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  • 1
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    Deconstructing Martial Arts (2021)
    Cardiff University Press
    Details
    Publication Date: 2024-03-28
    Description: "What is the essence of martial arts? What is their place in or relationship with culture and society? Deconstructing Martial Arts analyses familiar issues and debates that arise in scholarly, practitioner and popular cultural discussions and treatments of martial arts and argues that martial arts are dynamic and variable constructs whose meanings and values regularly shift, mutate and transform, depending on the context. It argues that deconstructing martial arts is an invaluable approach to both the scholarly study of martial arts in culture and society and also to wider understandings of what and why martial arts are. Placing martial arts in relation to core questions and concerns of media and cultural studies around identity, value, orientalism, and embodiment, Deconstructing Martial Arts introduces and elaborates deconstruction as a rewarding method of cultural studies."
    Keywords: Martial Arts ; Deconstruction ; Embodiment ; Ideology ; Culture ; Knowledge ; thema EDItEUR::G Reference, Information and Interdisciplinary subjects::GT Interdisciplinary studies::GTD Semiotics / semiology ; thema EDItEUR::Q Philosophy and Religion::QD Philosophy::QDT Topics in philosophy::QDTS Social and political philosophy ; thema EDItEUR::Q Philosophy and Religion::QD Philosophy::QDX Popular philosophy ; thema EDItEUR::Q Philosophy and Religion::QR Religion and beliefs::QRY Alternative belief systems ; thema EDItEUR::J Society and Social Sciences::JB Society and culture: general::JBC Cultural and media studies::JBCC Cultural studies ; thema EDItEUR::J Society and Social Sciences::JB Society and culture: general::JBC Cultural and media studies::JBCC Cultural studies::JBCC1 Popular culture ; thema EDItEUR::G Reference, Information and Interdisciplinary subjects::GT Interdisciplinary studies::GTD Semiotics / semiology ; thema EDItEUR::Q Philosophy and Religion::QD Philosophy::QDT Topics in philosophy::QDTS Social and political philosophy ; thema EDItEUR::Q Philosophy and Religion::QD Philosophy::QDX Popular philosophy ; thema EDItEUR::Q Philosophy and Religion::QR Religion and beliefs::QRY Alternative belief systems ; thema EDItEUR::J Society and Social Sciences::JB Society and culture: general::JBC Cultural and media studies::JBCC Cultural studies ; thema EDItEUR::J Society and Social Sciences::JB Society and culture: general::JBC Cultural and media studies::JBCC Cultural studies::JBCC1 Popular culture
    Language: English
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    Format: image/jpeg
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  • 2
    Electronic Resource
    Electronic Resource
    THE EFFECT OF ORGANIC BASES UPON THE EXTENT AND MECHANISM OF THE REDUCING ACTION OF SODIUM METHYLATE ON NITROBENZENE AND AZOXYBENZENE1 (1930)
    s.l. : American Chemical Society
    Journal of the American Chemical Society 52 (1930), S. 1531-1536 
    Details
    ISSN: 1520-5126
    Source: ACS Legacy Archives
    Topics: Chemistry and Pharmacology
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1021/ja01367a036
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    Paper (German National Licenses)
    Fulltext
  • 3
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    THE EFFECT OF ORGANIC BASES UPON THE EXTENT AND MECHANISM OF THE REDUCING ACTION OF SODIUM METHYLATE ON NITROBENZENE AND AZOXYBENZENE1 (1930)
    American Chemical Society
    Details
    Publication Date: 1930-04-01
    Print ISSN: 0002-7863
    Electronic ISSN: 1520-5126
    Topics: Chemistry and Pharmacology
    Published by American Chemical Society
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  • 4
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    A test of somatic mosaicism in the androgen receptor gene of Canada lynx ( Lynx canadensis ) (2015)
    BioMed Central
    Details
    Publication Date: 2015-10-27
    Description: Background: The androgen receptor, an X-linked gene, has been widely studied in human populations because it contains highly polymorphic trinucleotide repeat motifs that have been associated with a number of adverse human health and behavioral effects. A previous study on the androgen receptor gene in carnivores reported somatic mosaicism in the tissues of a number of species including Eurasian lynx (Lynx lynx). We investigated this claim in a closely related species, Canada lynx (Lynx canadensis). The presence of somatic mosaicism in lynx tissues could have implications for the future study of exonic trinucleotide repeats in landscape genomic studies, in which the accurate reporting of genotypes would be highly problematic. Methods: To determine whether mosaicism occurs in Canada lynx, two lynx individuals were sampled for a variety of tissue types (lynx 1) and tissue locations (lynx 1 and 2), and 1,672 individuals of known sex were genotyped to further rule out mosaicism. Results: We found no evidence of mosaicism in tissues from the two necropsied individuals, or any of our genotyped samples. Conclusions: Our results indicate that mosaicism does not manifest in Canada lynx. Therefore, the use of hide samples for further work involving trinucleotide repeat polymorphisms in Canada lynx is warranted.
