. Excess of the hydride 2 yielded small quantities of the zwitterionic [4.3.0]-bicyclic compound 4 , which formally resulted from the unique insertion of a diethylaluminum hydride molecule into the Al–C(vinyl) bond of the strained fourmembered heterocycle of 3 . A six-membered ring is formed which contains an Al–H–Al 3c-2e bond. More details can be found in the Article by Werner Uhl et al. on page 1181 ff.

Description: Using the bis(pyrazolyl)pyridinylmethane ligand α,α,α-bis(1-pyrazolyl)(2-pyridinyl)toluene {(ph)C(pz) 2 (py)} for bioinorganic inspired coordination chemistry studies, we synthesised and structurally characterised three monofacial complexes [{(ph)C(pz) 2 (py)}CoCl 2 ] ( C1 ), [{(ph)C(pz) 2 (py)}CuCl 2 ] ( C2 ), [{(ph)C(pz) 2 (py)}ZnCl 2 ] ( C3 ) and the binuclear halogenido-bridged complexes [{(ph)C(pz) 2 (py)} 2 (μ-Cl) 2 Fe 2 Cl 2 ] ( C4 ) and [{(ph)C(pz) 2 (py)} 2 (μ-Br) 2 Cu 2 Br 2 ] ( C5 ). In four of these complexes, severe disorders between pyrazolyl and pyridinyl donor groups are observed such that bis(pyrazolyl) and (pyrazolyl)(pyridinyl) coordination modes are concomitantly found. The donor competition is dissected by DFT calculation of the energy differences between the two coordination modes and NBO analysis of the donor situation. The pyrazolyl units provide with more donor strength although pyridine is considerably more basic.

Description: Metal ions poisoning can result from environmental factors, intentional action, or disruption of homeostasis. Although the origin of toxicity may be different, the treatment is similar. Chelation therapy aims to remove the excess of metal ions from tissues to stop further damage of cells. For almost every metal ion, molecules that are able to bind it and remove from the human body are known. Over the years some new chelating agents were discovered and introduced into clinical treatment. In this paper we have focused on typical chelators for metal ions, both essential and toxic for humans. The treatment of poisoning caused by essential metal ions is hard due to the risk of removing them from the biologically relevant molecules (e.g. enzymes). Acute metal ions poisoning is rather rare, so the development of chelators for such cases are historical, but prolonged toxicity of, especially, essential metal ions is extensively studied.

Description: The reactions of [Os(NO)Cl 5 ] 2– with glycine (GlyH), picolinic acid (PicoH), L -proline ( L -ProH) and D -proline ( D -ProH) afforded four novel complexes of the general formula [Os(NO)Cl 3 (AA)] – , where AA = Gly, Pico, L -Pro and D -Pro, respectively. X-ray diffraction studies have revealed that in all cases the same isomer type from three theoretically possible, has been isolated, namely mer (Cl), trans (NO, O)-[Os(NO)Cl 3 (AA)] – . Spectroscopic and electrochemical properties, behavior in aqueous solution and antiproliferative activity in three human cancer cell lines are also reported.

Description: The electron distributions in position and in momentum space of the hcp metals magnesium and zinc are investigated experimentally and compared to results of quantum-chemical calculations. Furthermore, a survey is given on recent analyses of the bonding properties of zinc and cadmium, using the method of increments. The experimental deformation densities were obtained by refining multipole models to X-ray diffraction data sets measured at 100 K with either Mo- K α (Mg) or Ag- K α (Zn) radiation. The final R F values (Valray/Jana2006) are 0.0028/0.0034 (Mg) and 0.0068/0.0068 (Zn). The differences to deformation densities obtained from periodic density functional calculations are discussed. The effect of dynamical electron correlation on the electron density was analyzed, using cluster models. Compton profiles were measured with 88.67 keV synchrotron radiation at beamline ID15B at the ESRF in Grenoble. Varied orientations of the samples allowed for probing the projected momentum distribution along the [100], [423] and [001] directions. Fourier transforms of the computed reciprocal form factor B ( r ) resulted in the corresponding theoretical Compton profiles. It is suggested that the anomalous hcp structure of zinc is favored by a kinetic balancing of the valence electrons, i.e. correlation mediated 4 s -3 d interactions.

Description: . This Research Report provides an overview on synthesis, structure, and reactivity of the recently discovered carboranylamidinate ligands. Carboranylamidinate anions of the type [( o -C 2 B 10 H 10 C(NHR)(=N R )] – ( R = i Pr, cyclohexyl) are readily accessible via addition of o -lithiocarborane to N , N ′-carbodiimides R –N=C=N– R . They combine the highly versatile characteristics of both amidinates and carboranes in one unique ligand system. Unlike simple amidinate anions, the carboranylamidinates coordinate to metal ions not as typical N , N ′-chelating ligands but adopt an unexpected κ 2 C, N -bonding mode. The free imine functionality in carboranylamidinates can be further deprotonated. The resulting dianions were demonstrated to be excellent starting materials for novel boron-rich heterocycles incorporating e.g. Si, Sn, P, or transition metals such as Ti, Zr, Rh, and Ir. Further modification of the carboranylamidinate cage structure includes the introduction of additional functional groups like –SH or –SeH as well as the selective removal of a boron atom with formation of novel nido -type dicarbollylamidinate ligands. An initial study already showed that transition metal carboranylamidinates are potentially useful as polymerization catalysts.

Description: KSbWO 6 was prepared by sol-gel method. N-doped KSbWO 6 (KSbWO 6– x N x ) was obtained by heating KSbWO 6 and urea at 400 °C. Both the compounds are characterized by powder X-ray diffraction (XRD), TEM, SEM-EDS, X-ray photo electronic spectroscopy (XPS), and UV/Vis diffuse reflectance spectroscopy (UV-DRS). A shift in the peak positions of powder XRD and XPS spectra was observed. The band gap energy ( E g ) of KSbWO 6 and N-doped KSbWO 6 was obtained from their diffused reflectance spectra. E g was reduced from 3.17 eV to 2.56 eV upon nitrogen doping in KSbWO 6 . The reduction of the E g is attributed to the lifting of valence band of N-doped KSbWO 6 , due to the mixing of O 2p states with N 2p states. The photocatalytic activity of both the samples was studied by degradation of methylene blue (MB). The nitrogen doped KSbWO 6 shows higher photocatalytic activity compared to that of KSbWO 6 .

