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Extending gene ontology with gene association networks (2016)

Peng, J., Wang, T., Wang, J., Wang, Y., Chen, J.

Oxford University Press

In: Bioinformatics

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Publication Date: 2016-04-08

Description: Motivation: Gene ontology (GO) is a widely used resource to describe the attributes for gene products. However, automatic GO maintenance remains to be difficult because of the complex logical reasoning and the need of biological knowledge that are not explicitly represented in the GO. The existing studies either construct whole GO based on network data or only infer the relations between existing GO terms. None is purposed to add new terms automatically to the existing GO. Results: We proposed a new algorithm ‘GOExtender’ to efficiently identify all the connected gene pairs labeled by the same parent GO terms. GOExtender is used to predict new GO terms with biological network data, and connect them to the existing GO. Evaluation tests on biological process and cellular component categories of different GO releases showed that GOExtender can extend new GO terms automatically based on the biological network. Furthermore, we applied GOExtender to the recent release of GO and discovered new GO terms with strong support from literature. Availability and implementation: Software and supplementary document are available at www.msu.edu/%7Ejinchen/GOExtender Contact: jinchen@msu.edu or ydwang@hit.edu.cn 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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Epidemic Clones, Oceanic Gene Pools, and Eco-LD in the Free Living Marine Pathogen Vibrio parahaemolyticus (2015)

Cui, Y., Yang, X., Didelot, X., Guo, C., Li, D., Yan, Y., Zhang, Y., Yuan, Y., Yang, H., Wang, J., Wang, J., Song, Y., Zhou, D., Falush, D., Yang, R.

Oxford University Press

In: Molecular Biology and Evolution

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Publication Date: 2015-05-30

Description: We investigated global patterns of variation in 157 whole-genome sequences of Vibrio parahaemolyticus , a free-living and seafood associated marine bacterium. Pandemic clones, responsible for recent outbreaks of gastroenteritis in humans, have spread globally. However, there are oceanic gene pools, one located in the oceans surrounding Asia and another in the Mexican Gulf. Frequent recombination means that most isolates have acquired the genetic profile of their current location. We investigated the genetic structure in the Asian gene pool by calculating the effective population size in two different ways. Under standard neutral models, the two estimates should give similar answers but we found a 27-fold difference. We propose that this discrepancy is caused by the subdivision of the species into a hundred or more ecotypes which are maintained stably in the population. To investigate the genetic factors involved, we used 51 unrelated isolates to conduct a genome-wide scan for epistatically interacting loci. We found a single example of strong epistasis between distant genome regions. A majority of strains had a type VI secretion system associated with bacterial killing. The remaining strains had genes associated with biofilm formation and regulated by cyclic dimeric GMP signaling. All strains had one or other of the two systems and none of isolate had complete complements of both systems, although several strains had remnants. Further "top down" analysis of patterns of linkage disequilibrium within frequently recombining species will allow a detailed understanding of how selection acts to structure the pattern of variation within natural bacterial populations.

Print ISSN: 0737-4038

Electronic ISSN: 1537-1719

Topics: Biology

Published by Oxford University Press

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Sprites: detection of deletions from sequencing data by re-aligning split reads (2016)

Zhang, Z., Wang, J., Luo, J., Ding, X., Zhong, J., Wang, J., Wu, F.-X., Pan, Y.

Oxford University Press

In: Bioinformatics

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Publication Date: 2016-06-16