    Electronic ISSN: 1471-2156
    Topics: Biology
    Published by BioMed Central
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  • 5
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    The value of RFID for RTI management (2009)
    Springer
    Details
    Publication Date: 2009-07-08
    Print ISSN: 1019-6781
    Electronic ISSN: 1422-8890
    Topics: Computer Science , Economics
    Published by Springer
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  • 6
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    Molecular Classifiers for Prediction of Minimal Residual Disease (MRD) and Event Free Survival (EFS) Improve Risk Assignment at Diagnosis in Pediatric High-Risk B Precursor Acute Lymphoblastic Leukemia (ALL): A Children’s Oncology Group Study. (2007)
    American Society of Hematology
    Details
    Publication Date: 2007-11-16
    Description: Gene expression profiling has significant potential to improve risk classification and therapeutic targeting in ALL. Our goal is to develop molecular classifiers that more reliably predict relapse or resistance to current treatment regimens in order to identify patients who may benefit from therapeutic intensification or experimental approaches. COG P9906, testing an augmented BFM regimen, enrolled 271 patients with B precursor ALL with NCI high risk features (older age/higher WBC) who had experienced very poor outcomes (45% EFS) on prior trials. Patients with favorable (trisomy 4+10/TEL-AML1) or very unfavorable (Ph+/hypodiploidy) genetics were excluded. Expression profiles (Affymetrix HG_U133Plus2) were obtained from pre-treatment leukemic blasts in 207/271 (76%) children on COG P9906; these 207 cases were representative of the overall cohort. EFS at 4 yrs was 61% and flow cytometric measures of MRD (flow MRD) at end-induction (day 28) were highly predictive of outcome. Using expression profiles, a molecular classifier predictive of EFS was modeled using a Cox regression-based supervised principal components analysis and modified score test with extensive nested cross validation. A 42 gene molecular classifier predictive of EFS differentiated this cohort into a low (4 yr EFS: 81%, n=109) and high (4 yr EFS: 50%, n=98) molecular risk group (log rank test, P〈 0.0001). In multivariate analysis, the molecular risk classifier (MRC) retained prognostic significance (likelihood ratio test, p=0.0001) when adjusted for flow MRD and WBC. The best predictive model for EFS resulted when the MRC was combined with flow MRD; the resulting low (MRC low risk, MRD-; 87% EFS), medium (MRC low risk, MRD+ or MRC high risk, MRD-; 62% EFS), and high risk (MRC high risk, MRD+; 29% EFS) groups had significant outcome differences (Fig. A). As one must wait until the end of induction to obtain flow MRD to apply the combined classifier, we next determined if we could develop a molecular classifier to predict end-induction MRD in pre-treatment samples. Using a modified t-test and diagonal linear discriminant analysis with extensive cross validation, we derived a 23 gene molecular classifier predictive of end-induction MRD (ROC Accuracy: 0.80; p
    Print ISSN: 0006-4971
    Electronic ISSN: 1528-0020
    Topics: Biology , Medicine
    Published by American Society of Hematology
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  • 7
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    Pharmacogenetics of Minimal Residual Disease Response in Children with Acute Lymphoblastic Leukemia (ALL). (2004)
    American Society of Hematology
    Details
    Publication Date: 2004-11-16