Description: Optical tweezers were used to scan individual Chronic Myelogenous Leukemia cells to determine if the cell death depends on the scanning conditions. Although increasing the scanning frequency or amplitude means greater force applied to the cells, their effects on cell death are not a simple increasing trend, as observed in the optical microscopy. Indeed, cell death sharply increased at particular screening frequencies and amplitudes, whereas other frequencies or amplitudes were less detrimental. These results suggest that cell damage was more sensitive to certain scanning conditions, rather than simply high applied forces. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: Odontoblasts, which derive from dental papilla, are a type of terminally differentiated matrix-secreting cells. Previous studies have identified various transcription factors involved in the differentiation process of odontoblasts. We have recently found that Krüppel-like factor 4 ( Klf4 ) was expressed in the polarizing and elongating odontoblasts, but the function of Klf4 in the differentiation of odontoblasts is still unclear. We hypothesized Klf4 promoted the differentiation of odontoblasts by up-regulating some odontoblast-related genes. In this study, we found that the expression of Klf4 increased significantly during the odontoblastic differentiation of primary mouse dental papilla cells and the mouse dental papilla cell line-mDPC6T. Overexpression of Klf4 significantly up-regulated odontoblast-related genes, such as Dmp1 , Dspp , and Alp , and promoted the accumulation of mineral nodules. Knock-down of Klf4 down-regulated expression of Dmp1 , Dspp , and Alp , and inhibited mineral deposition. We applied in silico analysis and identified one target gene of Klf4 — Dmp1 . Based on further analysis of ChIP data, EMSA and dual luciferase activity assays, we confirmed that Klf4 was able to specifically bind to the Dmp1 promoter and transactivate its expression. Furthermore, forced expression of Dmp1 in the Klf4 knock-down mDPC6T cell line significantly recovered its odontoblastic differentiation ability. Our data confirmed our hypothesis that Klf4 promotes the differentiation of odontoblasts via the up-regulation of Dmp1 . © 2013 Wiley Periodicals, Inc.

Description: Nociception is the sensory mechanism used to detect cues that can harm an organism. The understanding of the neural networks and molecular controls of the reception of pain remains an ongoing challenge for biologists. While we have made significant progress in identifying a number of molecules and pathways that are involved in transduction of noxious stimuli, from the skin through the sensory receptor cell and from this to the spinal cord on into the central nervous system, we still lack a clear understanding of the perceptual processes, the responses to pain and the regulation of pain perception. Mice and rat animal models have been extensively used for nociception studies. However, the study of pain and noiception in these organisms can be rather laborious, costly and time consuming. Conversely the use of Drosophila and C. elegans may be affected by the large evolutionary distance between these animals and humans. We outline here the reasons why zebrafish presents a new and attractive model for studying pain reception and responses and the most interesting findings in the study of nociception that have been obtained using the zebrafish model. © 2013 Wiley Periodicals, Inc.

Description: Transforming growth factor (TGF)-β is a multifunctional cytokine acting during development, tissue homeostasis, regeneration processes and disease progression. Due to its pleiotropic effects, tight regulation of the induced signaling cascades is mandatory. Caveolin proteins regulate a specific endocytic pathway and modulate diverse signaling pathways and thus have been related to severe disorders, e.g. cancer and fibrosis. Caveolin affects TGF-β/-Smad and non-Smad signaling in many ways and thus can determine the cellular outcome upon TGF-β challenge. Reciprocal regulation of caveolin and TGF-β is also evident, ranging from gene expression to miRNA regulation. Finally, there is in vivo evidence that this crosstalk influences disease development and progression. This review gives an overview about the multifaceted relations of caveolin and TGF-β. © 2013 Wiley Periodicals, Inc.

Description: The chemistry of cytotoxic platinum(II) complexes is more or less restricted to ligand exchange reactions, derivatization of coordinated ligands is cumbersome, and subsequent purification in many cases impossible. Consequently, kinetically more inert platinum(IV) complexes found their way into the development of novel, promising anticancer drugs. Research has focused more and more during the last years on the use of platinum(IV) complexes featuring one or two axial succinato ligands in which one carboxylic acid moiety is available for further derivatization. In order to gain a deeper insight into the mechanism of action, isotopically labeled platinum(IV) complexes with axial (1,4– 13 C 2 )succinato ligands were synthesized and fully characterized by multinuclear ( 1 H, 13 C, 15 N, and 195 Pt) 1D- and 2D-NMR spectroscopy. Especially of note in this context is a long range 1 H, 13 C shift correlation signal detected between the equatorial ammine protons and the axially coordinated carboxylato moiety. Furthermore, their behavior in extracts of SW480 cancer cells was investigated. Preliminary results demonstrate that cisplatin analogs are reduced significantly faster in comparison to carboplatin analogs.

Description: The Cu II solution chemistry of synthetic derivatives of naturally occurring pseudo-octapeptides (patellamides and ascidiacyclamide) is described. The complex stabilities [mono- and dicopper(II) complexes] of five different ligands were determined by isothermal microcalorimetry (ITC), and square wave voltammetry (SQW) was used to elucidate the electrochemical properties. In agreement with published spectroscopic data, there is cooperative binding of two Cu II ions and the overall stabilities are, in agreement with known stabilities of the natural ligands and expectations based on the donor sets (two N-based heterocycles and one amide per Cu II ), only moderate ( K ≤ 10 6 ). There is a slight dependence of the stabilities on the ligand structure (configuration of the side chains), and that derived from the natural products forms the most stable complexes. Due to the complex equilibria in solution and the instability of the reduced forms, voltammetry shows complex equilibria, which preclude the full assignment of all processes. The positive reduction potentials are in agreement with relatively low complex stabilities. These observations complete earlier studies, concentrating on spectroscopy and structural aspects, and are also discussed in relation to the possible biological function of the cyclic peptides, i.e. metal ion transport, oxygen activation, carboanhydrase, and phosphatase activities.

Description: Setting out from protected L -cysteine a 2,5-diketopiperazine V can be synthesized, the reduction of which with NaBH 4 /TiCl 4 leads to (6 R ,8 aR )-7-methyl-6-(sulfanylmethyl)-thiazolidine [3,4- a ] piperazine, L 1 H as well as N , N ′-dimethyl-(2 R ,5 R )-bis(sulfanylmethyl) piperazine, L 2 H 2 , which were separated and characterized. L 2 H 2 can be obtained selectively, if V is reduced by NaBH 4 /TiCl 4 in the presence of DIEA · HCl, and it represents a precursor for a novel, chiral ligand, as after deprotonation it provides two thiolato and two amino donor functions for the coordination of a metal atom. Deprotonation of L 1 H and L 2 H 2 with NaOMe followed by treatment with NiBr 2 (dme) led to the isolation of the dimeric complexes [L 1 NiBr] 2 ( 1 ) and [L 2 Ni] 2 ( 2 ), respectively. Both were fully characterized, and cyclic voltammetry indicated the possibility of Ni II → Ni III oxidations for complex 2 . 2 can be regarded as a structural model for the A clusters of the acetyl coenzyme A synthase.

