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Structural disorder and transformation in crystal growth: direct observation of ring-opening isomerization in a metal–organic solid solution (2015)

Jiang, J.-J.He, J.-R.Lü, X.-Q.Wang, D.-W.Li, G.-B.Su, C.-Y.

International Union of Crystallography (IUCr)

In: IUCrJ

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Publication Date: 2015-08-16

Description: A rare example is reported in which discrete Ag2L2 ring and (AgL)∞ chain motifs [L = N,N′-bis(3-imidazol-1-yl-propyl)-pyromellitic diimide] co-crystallize in the same crystal lattice with varying ratios and degrees of disorder. Crystal structures obtained from representative crystals reveal compatible packing arrangements of the cyclic and polymeric isomers within the crystal lattice, which enables them to co-exist within a crystalline solid solution. A feasible pathway for transformation between the isomers is suggested via facile rotation of the coordinating imidazolyl groups. This chemical system could provide a chance for direct observation of ring-opening isomerization at the crystal surface. Mass spectrometry and 1H NMR titration show a dynamic equilibrium between cyclic and oligomeric species in solution, and a potential crystallization process is suggested involving alignment of precursors directed by aromatic stacking interactions between pyromellitic diimide units, followed by ring-opening isomerization at the interface between the solid and the solution. Both cyclic and oligomeric species can act as precursors, with interconversion between them being facile due to a low energy barrier for rotation of the imidazole rings. Thermogravimetric analysis and variable-temperature powder X-ray diffraction indicate a transition to a different crystalline phase around 120°C, which is associated with loss of solvent from the crystal lattice.

Keywords: crystallizationstructural transformationring-opening isomerismsolid solutiondisorder

Electronic ISSN: 2052-2525

Topics: Geosciences , Physics

Published by International Union of Crystallography (IUCr)

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Charge-transport properties of 4-(1,2,2-triphenylvinyl)aniline salicylaldehyde hydrazone: tight-packing induced molecular `hardening' (2017)

Ma, H.Chai, S.Chen, D.Huang, J.-D.

International Union of Crystallography (IUCr)

In: IUCrJ

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Publication Date: 2017-09-02

Description: Based on first-principles calculations, the relationship between molecular packing and charge-transport parameters has been investigated and analysed in detail. It is found that the crystal packing forces in the flexible organic molecule 4-(1,2,2-triphenylvinyl)aniline salicylaldehyde hydrazone (A) can apparently overcome the dynamic intramolecular rotations and the intramolecular steric repulsion, effectively enhancing the molecular rigidity and decreasing the internal reorganization energy. The conducting properties of A have also been simulated within the framework of hopping models, and the calculation results show that the intrinsic electron mobility in A is much higher than the corresponding intrinsic hole mobility. These theoretical investigations provide guidance for the efficient and targeted control of the molecular packing and charge-transport properties of organic small-molecule semiconductors and conjugated polymeric materials.

Keywords: mobilityreorganization energypacking forcesrigidityflexible moleculescharge-transport properties

Electronic ISSN: 2052-2525

Topics: Geosciences , Physics

Published by International Union of Crystallography (IUCr)

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The mechanism behind the selection of two different cleavage sites in NAG-NAM polymers (2017)

Mihelič, M.Vlahoviček-Kahlina, K.Renko, M.Mesnage, S.Doberšek, A.Taler-Verčič, A.Jakas, A.Turk, D.

International Union of Crystallography (IUCr)

In: IUCrJ

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Publication Date: 2017-02-24

Description: Peptidoglycan is a giant molecule that forms the cell wall that surrounds bacterial cells. It is composed of alternating N-acetylglucosamine (NAG) and N-acetylmuramic acid (NAM) residues connected by β-(1,4)-glycosidic bonds and cross-linked with short polypeptide chains. Owing to the increasing antibiotic resistance against drugs targeting peptidoglycan synthesis, studies of enzymes involved in the degradation of peptidoglycan, such as N-acetylglucosaminidases, may expose new, valuable drug targets. The scientific challenge addressed here is how lysozymes, muramidases which are likely to be the most studied enzymes ever, and bacterial N-acetylglucosaminidases discriminate between two glycosidic bonds that are different in sequence yet chemically equivalent in the same NAG-NAM polymers. In spite of more than fifty years of structural studies of lysozyme, it is still not known how the enzyme selects the bond to be cleaved. Using macromolecular crystallography, chemical synthesis and molecular modelling, this study explains how these two groups of enzymes based on an equivalent structural core exhibit a difference in selectivity. The crystal structures of Staphylococcus aureus N-acetylglucosaminidase autolysin E (AtlE) alone and in complex with fragments of peptidoglycan revealed that N-acetylglucosaminidases and muramidases approach the substrate at alternate glycosidic bond positions from opposite sides. The recognition pocket for NAM residues in the active site of N-acetylglucosaminidases may make them a suitable drug target.

Keywords: Staphylococcus aureusautolysinssubstrate specificityN-acetylglucosaminidasemuramidaseslysozyme

Electronic ISSN: 2052-2525

Topics: Geosciences , Physics

Published by International Union of Crystallography (IUCr)

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