Description: Motivation : Advances of next generation sequencing technologies and availability of short read data enable the detection of structural variations (SVs). Deletions, an important type of SVs, have been suggested in association with genetic diseases. There are three types of deletions: blunt deletions, deletions with microhomologies and deletions with microsinsertions. The last two types are very common in the human genome, but they pose difficulty for the detection. Furthermore, finding deletions from sequencing data remains challenging. It is highly appealing to develop sensitive and accurate methods to detect deletions from sequencing data, especially deletions with microhomology and deletions with microinsertion. Results : We present a novel method called Sprites (SPlit Read re-alIgnment To dEtect Structural variants) which finds deletions from sequencing data. It aligns a whole soft-clipping read rather than its clipped part to the target sequence, a segment of the reference which is determined by spanning reads, in order to find the longest prefix or suffix of the read that has a match in the target sequence. This alignment aims to solve the problem of deletions with microhomologies and deletions with microinsertions. Using both simulated and real data we show that Sprites performs better on detecting deletions compared with other current methods in terms of F-score. Availability and implementation : Sprites is open source software and freely available at https://github.com/zhangzhen/sprites . Contact: jxwang@mail.csu.edu.cn Supplementary data: 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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A Trust Routing for Multimedia Social Networks (2015)

Wu, G., Liu, Z., Yao, L., Deng, J., Wang, J.

Oxford University Press

In: Computer Journal

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Publication Date: 2015-03-27

Description: Due to the disconnected and store-and-forward architecture in multimedia social networks (MSNs), routing becomes a great challenge with the frequent path disruptions. Moreover, some nodes in MSNs tend to be selfish or malicious, e.g. they sometimes will not forward packets for other nodes or will launch passive and active attacks in order to save their limited resources such as bandwidth, battery or storage. In order to address this issue, we propose a fuzzy-based trust management technique for context-based routing in MSNs. We incorporate social trust metrics and quality of service metrics into our trust model. By adopting fuzzy sets, every node can evaluate the credibility of other nodes based on the direct and indirect relationship. By ranking all its neighbors according to the trust values, each node can purge untrustworthy nodes. Since only trusted nodes’ packets will be forwarded, the selfish or malicious nodes have the incentive to behave well again in order to be able to send packets. Additionally, we perform extensive security and performance evaluation with the opportunistic network environment simulator. The simulation results show that our trust model can dynamically update the trust value in real time, effectively measure the trust relationship and correctly identify malicious or selfish nodes. Furthermore, the proposed trust routing is a lightweight protocol balancing the message overhead and delivery ratio.

Print ISSN: 0010-4620

Electronic ISSN: 1460-2067

Topics: Computer Science

Published by Oxford University Press

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Lnc2Cancer: a manually curated database of experimentally supported lncRNAs associated with various human cancers (2016)

Ning, S., Zhang, J., Wang, P., Zhi, H., Wang, J., Liu, Y., Gao, Y., Guo, M., Yue, M., Wang, L., Li, X.

Oxford University Press

In: Nucleic Acids Research

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Publication Date: 2016-01-07

Description: Lnc2Cancer ( http://www.bio-bigdata.net/lnc2cancer ) is a manually curated database of cancer-associated long non-coding RNAs (lncRNAs) with experimental support that aims to provide a high-quality and integrated resource for exploring lncRNA deregulation in various human cancers. LncRNAs represent a large category of functional RNA molecules that play a significant role in human cancers. A curated collection and summary of deregulated lncRNAs in cancer is essential to thoroughly understand the mechanisms and functions of lncRNAs. Here, we developed the Lnc2Cancer database, which contains 1057 manually curated associations between 531 lncRNAs and 86 human cancers. Each association includes lncRNA and cancer name, the lncRNA expression pattern, experimental techniques, a brief functional description, the original reference and additional annotation information. Lnc2Cancer provides a user-friendly interface to conveniently browse, retrieve and download data. Lnc2Cancer also offers a submission page for researchers to submit newly validated lncRNA-cancer associations. With the rapidly increasing interest in lncRNAs, Lnc2Cancer will significantly improve our understanding of lncRNA deregulation in cancer and has the potential to be a timely and valuable resource.

Print ISSN: 0305-1048

Electronic ISSN: 1362-4962

Topics: Biology

Published by Oxford University Press

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Structural basis for the Smad5 MH1 domain to recognize different DNA sequences (2015)

Chai, N., Li, W.-X., Wang, J., Wang, Z.-X., Yang, S.-M., Wu, J.-W.