Description: Transforming growth factor (TGF)-β1 regulates diverse cellular functions. Particularly, TGF-β1 induces monocyte migration to sites of injury or inflammation in early period, whereas TGF-β1 inhibits cell migration in late phase. In this study, we attempted to understand how TGF-β1 suppresses cell migration in late phase. We found that TGF-β1 of short exposure induces the production of chemokines, such as macrophage inflammatory protein (MIP)-1α, by Raw 264.7 cells. However, knock-down of small GTPase RhoA by sh-RhoA inhibited the production of MIP-1α and macrophage migration, suggesting that RhoA is essential for expression of this chemokine. An activator of Epac ( e xchange p roteins directly a ctivated by c AMP; a guanine nucleotide exchange factor of Rap1), 8CPT-2Me-cAMP which leads to Rap1 activation abrogated MIP-1α expression and macrophage migration. Indeed, GTP-RhoA and GTP-Rap1 levels were reciprocally regulated in a time-dependent manner following TGF-β1 stimulation. 8CPT-2Me-cAMP suppressed GTP-RhoA levels, whereas si-Rap1 augmented GTP-RhoA levels and cell migration. TGF-β1 produced cAMP in late period and si-RNAs of Epac1 (exchange protein directly activated by cAMP 1) and Epac2 reduced GTP-Rap1 levels leading to promotion of GTP-RhoA levels. Furthermore, si-RNA of ARAP3 (Rap-dependent RhoGAP) increased GTP-RhoA level and cell migration. Therefore, we propose the mechanism that prolonged TGF-β1 treatment produce cAMP, which activates sequentially Epac, Rap1 and ARAP3, resulting in suppression of RhoA, chemokine expression, and macrophage migration. Contrary to the general concept that Rap1 stimulates cell migration, we demonstrated in this study that Rap1 inhibits cell migration by suppression of RhoA activity in response to TGF-β1. © 2013 Wiley Periodicals, Inc.

Description: Polycyclic Aromatic Hydrocarbons (PAHs) are the products of incomplete combustion of organic materials, which are present in cigarette smoke, deep-fried food, and in natural crude oil. Since PAH-metabolites form DNA adducts and cause oxidative DNA damage, we asked if these environmental carcinogens could affect transforming potential of the human Polyomavirus JC oncoprotein, T-antigen (JCV T-antigen). We extracted DMSO soluble PAHs from Deepwater Horizon oil spill in the Gulf of Mexico (oil-PAHs), and detected several carcinogenic PAHs. The oil-PAHs were tested in exponentially growing cultures on normal mouse fibroblasts (R508), and in R508 stably expressing JCV T-antigen (R508/T). The oil-PAHs were cytotoxic only at relatively high doses (1:50–1:100 dilution), and at 1:500 dilution the growth and cell survival rates were practically unaffected. This non-toxic dose triggered however, a significant accumulation of reactive oxygen species (ROS), caused oxidative DNA damage and the formation of DNA double strand breaks (DSBs). Although oil-PAHs induced similar levels of DNA damage in R508 and R508/T cells, only T-antigen expressing cells demonstrated inhibition of high fidelity DNA repair by homologous recombination (HRR). In contrast, low-fidelity repair by non-homologous end joining (NHEJ) was unaffected. This potential mutagenic shift between DNA repair mechanisms was accompanied by a significant increase in clonal growth of R508/T cells chronically exposed to low doses of the oil-PAHs. Our results indicate for the first time carcinogenic synergy in which oil-PAHs trigger oxidative DNA damage and JCV T-antigen compromises DNA repair fidelity. © 2013 Wiley Periodicals, Inc.

Description: The intracellular pH is regulated by a delicate balance of ion distribution across the plasma membrane and the physico-chemical properties of intra- and extracellular components. We analysed the effects of glycosaminoglycans on the intracellular pH of fibroblasts by using the fluorescent pH indicator BCECF-AM. Addition of hyaluronan, hyaluronan oligosaccharides, chondroitin sulfate or heparin to the culture medium of fibroblasts caused intracellular acidification from pH 7.2 to pH 6.7 in a concentration dependent manner. High molecular weight hyaluronan acidified more than hyaluronan oligosaccharides at the same concentrations. Hyaluronidase treatment or inhibition of hyaluronan export with xanthohumol led to intracellular alkalization. These observations indicated that extracellular glycosaminoglycans participate in intracellular pH regulation. The mechanism was explained by Donnan effects and molecular crowding. © 2013 Wiley Periodicals, Inc.

Description: Purpose To test whether the use of a striatum weighted image may improve registration accuracy and diagnostic outcome in patients with parkinsonian syndromes (PS). Methods Weighted images were generated by increasing signal intensity of striatal voxels and used as intermediate dataset for co-registering the brain image onto template. Experimental validation was performed using an anthropomorphic striatal phantom. 123 I-FP-CIT SPECT binding ratios were manually determined in 67 PS subjects an and compared to those obtained using unsupervised standard (UWR) and weighted registered (WR) approach. Normalized cost function was used to evaluate the accuracy of phantom and subjects registered images to the template. Reproducibility between unsupervised and manual ratios was assessed by using intra-class correlation coefficient (ICC) and Bland and Altman analysis. Correlation coefficient was used to assess the dependence of semi-quantitative ratios on clinical findings. Results Weighted method improves accuracy of brain registration onto template as determined by cost function in phantom (0.86 ± 0.06vs.0.98 ± 0.02; Student's t test, P = 0.04) and in subject scans (0.69 ± 0.06vs.0.53 ± 0.06; Student's t test, P 〈 0.0001). Agreement between manual and unsupervised derived binding ratios as measured by ICC was significantly higher on WR as compared to UWR images (0.91vs.0.76). Motor UPDRS score was significantly correlated with manual and unsupervised derived binding potential. In phantom as well as in subjects studies, correlations were more significant using the WR method (BPm: R 2  = 0.36,p = 0.0001; BPwr: R 2  = 0.368, P  = 0.0001; BPuwr: R 2  = 0.300, P  = 0.0008). Conclusion Weighted registration improves accuracy of binding potential estimates and may be a promising approach to enhance the diagnostic outcome of SPECT imaging, correlation with disease severity, and for monitoring disease progression in parkinsonian syndromes. © 2013 Wiley Periodicals, Inc.

Description: A new chiral racemic ligand ( o -carboranyl)bis(2-hydroxymethyl)pyridine oCB(hmpH) 2 , that is composed of a central o -carborane unit where two arms radiate out of the cluster carbons each one containing a 2-pyridylmethylalcohol chelating arms, provides two potentially bidentate {NO} or one tetradentate {N 2 O 2 } binding pockets. An unprecedented octahedral Co II complex [CoCl 2 ( anti - oCB (hmpH) 2 ] was obtained under aerobic conditions and characterized by X-ray crystallography as well as IR and NMR spectroscopy. anti - oCB (hmpH) 2 acts as a tetradentate N 2 O 2 -ligand affording the complex as a racemic mixture of cis- α Δ-[CoCl 2 ( RR anti - oCB (hmpH) 2 )] and Λ-[CoCl 2 ( SS anti - oCB (hmpH) 2 )]. The new ligand oCB(hmpH) 2 appears to be suitable for producing a variety of new chiral-at-metal complexes.

