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Experimental determination of the instrumental transparency function of texture goniometers (2000)

Moras, K. ; Fischer, A. H. ; Klein, H. ; [et al.]

Copenhagen : International Union of Crystallography (IUCr)

Applied crystallography online 33 (2000), S. 1162-1174

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ISSN: 1600-5767

Source: Crystallography Journals Online : IUCR Backfile Archive 1948-2001

Topics: Geosciences , Physics

Notes: The instrumental transparency functions of five commercially available texture goniometers were measured experimentally with six monocrystalline samples cut in different orientations from a large highly perfect silicon crystal with a rocking curve of less than 0.01°. Transparency functions were measured in steps of 0.02 to 0.2° in the pole-figure angles α, β. The window size Δα depends on the Bragg angle θ in the form 1/sinθ; the window size Δω is constant for each goniometer. The dominant instrumental parameter determining the long axis Δα of the pole-figure window is the axial width of the detector entrance slit. This parameter is smallest for area detectors (smaller by more than an order of magnitude compared with conventional scintillation detectors as well as one-dimensional position-sensitive detectors). The main features of the pole-figure window and their dependence on the instrumental parameters can be deduced fairly well from a simple geometrical model. The particular shapes of the transparency functions of the studied goniometers are markedly different. Particularly, they are not very well represented by Gauss functions. The two-dimensional transparency function can be fairly well characterized by its α and β profiles. The normalized profiles are virtually independent of the goniometer angles 2θ and α. The increasing size of the pole-figure window with decreasing θ puts a lower limit on the Bragg angle below which pole-figure measurement ceases to be meaningful.

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1107/S0021889800007251

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2

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Structure of dichlorobis(trimethylphosphine oxide)cobalt(II) (1989)

Menu, M. J. ; Simard, M. ; Beauchamp, A. L. ; [et al.]

Oxford [u.a.] : International Union of Crystallography (IUCr)

Acta crystallographica 45 (1989), S. 1697-1699

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ISSN: 1600-5759

Source: Crystallography Journals Online : IUCR Backfile Archive 1948-2001

Topics: Chemistry and Pharmacology , Geosciences , Physics

Type of Medium: Electronic Resource

URL: http://dx.doi.org/10.1107/S0108270189003598

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An evaluation of methods to test predefined genomic regions for differential methylation in bisulfite sequencing data (2016)

Klein, H.-U., Hebestreit, K.

Oxford University Press

In: Briefings in Bioinformatics

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Publication Date: 2016-09-17

Description: In the biology of tissue development and diseases, DNA methylation plays an important role. For a deeper understanding, it is crucial to accurately compare DNA methylation patterns between groups of samples representing different conditions. A widely used method to investigate DNA methylation in the CpG context is bisulfite sequencing, which produces data on the single-nucleotide scale. While there are benefits to analyzing CpG sites on a basepair level, there are both biological and statistical reasons to test entire genomic regions for differential methylation. However, the analysis of DNA methylation is hampered by the lack of best practice standards. Here, we compared multiple approaches for testing predefined genomic regions for differential DNA methylation in bisulfite sequencing data. Nine methods were evaluated: BiSeq, COHCAP, Goeman's Global Test, Limma, methylKit/eDMR, RADMeth and three log-linear regression approaches with different distribution assumptions. We applied these methods to simulated data and determined their sensitivity and specificity. This revealed performance differences, which were also seen when applied to real data. Methods that first test single CpG sites and then test regions based on transformed CpG-wise P -values performed better than methods that summarize methylation levels or raw reads. Interestingly, smoothing of methylation levels had a negligible impact. In particular, Global Test, BiSeq and RADMeth/ z -test outperformed the other methods we evaluated, providing valuable guidance for more accurate analysis of DNA methylation.