Oxford University Press

In: Nucleic Acids Research

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Publication Date: 2015-10-15

Description: Smad proteins are important intracellular mediators of TGF-β signalling, which transmit signals directly from cell surface receptors to the nucleus. The MH1 domain of Smad plays a key role in DNA recognition. Two types of DNA sequence were identified as Smad binding motifs: the Smad binding element (SBE) and the GC-rich sequence. Here we report the first crystal structure of the Smad5 MH1 domain in complex with the GC-rich sequence. Compared with the Smad5-MH1/SBE complex structure, the Smad5 MH1 domain contacts the GC-rich site with the same β-hairpin, but the detailed interaction modes are different. Conserved β-hairpin residues make base specific contacts with the minimal GC-rich site, 5'-GGC-3'. The assembly of Smad5-MH1 on the GC-rich DNA also results in distinct DNA conformational changes. Moreover, the crystal structure of Smad5-MH1 in complex with a composite DNA sequence demonstrates that the MH1 domain is targeted to each binding site (GC-rich or SBE) with modular binding modes, and the length of the DNA spacer affects the MH1 assembly. In conclusion, our work provides the structural basis for the recognition and binding specificity of the Smad MH1 domain with the DNA targets.

Print ISSN: 0305-1048

Electronic ISSN: 1362-4962

Topics: Biology

Published by Oxford University Press

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The deepest X-ray view of high-redshift galaxies: constraints on low-rate black hole accretion (2016)

Vito, F., Gilli, R., Vignali, C., Brandt, W. N., Comastri, A., Yang, G., Lehmer, B. D., Luo, B., Basu-Zych, A., Bauer, F. E., Cappelluti, N., Koekemoer, A., Mainieri, V., Paolillo, M., Ranalli, P., Shemmer, O., Trump, J., Wang, J. X., Xue, Y. Q.

Oxford University Press

In: Monthly Notices of the Royal Astronomical Society

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Publication Date: 2016-09-10

Description: We exploit the 7 Ms Chandra observations in the Chandra Deep Field-South (CDF-S), the deepest X-ray survey to date, coupled with CANDELS/GOODS-S data, to measure the total X-ray emission arising from 2076 galaxies at 3.5 ≤ z 〈 6.5. This aim is achieved by stacking the Chandra data at the positions of optically selected galaxies, reaching effective exposure times of ≥10 9 s. We detect significant (〉3.7) X-ray emission from massive galaxies at z 4. We also report the detection of massive galaxies at z 5 at a 99.7 per cent confidence level (2.7), the highest significance ever obtained for X-ray emission from galaxies at such high redshifts. No significant signal is detected from galaxies at even higher redshifts. The stacking results place constraints on the BHAD associated with the known high-redshift galaxy samples, as well as on the SFRD at high redshift, assuming a range of prescriptions for X-ray emission due to X- ray binaries. We find that the X-ray emission from our sample is likely dominated by processes related to star formation. Our results show that low-rate mass accretion on to SMBHs in individually X-ray-undetected galaxies is negligible, compared with the BHAD measured for samples of X-ray detected AGN, for cosmic SMBH mass assembly at high redshift. We also place, for the first time, constraints on the faint-end of the AGN X-ray luminosity function (logL X ~ 42) at z 〉 4, with evidence for fairly flat slopes. The implications of all of these findings are discussed in the context of the evolution of the AGN population at high redshift.

Print ISSN: 0035-8711

Electronic ISSN: 1365-2966

Topics: Physics

Published by Oxford University Press

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Predicting regulatory variants with composite statistic (2016)

Li, M. J., Pan, Z., Liu, Z., Wu, J., Wang, P., Zhu, Y., Xu, F., Xia, Z., Sham, P. C., Kocher, J.-P. A., Li, M., Liu, J. S., Wang, J.