Description: Abstract. The title compounds NH 4 [Cu(S 2 CNH 2 ) 2 ] · H 2 O (A) and CuS 2 CNH 2 (B) were prepared from aqueous alcoholic solutions by reaction of ammoniumdithiocarbamate with copper sulfate in presence of excess cyanide as reductive. (A) crystallizes in the orthorhombic space group C 222 1 (No. 20) with a = 8.9518(6), b = 9.6414(6) and c = 10.6176(8) Å, Z = 4. (B) crystallizes in the orthorhombic space group P 2 1 2 1 2 1 (No. 19) with a = 5.9533(4), b = 6.6276(4) and c = 9.4834(5) Å, Z = 4. In the crystal structure of (A) copper has a tetrahedral surrounding of four monodentate dithiocarbamate ligands. These structural units form 2D nets stacked along [001]. Staggered chains consisting of H 2 O and NH 4 + penetrate the crystal structure along [001] yielding additional coherence via hydrogen bonds. The crystal structure of (B) comprises a three-dimensional tetrahedral framework of CuS 4 units exclusively linked by vertices. The arrangement is reminiscent of a filled β -cristobalite structure with the dithiocarbamate ligands extending into the hollow spaces. Thermal decomposition precedes stepwise finally giving Cu 2 S in each case.

Description: A thorough study on the thermoelectric potential of the layered compound SnBi 2 Te 4 is presented. Phase range studies on SnBi 2 Te 4 , unit cell parameters by powder X-ray diffraction, and electronic structure calculations (both LDA and GGA functional) were performed. Physical property measurements regarding substitution of tin and bismuth with the triel ( Tr = Ga, In, Tl) elements are presented towards the improvement of thermoelectric properties, according to Tr x Sn 1– x Bi 2 Te 4 and Tr x SnBi 2– x Te 4 . The range of inclusion was generally over 0.01 ≤ x ≤ 0.15 to monitor compound changes as well as phase purity limits. Seebeck coefficient, S , electrical conductivity, σ , and thermal conductivity, κ , were measured, yielding the dimensionless Figure of merit, ZT , data over a temperature range between 300 K and 680 K. Results of partial replacements of tin and bismuth are compared and reported. ZT max values range from 0.10 to 0.34 depending on the dopant, achieved at temperatures from 355 K to 420 K.

Description: A new two-step procedure for the synthesis of MoS 2 nanotubes using lead as a growth promoter is reported. In the first step, molybdenum suboxide nanowhiskers containing a small amount of lead atoms were created by exposing a pressed MoS 2 +Pb mixture to highly compressed shock-heated argon gas, with estimated temperatures exceeding 9900 K. In the second step, these molybdenum suboxide nanowhiskers served as templates for the sulfidization of the oxide into MoS 2 nanotubes (by using H 2 S gas in a reducing atmosphere at 820 °C). Unlike the case of WS 2 nanotubes, the synthesis of a pure phase of MoS 2 nanotubes from molybdenum oxide has proven challenging, due mostly to the volatile nature of the latter at the high requisite reaction temperatures (〉800 °C). In contrast, the nature and apparent reaction mechanism of the method reported herein are amenable to future scale-up. The high-temperature shockwave system should also facilitate the synthesis of new nanostructures from other layered materials.

Description: The reaction of RuCl 2 (PPh 3 ) 3 with N -pyrazolylpropanamide ( N -ppa) displaces a single PPh 3 producing the six-coordinate complex RuCl 2 (PPh 3 ) 2 ( N -ppa) ( 1 ). A crystal structure determination of the dichloromethane solvate RuCl 2 (PPh 3 ) 2 ( N -ppa) · 2CH 2 Cl 2 ( 1·2CH 2 Cl 2 ) revealed that the geometry about the central Ru atom is distorted octahedral with the chloride ligands in trans -position and the N -ppa acting as N , O -chelating ligand. In the solid state, RuCl 2 (PPh 3 ) 2 ( N -ppa) molecules are dimerized via N–H ··· Cl hydrogen bonds. The dimers pack as chains in the c direction and form voids that are occupied by dichloromethane solvent molecules.

Description: Four complexes with supramolecular architectures, namely, MZCA · 3H 2 O ( 1 ), [Zn(H 2 O) 6 ] 2+ · [MZCA] 2 · [H 2 O] 6 ( 2 ), [Mn(MZCA) 2 (H 2 O) 4 ] · 2H 2 O ( 3 ), and [Ni(MZCA) 2 (H 2 O) 4 ] · 2H 2 O ( 4 ) [MZCA = 3-(carboxymethyl)-2, 7-dimethyl-3H-benzo[d]imidazole-5-carboxylic acid], were synthesized and characterized by elemental analysis, IR spectroscopy, and single-crystal X-ray diffraction. Complexes 1 and 2 display a remarkable 3D network with 1D hydrophilic channels. Complexes 3 and 4 are isostructural and exhibit a 3D structure encapsulating 1D 24-membered ring microporous channels. The UV/Vis and fluorescent spectra were measured to characterize complexes 1 – 4 . The thermal stability of complexes 2 – 4 were also examined.

Description: The transition metal dihydrogen hypodiphosphate hydrates K 2 [Co(H 2 P 2 O 6 ) 2 (H 2 O) 2 ] · H 2 O ( 1 ), K 2 [Ni(H 2 P 2 O 6 ) 2 (H 2 O) 2 ] · H 2 O ( 2 ), K 2 [Cu(H 2 P 2 O 6 ) 2 (H 2 O) 2 ] · H 2 O ( 3 ) and K 2 [Zn(H 2 P 2 O 6 ) 2 (H 2 O) 2 ] · H 2 O ( 4 ) were synthesized and characterized by single crystal structure determination. The compounds 1 – 4 crystallize isotypic in the monoclinic space group C 2/ m (no. 12) with two formula units in the unit cell. The crystal structure is built up by [H 2 P 2 O 6 ] 2– units in an eclipsed conformation, by the corresponding transition metal, potassium cations, and water molecules. The eclipsed conformation of the [H 2 P 2 O 6 ] 2– has not been previously observed in none of known hypodiphosphates(IV) analyzed via X-ray diffraction. However, its proposed based on spectroscopic methods. FT-IR/FIR and FT-Raman spectra of the crystalline salts were recorded and the thermal behavior of the compounds was investigated.

Description: Two coordination polymers, [Co 2 (Hcpip) 2 (phth)] n · 3 n (H 2 O) ( 1 ) and [Mn 2 (Hcpip) 2 (phth)] n ( 2 ), {H 2 cpip = 2-(2-carboxyphenyl)imidazo[4,5-f](1,10)- phenanthroline, H 2 phth = phthalic acid}, were hydrothermally synthesized and characterized by elemental analysis, IR spectroscopy, and single-crystal X-ray diffraction. Complex 1 is a 1D chain, in which the dinuclear [Co 2 (Hcpip) 2 ] 2+ units are linked through (phth) 2– anions. Complex 2 is a 2D layer structure, which is constructed from the 1D chains bridged by (phth) 2– anions. The magnetic properties of 1 and 2 show that the weak ferromagnetic interactions occurred between Co II ions in 1 and a weak antiferromagnetic interactions exist between Mn II ions in 2 . These two complexes have good thermal stabilities.