    Description: The presence of minimal residual disease (MRD) as a marker of antileukemic drug efficacy is being used to assess risk status and, in some cases, to adjust the intensity of therapy. Within known prognostic categories, the determinants of MRD are not yet known. Specific host germline pharmacogenetic polymorphisms have been linked to event-free survival in ALL in some studies, but their relationship to level of MRD after remission induction therapy has not been clearly elucidated. Herein, we determined whether the presence of MRD in bone marrow, measured by flow cytometry at day 8 and day 28 of remission induction therapy in over 1,000 children enrolled on Pediatric Oncology Group anti-metabolite based therapy protocols 9904, 9905, and 9906 was related to the following germline polymorphisms: MTHFR (A1298G, n=1413 and C677T, n=334), NQO1 (n=334), GSTP1 (n=334), TYMS (n=309), ADRB2 (n=715), RFC 80A/G (n=578), VDR (n=714), MDR1 C3435T (n=333), and MDR1 G2677T/A (n=328). We found that, after adjustment for ploidy, race and TEL-AML1 status (believed to influence blast clearance) the level of MRD at day 28 differed significantly by MTHFR A1298C genotype (p=0.005). MRD was detected in 31%, and 19% of those with A/A or A/C versus CC genotypes, respectively. Similarly, after adjustment for ploidy, race and TEL-AML1 status the level of MRD at day 28 differed by MDR1 2677 genotype (p=0.02). MRD was detected in 39% and 25% of those with GG versus other MDR1 2677 genotypes, respectively. MTHFR C677T, NQO1, GSTP1, TYMS, ADRB2, RFC, and MDR1 G2677T genotypes were not associated with presence of MRD. There was a trend towards an association between VDR genotype and presence of MRD. No significant associations were detected between any pharmacogenetic genotype and MRD at day 8. Comment: These data indicate that presence of minimal residual disease at the end of induction, a known adverse risk factor in ALL, is importantly influenced by pharmacogenetic polymorphism. The strong association with MTHFR genotype, before the use of significant doses of methotrexate, illustrates the key role of folate in ALL blast metabolism. These data also indicate the value of an early endpoint such as MRD in identifying pharmacogenetic variables likely to influence outcome of specific therapeutic regimens, allowing prompt development of relevent mechanistic studies. Additional analyses will determine the impact of these polymorphisms on overall survival when the clinical outcome data from these studies is mature.
    Print ISSN: 0006-4971
    Electronic ISSN: 1528-0020
    Topics: Biology , Medicine
    Published by American Society of Hematology
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  • 8
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    Tyrosine kinome sequencing of pediatric acute lymphoblastic leukemia: a report from the Children's Oncology Group TARGET Project (2013)
    American Society of Hematology
    Details
    Publication Date: 2013-01-17
    Description: One recently identified subtype of pediatric B-precursor acute lymphoblastic leukemia (ALL) has been termed BCR-ABL1–like or Ph-like because of similarity of the gene expression profile to BCR-ABL1 positive ALL suggesting the presence of lesions activating tyrosine kinases, frequent alteration of IKZF1, and poor outcome. Prior studies demonstrated that approximately half of these patients had genomic lesions leading to CRLF2 overexpression, with half of such cases harboring somatic mutations in the Janus kinases JAK1 and JAK2. To determine whether mutations in other tyrosine kinases might also occur in ALL, we sequenced the tyrosine kinome and downstream signaling genes in 45 high-risk pediatric ALL cases with either a Ph-like gene expression profile or other alterations suggestive of activated kinase signaling. Aside from JAK mutations and 1 FLT3 mutation, no somatic mutations were found in any other tyrosine kinases, suggesting that alternative mechanisms are responsible for activated kinase signaling in high-risk ALL.