Print ISSN: 1467-5463

Electronic ISSN: 1477-4054

Topics: Biology , Computer Science

Published by Oxford University Press

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Rad52 SUMOylation affects the efficiency of the DNA repair (2012)

Altmannova, V., Eckert-Boulet, N., Arneric, M., Kolesar, P., Chaloupkova, R., Damborsky, J., Sung, P., Zhao, X., Lisby, M., Krejci, L., Colavito, S., Macris-Kiss, M., Seong, C., Gleeson, O., Greene, E. C., Klein, H. L., Krejci, L., Sung, P.

Oxford University Press

In: Nucleic Acids Research

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Publication Date: 2012-04-24

Print ISSN: 0305-1048

Electronic ISSN: 1362-4962

Topics: Biology

Published by Oxford University Press

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Integrative analysis of histone ChIP-seq and transcription data using Bayesian mixture models (2014)

Klein, H.-U., Schafer, M., Porse, B. T., Hasemann, M. S., Ickstadt, K., Dugas, M.

Oxford University Press

In: Bioinformatics

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Publication Date: 2014-04-11

Description: Motivation: Histone modifications are a key epigenetic mechanism to activate or repress the transcription of genes. Datasets of matched transcription data and histone modification data obtained by ChIP-seq exist, but methods for integrative analysis of both data types are still rare. Here, we present a novel bioinformatics approach to detect genes that show different transcript abundances between two conditions putatively caused by alterations in histone modification. Results: We introduce a correlation measure for integrative analysis of ChIP-seq and gene transcription data measured by RNA sequencing or microarrays and demonstrate that a proper normalization of ChIP-seq data is crucial. We suggest applying Bayesian mixture models of different types of distributions to further study the distribution of the correlation measure. The implicit classification of the mixture models is used to detect genes with differences between two conditions in both gene transcription and histone modification. The method is applied to different datasets, and its superiority to a naive separate analysis of both data types is demonstrated. Availability and implementation: R/Bioconductor package epigenomix. Contact: h.klein@uni-muenster.de Supplementary information: Supplementary data are available at Bioinformatics online.

Print ISSN: 1367-4803

Electronic ISSN: 1460-2059

Topics: Biology , Computer Science , Medicine

Published by Oxford University Press

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How the misincorporation of ribonucleotides into genomic DNA can be both harmful and helpful to cells (2014)

Potenski, C. J., Klein, H. L.

Oxford University Press

In: Nucleic Acids Research

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Publication Date: 2014-09-17

Description: Ribonucleotides are misincorporated into replicating DNA due to the similarity of deoxyribonucleotides and ribonucleotides, the high concentration of ribonucleotides in the nucleus and the imperfect accuracy of replicative DNA polymerases in choosing the base with the correct sugar. Embedded ribonucleotides change certain properties of the DNA and can interfere with normal DNA transactions. Therefore, misincorporated ribonucleotides are targeted by the cell for removal. Failure to remove ribonucleotides from DNA results in an increase in genome instability, a phenomenon that has been characterized in various systems using multiple assays. Recently, however, another side to ribonucleotide misincorporation has emerged, where there is evidence for a functional role of misinserted ribonucleotides in DNA, leading to beneficial consequences for the cell. This review examines examples of both positive and negative effects of genomic ribonucleotide misincorporation in various organisms, aiming to highlight the diversity and the utility of this common replication variation.

Print ISSN: 0305-1048

Electronic ISSN: 1362-4962

Topics: Biology

Published by Oxford University Press

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Cancer gene prioritization by integrative analysis of mRNA expression and DNA copy number data: a comparative review (2013)

Lahti, L., Schafer, M., Klein, H.-U., Bicciato, S., Dugas, M.

Oxford University Press

In: Briefings in Bioinformatics

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Publication Date: 2013-01-19

Description: A variety of genome-wide profiling techniques are available to investigate complementary aspects of genome structure and function. Integrative analysis of heterogeneous data sources can reveal higher level interactions that cannot be detected based on individual observations. A standard integration task in cancer studies is to identify altered genomic regions that induce changes in the expression of the associated genes based on joint analysis of genome-wide gene expression and copy number profiling measurements. In this review, we highlight common approaches to genomic data integration and provide a transparent benchmarking procedure to quantitatively compare method performances in cancer gene prioritization. Algorithms, data sets and benchmarking results are available at http://intcomp.r-forge.r-project.org .