Description: Three tungsten oxychloride clusters containing the nearly D 3 d symmetric [(W 6 O 6 i Cl 6 i )Cl 6 a ] n – ( n = 2, 3) core were prepared from the cluster acid (H 5 O 2 ) 2 [W 6 O 6 Cl 12 ] · 4H 2 O and structurally characterized by single-crystal X-ray diffraction. The copper compound [Cu(H 2 O) 4 ][W 6 O 6 Cl 12 ] · 12H 2 O releases water molecules to yield [Cu(H 2 O) 6 ][W 6 O 6 Cl 12 ]. Both compounds are represented as diamagnetic clusters, having 14 electrons in W–W bonding states. Magnetic measurements on the calcium compound [Ca(H 2 O) 7 ] 2 [W 6 O 6 Cl 12 ]Cl revealed a paramagnetic cluster having 15 valence electrons.

Description: Phase equilibrium in the Ca-Mn-Sb-O system was studied in air at the temperature range from 1160 to 1250 °C and a pseudo-quaternary phase diagram for the system CaO-MnO-Mn 2 O 3 -Sb 2 O 5 is presented. The following compounds were discovered: new antimonate Ca 7 Sb 2 O 12 with a perovskite-like structure, solid solutions Mn 2– x Ca x Sb 2 O 7 (0 ≤ x ≤ 1.6) with a 3 T -weberite structure, and Ca 2– x Mn x Sb 2 O 7 (0 ≤ x ≤ 0.23) with a 2 O -weberite structure, as well as solid solutions Ca 2 Mn 1+ x Sb 1– x O 6 with monoclinic (0 ≤ x ≤ 0.67) and orthorhombic (0.75 ≤ x ≤ 1) perovskite structures. The existence of a number of double and ternary oxides and solid solutions on the basis of Sb 5+ and Mn 2+ , Mn 3+ , Mn 4+ and with mixed manganese valence is confirmed.

Description: The reaction of LAlMe 2 ( 1 ) [L = HC(CMeNAr) 2 , Ar = 2,6- i Pr 2 C 6 H 3 ] with diphenylstannanediol resulted in the methylalumoxane compound L(Me)Al(μ-O)Al(Me)L ( 3 ). Compound (LAlO) 2 B(2, 6-OCH 3 C 6 H 4 )(μ-O) ( 4 ) containing the Al 2 BO 3 six-membered ring was accomplished by reacting the precursor LAlH 2 ( 2 ) with 2,6-dimethoxyphenylboronic acid. The two compounds were characterized by 1 H NMR spectroscopy, elemental analysis, and single-crystal X-ray structural analysis.

Description: A novel fairly stable N -trimethylsilylamino(dichloro)phosphine was prepared, in which the nitrogen atom bears a 9-borabicyclo[3.3.1]nonyl group. The gas phase structures of various amino- and silylaminophosphines including a phosphenium cation and an amino(imono)phosphine were optimized at the B3LYP/6-311+G(d, p) level of theory, and NMR parameters were calculated. Both magnitude and sign of the two-bond coupling constants 2 J ( 31 P, N, 13 C) and 2 J ( 31 P, N, 29 Si), known to be sensitive towards the respective conformation, are well reproduced by the calculations. This also holds for 1 J ( 31 P, 15 N), although calculated values 1 K ( 31 P, 15 N) (all 〈 0) are slightly more negative [ 1 J ( 31 P, 15 N) more positive] than experimental values.

Description: A new synthetic entry to iridium Keggin-type polyoxometalate complexes from [PW 11 O 39 ] 7– and K 3 [IrCl 6 ] under harsh conditions is reported. The complex [PW 11 O 39 IrCl] 5– ( 1 5– ) featuring an IrCl functionality was obtained in high yield and characterized by NMR spectroscopic and ESI-MS techniques. The presence of Li + (3–4 M) is essential for a quantitative yield of 1 5– . The reactivities of 1 5– and its rhodium analogue [PW 11 O 39 RhCl] 5– in ligand substitution at the noble metal site were studied. Thiocyanate coordination successfully yielded (Bu 4 N) 5 [PW 11 O 39 M (SCN)] [ M = Rh ( 2a ), Ir, ( 3a )]. In both cases, the SCN ligands are coordinated by sulfur atoms, according to 13 C NMR and IR spectroscopic data. Gas-phase fragmentation reactions of compounds 2a and 3a were also investigated by collision-induced dissociation (CID) experiments. Reaction of [PW 11 O 39 RhCl] 5– with NaN 3 resulted in Cl – to OH – replacement accompanied by the liberation of the RhCl fragment, whereas 1 5– proved unreactive with NaN 3 . Attempts to coordinate NO 2 – are adversely affected by competing noble metal excision with formation of free [PW 11 O 39 ] 7– .

Description: Four discrete metal-radical complexes, [Cu( p -MePh-COO) 2 (NITpPy) 2 ] ( 1 ), [Ni( m -MePhCOO) 2 (NITpPy) 2 (H 2 O) 2 ] · (CH 3 -OH) 2 ( 2 ), [Mn( p -MePhCOO) 2 (NITpPy) 2 (H 2 O) 2 ] ( 3 ), and [Mn( m -MePhCOO) 2 (NITpPy) 2 (H 2 O) 2 ] ( 4 ) [NITpPy = 2-(4-pyridyl)-4,4,5,5-tetramethyl-4,5-dihydro-1H-imidazolyl-1-oxyl-3-oxide] were synthesized and characterized by elemental analyses, IR spectroscopy, PXRD, single-crystal X-ray diffraction, and magnetic susceptibility. For the four complexes, the crystal structural analyses indicate that the two radical ligands coordinated to the metal ions by the nitrogen atoms of the pyridine rings form three spin complexes, where toluates act as co-ligands. Weak antiferromagnetic interactions [ J Cu–Rad = –6.75 cm –1 ( 1 ), J Co–Rad = –4.15 cm –1 ( 2 ), J Mn–Rad = –0.22 cm –1 ( 3 ), and J Mn–Rad = –3.74 cm –1 ( 4 )] were observed, spin polarization mechanism and orbital symmetry are used to explain the magnetic coupling in these complexes.