    Print ISSN: 0006-4971
    Electronic ISSN: 1528-0020
    Topics: Biology , Medicine
    Published by American Society of Hematology
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  • 9
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    Delayed Intensification (DI) Enhances Event-Free Survival (EFS) of Children with B-Precursor Acute Lymphoblastic Leukemia (ALL) Who Received Intensification Therapy with Six Courses of Intravenous Methotrexate (MTX): POG 9904/9905: A Childrens Oncology Group Study (COG). (2007)
    American Society of Hematology
    Details
    Publication Date: 2007-11-16
    Description: Post-induction (ind) intensification with non-anti-metabolite based blocks of therapy, improved EFS on BFM 76/79, CCG 105 and UKALL X. The DI phase of reinduction-reconsolidation (BFM protocol II) was a major component of these strategies. An anti-metabolite based (MTX/mercaptopurine [MP]) intensification also improved EFS (POG 9005/9006). COG 9904 and 9905 addressed whether addition of DI improved EFS for a subset of lower, standard (std) and a subset of NCI high risk (HR) pts who all received 6 courses (cs) of IV MTX (1 gm/m2/24 hrs vs 2 gm/m2/4 hrs) plus oral MP as intensification. The results of the MTX randomization (4 vs 24 hrs) are still blinded. Ind was a dexamethasone (dex)-based 3-drug (NCI std risk) or prednisone-based 4-drug (NCI HR or std with extramedullary disease) regimen. The 3-drug ind was modified because of excessive mortality with the intrathecal (IT) MTX on day 1 changed to IT Ara-C and 6 doses of native asparaginase (asp) (10,000 IU/m2) replaced with 1 dose of PEG asp. 1124 pts were treated pre-; 477 post-amendment. Post-ind, NCI std risk pts with trisomies of chromosomes 4 and 10 or a TELAML1 (TEL) translocation were classified as lower risk and enrolled on 9904. Only the TEL pts participated in the DI randomization. Std risk pts without and HR pts with favorable blast cytogenetics, or pts who did not meet refined NCI high risk age and WBC criteria were eligible for 9905. Pts with CNS3 disease, t(9;22), t(4;11), or hypodiploidy were excluded from both studies. Consolidation on 9904/9905 included 6 cs of IV MTX with leucovorin rescue for all pts. DI began at wk 16 after the 3rd course of IV MTX and was delivered over 8 wks: 1.5 mg/m2 vincristine and 30 mg/m2 daunomycin (wks 1, 2 and 3), daily dex (6 mg/m2 × 21 days), 2500 IU/m2 PEG asp (wk 1), age adjusted IT MTX (wks 1, 5, 6), 75 mg/m2 Ara-C (IV /SC) daily × 4 days (wks 5 and 6), 1 gm/m2 cyclophosphamide (wk 5) and 60 mg/m2 6-thioguanine daily × 14 doses (wks 6–7). A total of 1403 patients were randomized to +/− DI between April 7, 2000 and April 15, 2005. There were only 2 remission deaths; 1 each in +/− DI arms. There was a statistically significant improvement in EFS for all pts receiving the DI, with no statistically significant interaction (size of treatment differences in 4 yr EFS) between any pair of subsets. The difference, though not significant (study not powered to look at subsets), for the 9905 NCI HR pts with and without favorable cytogenetics, was in the same direction as the overall results, but still suboptimal with EFS below 80%. This may reflect differences between the dex and anthracycline used during the DI phase in this study versus BFM 76/69 and CCG 105 and/or the need for an intervention other than this DI in NCI HR patients. No DI DI Cohort 4 yr EFS N 4 yr EFS N 1 sided p-value* *p-values are by the logrank test Overall (9904/9905 NCI Std & High Risk) 81.6±2.0% 710 86.5±1.7% 693 0.0049 9904/9905 NCI Standard Risk 84.5±2.1% 517 90.3±1.7% 512 0.0012 9904 NCI Std Risk with TELAML1 91.1±2.6% 217 93.6±2.2% 216 0.0900 9905 NCI Std Risk 79.8±3.2% 300 87.9±2.5% 296 0.0027 9905 NCI HR 74.3±4.3% 93 76.2±4.5% 181 0.3839