Oxford University Press

In: Bioinformatics

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Publication Date: 2016-09-12

Description: Motivation: Prediction and prioritization of human non-coding regulatory variants is critical for understanding the regulatory mechanisms of disease pathogenesis and promoting personalized medicine. Existing tools utilize functional genomics data and evolutionary information to evaluate the pathogenicity or regulatory functions of non-coding variants. However, different algorithms lead to inconsistent and even conflicting predictions. Combining multiple methods may increase accuracy in regulatory variant prediction. Results: Here, we compiled an integrative resource for predictions from eight different tools on functional annotation of non-coding variants. We further developed a composite strategy to integrate multiple predictions and computed the composite likelihood of a given variant being regulatory variant. Benchmarked by multiple independent causal variants datasets, we demonstrated that our composite model significantly improves the prediction performance. Availability and Implementation: We implemented our model and scoring procedure as a tool, named PRVCS, which is freely available to academic and non-profit usage at http://jjwanglab.org/PRVCS . Contact: wang.junwen@mayo.edu , jliu@stat.harvard.edu , or limx54@gmail.com 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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Gas-phase metallicity profiles of the Bluedisk galaxies: Is metallicity in a local star formation regulated equilibrium? (2015)

Carton, D., Brinchmann, J., Wang, J., Bigiel, F., Cormier, D., Hulst, T. v. d., Jozsa, G. I. G., Serra, P., Verheijen, M. A. W.

Oxford University Press

In: Monthly Notices of the Royal Astronomical Society

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Publication Date: 2015-05-29

Description: As part of the Bluedisk survey, we analyse the radial gas-phase metallicity profiles of 50 late-type galaxies. We compare the metallicity profiles of a sample of H i -rich galaxies against a control sample of H i -‘normal’ galaxies. We find the metallicity gradient of a galaxy to be strongly correlated with its H i mass fraction ( $\textrm {M(H\,\small {I})} / \textrm {M}_{\ast }$ ). We note that some galaxies exhibit a steeper metallicity profile in the outer disc than in the inner disc. These galaxies are found in both the H i -rich and control samples. This contradicts a previous indication that these outer drops are exclusive to H i -rich galaxies. These effects are not driven by bars, although we do find some indication that barred galaxies have flatter metallicity profiles. By applying a simple analytical model, we are able to account for the variety of metallicity profiles that the two samples present. The success of this model implies that the metallicity in these isolated galaxies may be in a local equilibrium, regulated by star formation. This insight could provide an explanation of the observed local mass–metallicity relation.

Print ISSN: 0035-8711

Electronic ISSN: 1365-2966

Topics: Physics

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Arginine methylation of DRBD18 differentially impacts its opposing effects on the trypanosome transcriptome (2015)

Lott, K., Mukhopadhyay, S., Li, J., Wang, J., Yao, J., Sun, Y., Qu, J., Read, L. K.

Oxford University Press

In: Nucleic Acids Research

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Publication Date: 2015-06-24

Description: Arginine methylation is a posttranslational modification that impacts wide-ranging cellular functions, including transcription, mRNA splicing and translation. RNA binding proteins (RBPs) represent one of the largest classes of arginine methylated proteins in both mammals and the early diverging parasitic protozoan, Trypanosoma brucei . Here, we report the effects of arginine methylation on the functions of the essential and previously uncharacterized T. brucei RBP, DRBD18. RNAseq analysis shows that DRBD18 depletion causes extensive rearrangement of the T. brucei transcriptome, with increases and decreases in hundreds of mRNAs. DRBD18 contains three methylated arginines, and we used complementation of DRBD18 knockdown cells with methylmimic or hypomethylated DRBD18 to assess the functions of these methylmarks. Methylmimic and hypomethylated DRBD18 associate with different ribonucleoprotein complexes. These altered macromolecular interactions translate into differential impacts on the T. brucei transcriptome. Methylmimic DRBD18 preferentially stabilizes target RNAs, while hypomethylated DRBD18 is more efficient at destabilizing RNA. The protein arginine methyltransferase, TbPRMT1, interacts with DRBD18 and knockdown of TbPRMT1 recapitulates the effects of hypomethylated DRBD18 on mRNA levels. Together, these data support a model in which arginine methylation acts as a switch that regulates T. brucei gene expression.

Print ISSN: 0305-1048

Electronic ISSN: 1362-4962

Topics: Biology

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