Description: The new ternary compounds UP 2 S 6 , UP 2 S 7 , U(P 2 S 6 ) 2 , and U 3 (PS 4 ) 4 were prepared from uranium metal, phosphorus pentasulfide, and sulfur at 700 °C. The crystal structures were determined by single-crystal X-ray diffraction methods. UP 2 S 6 ( I ) crystallizes in the ZrP 2 S 6 structure type [tetragonal, P 4 2 / m , a = 6.8058(7) Å, c = 9.7597(14) Å, Z = 2], which consists of central uranium(IV) atoms coordinated by P 2 S 6 4– anions (staggered conformation). The anions are two-dimensional connectors for four uranium cations arranged in one plane. The structure of UP 2 S 7 ( II ) [orthorhombic, Fddd , a = 8.9966(15) Å, b = 15.2869(2) Å, c = 30.3195(5) Å, Z = 16] is closely related to the monoclinic ZrP 2 S 7 structure type. It consists of U 4+ cations linked by P 2 S 7 4– ligands, the resulting 3D network contains large pores (diameter approx. 3.5 × 16.7 Å). In the previously reported compound U(P 2 S 6 ) 2 ( III ) [ I 4 1 / a , a = 12.8776(9) Å, c = 9.8367(10) Å, Z = 2], the metal atoms are coordinated by four bidentate P 2 S 6 2– ligands. This arrangement can be considered as a pseudotetrahedral coordination of the uranium atoms by the linear ligands. Three of the resulting diamondoid frameworks are inseparably interwoven in order to optimize space filling. U 3 (PS 4 ) 4 ( IV ) [ I 4 1 / acd , a = 10.7440(9) Å, c = 19.0969(2) Å, Z = 2] crystallizes in a defect variant of the PrPS 4 structure type, with 50 % of the U2 sites statistically occupied with uranium atoms. The resulting stoichiometry is U 3 (PS 4 ) 4 with tetravalent uranium atoms. The structure of U 3 (PS 4 ) 4 consists of uranium atoms connected by PS 4 3– groups, each PS 4 group linking four central uranium atoms. Vibrational spectra, which were recorded for I – III , show good agreement between the obtained results and the expected values for the anionic units, while magnetic measurements confirm the presence of tetravalent uranium.

Description: G-protein coupled receptors (GPCRs) are a large family of proteins that coordinate extracellular signals to produce physiologic outcomes. Adenosine receptors (AR) are one class of GPCRs that have been shown to regulate functions as diverse as inflammation, blood flow, and cellular differentiation. Adenosine signals through four GPCRs that either inhibit (A1AR and A3AR) or activate (A2aAR and A2bAR) adenylyl cyclase. This review will focus on the role of GPCRs, and in particular, adenosine receptors, in adipogenesis. Preadipocytes differentiate to mature adipocytes as the adipose tissue expands to compensate for the consumption of excess nutrients. These newly generated adipocytes contribute to maintaining metabolic homeostasis. Understanding the key drivers of this differentiation process can aid the development of therapeutics to combat the growing obesity epidemic and associated metabolic consequences. Although much literature has covered the transcriptional events that culminate in the formation of an adipocyte, less focus has been on receptor-mediated extracellular signals that direct this process. This review will highlight GPCRs and their downstream messengers as significant players controlling adipocyte differentiation. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: The Toll and Toll-Like Receptor signaling pathways are evolutionarily conserved pathways that regulate innate immunity in insects and mammals. While efforts have been made to clarify the signal transduction events that occur during infection, much less is known about the components that maintain immune quiescence. Here we show that retromer, an intracellular protein complex known for regulating vesicle trafficking, functions in modulating the Toll pathway in Drosophila melanogaster . In mutant animals lacking retromer function, the Toll pathway but not JAK-STAT or IMD pathway is activated, triggering both cellular and humoral responses. Genetic epistasis and clonal analysis suggest that retromer regulates a component that acts upstream of Toll. Our data further show that in the mutant the Toll ligand Spätzle has a processing pattern similar to that of after infection. Together, the results suggest a novel function of retromer in regulating Toll pathway and innate immunity at a step that modulates ligand processing or activity. J. Cell. Physiol. © 2013 Wiley Periodicals, Inc.

Description: 2-Pivaloylpterin, an acylated derivative of the biochemically relevant pterin [2-amino-4-oxo-(3 H )pteridine] heterocyclus, undergoes stepwise metallation by the 1, 1′-bis(diphenylphosphanyl)ferrocene-copper(I) cation, [(dppf)Cu] + . The final product obtained, [Cu 3 (dppf)(μ 2 -dppf)(PP)(PP-H + )] 2 (BF 4 ) 4 , could be structurally characterized to reveal coordinative saturation with binding of central Cu + ions to N 1 ,N 3 ,O 4 ,N 5 ,N 8 and pivaloyl-O donor atoms.

Description: Abstract . Two coordination polymers, namely, {[Cd(cdpc)(hmt)(H 2 O)] · H 2 O} n ( 1 ), and [Mn(Hcdpc) 2 (4, 4′-bpy)(H 2 O)] n ( 2 ), were constructed by synergistic assembly through the mixed-ligand synthetic strategy (H 2 cdpc = 1-carboxymethyl-3, 5-dimethyl-1H-pyrazole-4-carboxylic acid, hmt = hexamethylenetetramine, and 4, 4′-bpy = 4, 4′-dipyridine). Their structures were determined by single-crystal X-ray diffraction analyses and further characterized by elemental analyses, IR spectra, powder X-ray diffraction (PXRD), and thermogravimetric (TG) analyses. Single X-ray diffraction analysis reveals that complex 1 is a 2D 4-connected sql sheet, and complex 2 is an interesting 1D loop chain. The two complexes are further expanded to 3D supramolecular structure through non-covalent bonds. Besides, luminescent properties of two complexes in the solid state and magnetic property of 2 were also investigated.

Description: Similar to phosphorylation, transient conjugation of ubiquitin to target proteins (ubiquitination) mediated by the concerted action of ubiquitin ligases and de-ubiquitinating enzymes (DUBs) can affect substrate function. As obligate intracellular parasites, viruses rely on different cellular pathways for their own replication and the well conserved ubiquitin conjugating/de-conjugating system is not an exception. Viruses not only usurp the host proteins involved in the ubiquitination/de-ubiquitination process, but they also encode their own ubiquitin ligases and DUBs. Here we report that an N-terminal variant of the herpes simplex virus (HSV) type-1 large tegument protein VP1/2 (VP1/2 1–767 ), encompassing an active DUB domain (herpesvirus tegument ubiquitin specific protease, htUSP), and TSG101, a component of the endosomal sorting complex required for transport (ESCRT)-I, functionally interact. In particular, VP1/2 1–767 modulates TSG101 ubiquitination and influences its intracellular distribution. Given the role played by the ESCRT machinery in crucial steps of both cellular pathways and viral life cycle, the identification of TSG101 as a cellular target for the HSV-1 specific de-ubiquitinating enzyme contributes to the clarification of the still under debate function of viral encoded DUBs highly conserved throughout the Herpesviridae family. This article is protected by copyright. All rights reserved

Description: The chemical preparation, structure, luminescence, and electronic properties are given for a new potassium holmium cyclotetraphosphate KHoP 4 O 12 , a promising optics material for applications. Single-crystal X-ray diffraction analysis shows that the newly synthesized compound crystallizes in the monoclinic system with space group C 2/ c and Z = 4. [P 4 O 12 ] 4– anionic rings and HoO 8 polyhedra display a three-dimensional (3D) framework by corner-sharing. The ten-coordinated potassium atoms are located in the delimited tunnels. KHoP 4 O 12 exhibits the blue light emission under the excitation of 330 nm. To gain further insights into electronic properties of crystal KHoP 4 O 12 , theoretical calculation based on density functional theory (DFT) was performed using the total-energy code CASTEP with the LDA + U approach. The calculated bandgap with U = 3.0–3.5 eV is in good agreement with the experimental measurement.