    Print ISSN: 0006-4971
    Electronic ISSN: 1528-0020
    Topics: Biology , Medicine
    Published by American Society of Hematology
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  • 10
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    Expression Profiling Identifies Novel Genetic Subgroups with Distinct Clinical Features and Outcome in High-Risk Pediatric Precursor B Acute Lymphoblastic Leukemia (B-ALL). A Children’s Oncology Group Study. (2007)
    American Society of Hematology
    Details
    Publication Date: 2007-11-16
    Description: While 80% of children with B-ALL achieve long term survival, a significant number still relapse. In contrast to low and intermediate risk ALL, the biologic and genetic features of high risk disease have not been well characterized. COG P9906, testing an augmented BFM regimen, enrolled 271 B-ALL patients from 2000–2003 who were predicted to have poor outcomes based on prior trials. To study the heterogeneity of high risk B-ALL and to identify novel therapeutic targets, we obtained gene expression profiles (Affymetrix HG-U133Plus2) from the pre-treatment samples of 207/271 children on COG P9906. This cohort had a mean age of 10.9 yrs, a male predominance (66%), and a 4 year event free survival (EFS) of 61%. Patients with favorable (TEL-AML/trisomy 4+10) or very unfavorable (BCR-ABL/hypodiploidy) genetic features were excluded. While the cohort contained 20 cases with MLL rearrangements and 23 with E2A-PBX, the remainder had no known recurring genetic abnormalities. Using two unsupervised clustering methods (VxInsight, Hierarchical Clustering), an established method to identify outlier genes (COPA), and a novel method we developed to find genes tightly associated with recurring genetic abnormalities (ROSE), we identified 7 distinct cluster groups. Two of these clusters contained the MLL and E2A-PBX cases, while a third had cases with expression profiles similar to E2A-PBX but lacked the fusion transcript. Four clusters were completely novel and two of these were further distinguished by unique clinical and outcome features (see Fig.). One novel cluster (MC5) had strikingly favorable EFS (94.7% at 4 yrs.) with older children (mean age 14.1 yr) who were predominantly male (4:1). Highly expressed genes distinguishing this cluster included BRDG1, CABLES1, CENTG2, CHST2, MCAM and PTPRM. This cluster is very similar to the novel cluster previously described by Yeoh et al. (Cancer Cell, 1:133, 2002). A second novel cluster (MC4) had the most unfavorable outcome, with a 4 year EFS of only 21.0%. MC4 cases were notable for the highest mean WBC (196.7K/μL) and a preponderance of Hispanic children (p=0.002), known to have poorer responses to established therapies. Highly expressed genes in MC4 which may represent novel diagnostic and therapeutic targets include CRLF2, GPR110, IFITM1, MUC4 and TNFSF4. Many of these genes have been associated with an adverse response in solid tumors. As part of the NCI TARGET Project, in collaboration with St. Jude Children’s Research Hospital, genome wide copy number changes are being integrated with expression data to identify the initiating genetic lesions in these novel clusters. Gene expression profiling is highly useful in resolving the genetic heterogeneity of high risk ALL and in identifying novel therapeutic targets for this resistant disease. Figure Figure
    Print ISSN: 0006-4971
    Electronic ISSN: 1528-0020
    Topics: Biology , Medicine
    Published by American Society of Hematology
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