Print ISSN: 1467-5463

Electronic ISSN: 1477-4054

Topics: Biology , Computer Science

Published by Oxford University Press

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Detection of significantly differentially methylated regions in targeted bisulfite sequencing data (2013)

Hebestreit, K., Dugas, M., Klein, H.-U.

Oxford University Press

In: Bioinformatics

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Publication Date: 2013-06-24

Description: Motivation: Bisulfite sequencing is currently the gold standard to obtain genome-wide DNA methylation profiles in eukaryotes. In contrast to the rapid development of appropriate pre-processing and alignment software, methods for analyzing the resulting methylation profiles are relatively limited so far. For instance, an appropriate pipeline to detect DNA methylation differences between cancer and control samples is still required. Results: We propose an algorithm that detects significantly differentially methylated regions in data obtained by targeted bisulfite sequencing approaches, such as reduced representation bisulfite sequencing. In a first step, this approach tests all target regions for methylation differences by taking spatial dependence into account. A false discovery rate procedure controls the expected proportion of incorrectly rejected regions. In a second step, the significant target regions are trimmed to the actually differentially methylated regions. This hierarchical procedure detects differentially methylated regions with increased power compared with existing methods. Availability: R/Bioconductor package BiSeq. Contact: katja.hebestreit@uni-muenster.de Supplementary information: Supplementary Data are available at Bioinformatics online.

Print ISSN: 1367-4803

Electronic ISSN: 1460-2059

Topics: Biology , Computer Science , Medicine

Published by Oxford University Press

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Rheumatoid arthritis-associated RBPJ polymorphism alters memory CD4+ T cells (2016)

Orent, W., Mchenry, A. R., Rao, D. A., White, C., Klein, H.-U., Bassil, R., Srivastava, G., Replogle, J. M., Raj, T., Frangieh, M., Cimpean, M., Cuerdon, N., Chibnik, L., Khoury, S. J., Karlson, E. W., Brenner, M. B., De Jager, P., Bradshaw, E. M., Elyaman, W.

Oxford University Press

In: Human Molecular Genetics

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Publication Date: 2016-01-09

Description: Notch signaling has recently emerged as an important regulator of immune responses in autoimmune diseases. The recombination signal-binding protein for immunoglobulin kappa J region (RBPJ) is a transcriptional repressor, but converts into a transcriptional activator upon activation of the canonical Notch pathway. Genome-wide association studies of rheumatoid arthritis (RA) identified a susceptibility locus, rs874040 CC , which implicated the RBPJ gene. Here, chromatin state mapping generated using the chromHMM algorithm reveals strong enhancer regions containing DNase I hypersensitive sites overlapping the rs874040 linkage disequilibrium block in human memory, but not in naïve CD4 + T cells. The rs874040 overlapping this chromatin state was associated with increased RBPJ expression in stimulated memory CD4 + T cells from healthy subjects homozygous for the risk allele (CC) compared with memory CD4 + T cells bearing the protective allele (GG). Transcriptomic analysis of rs874040 CC memory T cells showed a repression of canonical Notch target genes IL (interleukin)-9, IL-17 and interferon (IFN) in the basal state. Interestingly, activation of the Notch pathway using soluble Notch ligand, Jagged2-Fc, induced IL-9 and IL-17A while delta-like 4Fc, another Notch ligand, induced higher IFN expression in the rs874040 CC memory CD4 + T cells compared with their rs874040 GG counterparts. In RA, RBPJ expression is elevated in memory T cells from RA patients compared with control subjects, and this was associated with induced inflammatory cytokines IL-9, IL-17A and IFN in response to Notch ligation in vitro . These findings demonstrate that the rs874040 CC allele skews memory T cells toward a pro-inflammatory phenotype involving Notch signaling, thus increasing the susceptibility to develop RA.

Print ISSN: 0964-6906

Electronic ISSN: 1460-2083

Topics: Biology , Medicine

Published by Oxford University Press

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