Description: The transition to a pathological phenotype such as Barrett's esophagus occurs via induction of resistance upon repeated contact with gastric refluxate in esophagus. This study examined the molecular changes within normal esophageal epithelial cells (EECs) under short-term acid loading and the role of these changes in defensive resistance against acidic cytotoxicity. After primary cultured EECs were exposed to pH 4-acidified medium (AM4), cell viability was determined by the MTT assay. Reactive oxygen species (ROS) and NAD(P)H oxidase (NOX) activity were measured. Activation of the mitogen-activated protein kinases (MAPKs) MEK/ERK1/2, p38 and JNK; phosphoinositol-3-kinase (PI3K)/Akt, and nuclear factor-kappa B (NF-κB) were detected by Western blot analysis or immunofluorescence staining. AM4 incubation induced intracellular ROS generation accompanied by increase in NOX activity, which was further increased by Na + /H + exchange-1 (NHE1)-dependent inhibition but was prevented by inhibition of NOX or mitochondria complex I. AM4 also induced phosphorylation of MEK/ERK1/2, p38 MAPK, PI3K/Akt, and nuclear translocation of NF-κB, and all these effects, except for p38 MAPK phosphorylation, were abolished by inhibition of ROS. ROS-dependent PI3K/Akt activation, which mediates NF-κB nuclear translocation, was inhibited by protein tyrosine kinase (PTK) inhibitors and NHE1-specific inhibitor. All inhibitors of NHE, ROS, PTK, PI3K or NF-κB further decreased AM4-induced cell viability. Acid loading in the presence of NHE1-dependent protection induced ROS generation by activating NOX and mitochondria complex I, which stimulated PTK/PI3K/Akt/NF-κB-dependent survival in EEC. Our data indicate that normal EEC initially respond to acid loading through intrinsic survival activation. This article is protected by copyright. All rights reserved

Description: The facile synthesis, molecular structure, and reactivity of [Cu(C 7 H 7 NH 2 )Cl] 4 ( 1 ) towards dioxygen and derivatives is reported. The compound could easily be prepared in good yields by mixing CuCl and benzylamine under inert conditions in dichloromethane. Surprisingly this copper(I) compound, a copper(I) tetramer with Cu I ··· Cu I interactions of 2.89 Å, was formed instead of an expected cubane cluster. Oxidation reactions led to formation of μ-oxido-species as intermediates, however 1 did not show any catalytic activity in the activation of CH bonds. In contrast it turned out that 1 was quite stable towards oxidation. Analogous reactions with CuBr or CuI were different and neither cluster units or polynuclear copper(I) complexes were obtained.

Description: Osteolytic bone diseases are characterized by excessive osteoclast formation and activation. Protein kinase C (PKC)-dependent pathways regulate cell growth, differentiation and apoptosis in many cellular systems, and have been implicated in cancer development and osteoclast formation. A number of PKC inhibitors with anti-cancer properties have been developed, but whether they might also influence osteolysis (a common complication of bone invading cancers) is unclear. We studied the effects of the PKC inhibitor compound, GF109203X on osteoclast formation and activity, processes driven by receptor activator of NFκB ligand (RANKL). We found that GF109203X strongly and dose dependently suppresses osteoclastogenesis and osteoclast activity in RANKL-treated primary mouse bone marrow cells. Consistent with this GF109203X reduced expression of key osteoclastic genes, including cathepsin K, calcitonin receptor, tartrate resistant acid phosphatase (TRAP) and the proton pump subunit V-ATPase-d2 in RANKL-treated primary mouse bone marrow cells. Expression of these proteins is dependent upon RANKL-induced NF-κB and NFAT transcription factor actions; both were reduced in osteoclast progenitor populations by GF109203X treatment, notably NFATc1 levels. Furthermore, we showed that GF109203X inhibits RANKL-induced calcium oscillation. Together, this study shows GF109203X may block osteoclast functions, suggesting that pharmacological blockade of PKC-dependent pathways has therapeutic potential in osteolytic diseases. J. Cell. Physiol. © 2014 Wiley Periodicals, Inc.

Description: The sesquiterpene lactone Parthenolide (PN) exerted a cytotoxic effect on MDA-MB231 cells, a triple-negative breast cancer (TNBC) cell line, but its effectiveness was scarce when employed at low doses. This represents an obstacle for a therapeutic utilization of PN. In order to overcome this difficulty we associated to PN the suberoylanilide hydroxamic acid (SAHA), an histone deacetylase inhibitor. Our results show that SAHA synergistically sensitized MDA-MB231 cells to the cytotoxic effect of PN. It is noteworthy that treatment with PN alone stimulated the survival pathway Akt/mTOR and the consequent nuclear translocation of Nrf2, while treatment with SAHA alone induced autophagic activity. However when the cells were treated with SAHA/PN combination, SAHA suppressed PN effect on Akt/mTOR/Nrf2 pathway, while PN reduced the prosurvival autophagic activity of SAHA. In addition SAHA/PN combination induced GSH depletion, fall in Δψm, release of cytochrome c, activation of caspase 3 and apoptosis. Finally we demonstrated that combined treatment maintained both hyperacetylation of histones H3 and H4 induced by SAHA and down-regulation of DNMT1 expression induced by PN. Inhibition of the DNA-binding activity of NF-kB, which is determined by PN, was also observed after combined treatment. In conclusion, combination of PN to SAHA inhibits the cytoprotective responses induced by the single compounds, but does not alter the mechanisms leading to the cytotoxic effects. Taken together our results suggest that this combination could be a candidate for TNBC therapy. J. Cell. Physiol. © 2014 Wiley Periodicals, Inc.

Description: The effect of different factors, such as pH of the medium (1.5 〈 pH 〈 4.0; 1 × 10 –4 mol · L –1 〈 [SO 4 2– ] 〈 1 × 10 –1 mol · L –1 ), the concentration of extracting agent, temperature and the type of the solvent, on the extraction of vanadium(V) by trioctylamine was studied. It was shown that the extraction of vanadium(V) by trioctylamine at 25 ± 0.5 °C takes place in the pH range 2.0–3.5 and the extracting complex contains decavanadate anion H 2 V 10 O 28 4– and four molecules of the extracting agent. This allows the reaction of vanadium(V) extraction by trioctylamine to be described by the following equation: 2( R 3 NH) 2 SO 4 + H 2 V 10 O 28 4– ( R 3 NH) 4 H 2 V 10 O 28 + 2SO 4 . The effect of the length of the alkyl chain of alcohol (propyl, butyl, isododecyl alcohol) on the homogeneity of the system V V -TOA-toluene-alcohol was investigated. It was established that the solubility of the extracting complexes of vanadium(V) with trioctylamine can be increased by using isododecyl alcohol C 12 H 25 OH as a modifying agent. It was shown that under optimal conditions in the presence of isododecyl alcohol at temperatures above 25 °C in the pH interval 2.0–3.5 trioctylamine extracts vanadium(V) with a high distribution coefficient (lg D V V 〉 2).

Description: Genomic and trascriptomic profiling has recently contributed details to the characterization of luminal B breast cancer. We explored the contribution of anthropometric, metabolic and molecular determinants to the multifaceted heterogeneity of this breast cancer subtype, with a specific focus on the association between body mass index (BMI), pre-treatment fasting glucose, hormone receptors and expression of human epidermal growth factor receptor 2 (HER2). Extensively annotated specimens were obtained from 154 women with luminal B breast cancer diagnosed at two Italian comprehensive cancer centres. Participants' characteristics were descriptively analyzed overall and by HER2 status (positive vs negative). BMI (〈25 vs ≥25), pre-treatment fasting glucose (〈median value of 94 mg/dl vs ≥94) and percentage of hormone receptors were tested for association with HER2 expression in regression models. In univariate models, BMI, fasting glucose and, at a lesser extent, percentage of estrogen receptors (ER) were significantly and inversely associated with HER2 expression (OR: 0.32, 95%CI: 0.16-0.66; 0.43, 0.23-0.0.82; 0.96, 0.94-0.97, respectively). The multivariate models confirmed the protective role of BMI and ER on HER2 expression, with luminal B HER2 positive patients being significantly less frequent among women within the highest category of BMI and percentage expression of ER compared with their counterparts (OR: 0.22, 95%CI: 0.09-0.53; 0.95, 0.93-0.97). In conclusions, BMI and percentage of ER representation are inversely associated with HER2 expression in luminal B breast cancers. Upon confirmatory findings, this might help identify patient subgroups who may best benefit from the use of interventions targeting insulin resistance in well depicted breast cancer scenarios. This article is protected by copyright. All rights reserved

Description: Histone deacetylases (HDACs) play a crucial role in the regulation of gene expression through remodeling of chromatin structures. However, the molecular mechanisms involved in this event remain unknown. In this study, we sought to examine whether HDAC inhibition-mediated protective effects involved HDAC4 sumoylation, degradation, and the proteasome pathway. Isolated neonatal mouse ventricular myocytes (NMVM) and H9c2 cardiomyoblasts were subjected to 48 hours of hypoxia (H) (1% O 2 ) and 2 hours of reoxygenation (R). Treatment of cardiomyocytes with trichostatin A (TSA) attenuated H/R-elicited injury, as indicated by a reduction of lactate dehydrogenase (LDH) leakage, an increase in cell viability, and decrease in apoptotic positive cardiomyocytes. MG132, a potent proteasome pathway inhibitor, abrogated TSA-induced protective effects, which was associated with the accumulation of ubiquitinated HDAC4. NMVM transduced with adenoviral HDAC4 led to an exaggeration of H/R-induced injury. TSA treatment resulted in a decrease in HDAC4 in cardiomyocytes infected with adenoviral HDAC4, and HDAC4-induced injury was attenuated by TSA. HDAC inhibition resulted in a significant reduction in reactive oxygen species (ROS) in cardiomyoblasts exposed to H/R, which was attenuated by blockade of the proteasome pathway. Cardiomyoblasts carrying wild type and sumoylation mutation (K559R) were established to examine effects of HDAC4 sumoylation and ubiquitination on H/R injury. Disruption of HDAC4 sumoylation brought about HDAC4 accumulation and impairment of HDAC4 ubiquitination in association with enhanced susceptibility of cardiomyoblasts to H/R. Taken together, these results demonstrated that HDAC inhibition stimulates proteasome dependent degradation of HDAC4, which is associated with HDAC4 sumoylation to induce these protective effects. This article is protected by copyright. All rights reserved

Description: The lanthanide selenidogermanates [{Eu(en) 3 } 2 (μ-OH) 2 ]Ge 2 Se 6 ( 1 ), [{Ho(en) 3 } 2 (μ-OH) 2 ]Ge 2 Se 6 ( 2 ), and [{Ho(dien) 2 } 2 (μ-OH) 2 ]Ge 2 Se 6 ( 3 ) (en = ethylenediamine, dien = diethylenetriamine) were solvothermally prepared by the reactions of Eu 2 O 3 (or Ho 2 O 3 ), germanium, and selenium in en and dien solvents respectively. Compounds 1 – 3 are composed of selenidogermanate [Ge 2 Se 6 ] 4– anion and dinuclear lanthanide complex cation [{ Ln (en) 3 } 2 (μ-OH) 2 ] 4+ ( Ln = Eu, Ho) or [{Ho(dien) 2 } 2 (μ-OH) 2 ] 4+ . The [Ge 2 Se 6 ] 4– anion is composed of two GeSe 4 tetrahedra sharing a common edge. The dinuclear lanthanide complex cations are built up from two [ Ln (en) 3 ] 3+ or [Ho(dien) 2 ] 3+ ions joined by two μ-OH bridges. All lanthanide(III) ions are in eight-coordinate environments forming distorted bicapped trigonal prisms. In 1 – 3 , three-dimensional supramolecular networks of the anions and cations are formed by N–H ··· Se and N–H ··· O hydrogen bonds. To the best of our knowledge, 1 – 3 are the first examples of selenidogermanate salts with lanthanide complex counter cations.

Description: Density functional theory calculations using the BP86 functional in combination with triple-ζ quality basis sets have been carried out for the “early-late” transition metal complexes Cl 3 M – M ′(PCl 3 ) 4 ( M = Ti, Zr, Hf; M ′ = Co, Rh, Ir) and the derivatives R 3 M – M ′L 4 ( R = Cl, NH 2 ; L = PCl 3 , PH 3 , CO). The calculations demonstrate that the metal–metal bond strength in R 3 M – M ′L 4 can be strongly influenced by the nature of the ligands R and L. The intrinsic interaction energy Δ E int and the bond dissociation energy of the M – M ′ bonds in Cl 3 M – M ′(PCl 3 ) 4 are much smaller than in the previously investigated species (H 2 N) 3 M – M ′(CO) 4 . The M – M ′ bonds become stronger in both sets of compounds when the metal atoms become heavier. The equilibrium geometries of Cl 3 M – M ′(PCl 3 ) 4 which have bipyramidal structures have C 3 symmetry. The M –Co bonds in Cl 3 Zr–Co(PCl 3 ) 4 and Cl 3 Hf–Co(PCl 3 ) 4 and to a lesser degree in Cl 3 Ti–Co(PCl 3 ) 4 are unusually long because of direct interactions between the equatorial PCl 3 groups and the group 4 atoms Zr, Hf. The analysis of the metal–metal interactions suggests that Cl 3 M – M ′(PCl 3 ) 4 has M – M ′ single bonds.