GLORIA — GEOMAR Library Ocean Research Information Access

1

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Demographic history and rare allele sharing among human populations

Gravel, Simon ; Henn, Brenna M. ; Gutenkunst, Ryan N. ; [weitere]

Proceedings of the National Academy of Sciences ; 2011

In: Proceedings of the National Academy of Sciences Vol. 108, No. 29 ( 2011-07-19), p. 11983-11988

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 108, No. 29 ( 2011-07-19), p. 11983-11988

Kurzfassung: High-throughput sequencing technology enables population-level surveys of human genomic variation. Here, we examine the joint allele frequency distributions across continental human populations and present an approach for combining complementary aspects of whole-genome, low-coverage data and targeted high-coverage data. We apply this approach to data generated by the pilot phase of the Thousand Genomes Project, including whole-genome 2–4× coverage data for 179 samples from HapMap European, Asian, and African panels as well as high-coverage target sequencing of the exons of 800 genes from 697 individuals in seven populations. We use the site frequency spectra obtained from these data to infer demographic parameters for an Out-of-Africa model for populations of African, European, and Asian descent and to predict, by a jackknife-based approach, the amount of genetic diversity that will be discovered as sample sizes are increased. We predict that the number of discovered nonsynonymous coding variants will reach 100,000 in each population after ∼1,000 sequenced chromosomes per population, whereas ∼2,500 chromosomes will be needed for the same number of synonymous variants. Beyond this point, the number of segregating sites in the European and Asian panel populations is expected to overcome that of the African panel because of faster recent population growth. Overall, we find that the majority of human genomic variable sites are rare and exhibit little sharing among diverged populations. Our results emphasize that replication of disease association for specific rare genetic variants across diverged populations must overcome both reduced statistical power because of rarity and higher population divergence.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.1019276108

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 2011

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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2

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Mouse mammary tumor virus/v-Ha- ras transgene-induced mammary tumors exhibit strain-specific allelic loss on mouse chromosome 4

Radany, Eric H. ; Hong, Karen ; Kesharvarzi, Sima ; [weitere]

Proceedings of the National Academy of Sciences ; 1997

In: Proceedings of the National Academy of Sciences Vol. 94, No. 16 ( 1997-08-05), p. 8664-8669

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 94, No. 16 ( 1997-08-05), p. 8664-8669

Kurzfassung: Hybrid mice carrying oncogenic transgenes afford powerful systems for investigating loss of heterozygosity (LOH) in tumors. Here, we apply this approach to a neoplasm of key importance in human medicine: mammary carcinoma. We performed a whole genome search for LOH using the mouse mammary tumor virus/v-Ha- ras mammary carcinoma model in female (FVB/N × Mus musculus castaneus )F 1 mice. Mammary tumors developed as expected, as well as a few tumors of a second type (uterine leiomyosarcoma) not previously associated with this transgene. Genotyping of 94 anatomically independent tumors revealed high-frequency LOH (≈38%) for markers on chromosome 4. A marked allelic bias was observed, with M. musculus castaneus alleles almost exclusively being lost. No evidence of genomic imprinting effects was noted. These data point to the presence of a tumor suppressor gene(s) on mouse chromosome 4 involved in mammary carcinogenesis induced by mutant H- ras expression, and for which a significant functional difference may exist between the M. musculus castaneus and FVB/N alleles. Provisional subchromosomal localization of this gene, designated Loh-3 , can be made to a distal segment having syntenic correspondence to human chromosome 1p; LOH in this latter region is observed in several human malignancies, including breast cancers. Evidence was also obtained for a possible second locus associated with LOH with less marked allele bias on proximal chromosome 4.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.94.16.8664

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 1997

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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3

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An initial strategy for the systematic identification of functional elements in the human genome by low-redundancy comparative sequencing

Margulies, Elliott H. ; Vinson, Jade P. ; Miller, Webb ; [weitere]

Proceedings of the National Academy of Sciences ; 2005

In: Proceedings of the National Academy of Sciences Vol. 102, No. 13 ( 2005-03-29), p. 4795-4800

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 102, No. 13 ( 2005-03-29), p. 4795-4800

Kurzfassung: With the recent completion of a high-quality sequence of the human genome, the challenge is now to understand the functional elements that it encodes. Comparative genomic analysis offers a powerful approach for finding such elements by identifying sequences that have been highly conserved during evolution. Here, we propose an initial strategy for detecting such regions by generating low-redundancy sequence from a collection of 16 eutherian mammals, beyond the 7 for which genome sequence data are already available. We show that such sequence can be accurately aligned to the human genome and used to identify most of the highly conserved regions. Although not a long-term substitute for generating high-quality genomic sequences from many mammalian species, this strategy represents a practical initial approach for rapidly annotating the most evolutionarily conserved sequences in the human genome, providing a key resource for the systematic study of human genome function.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.0409882102

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 2005

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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4

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Complementary genomic approaches highlight the PI3K/mTOR pathway as a common vulnerability in osteosarcoma

Perry, Jennifer A. ; Kiezun, Adam ; Tonzi, Peter ; [weitere]

Proceedings of the National Academy of Sciences ; 2014

In: Proceedings of the National Academy of Sciences Vol. 111, No. 51 ( 2014-12-23)

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 111, No. 51 ( 2014-12-23)

Kurzfassung: Osteosarcoma is the most common primary bone tumor, yet there have been no substantial advances in treatment or survival in three decades. We examined 59 tumor/normal pairs by whole-exome, whole-genome, and RNA-sequencing. Only the TP53 gene was mutated at significant frequency across all samples. The mean nonsilent somatic mutation rate was 1.2 mutations per megabase, and there was a median of 230 somatic rearrangements per tumor. Complex chains of rearrangements and localized hypermutation were detected in almost all cases. Given the intertumor heterogeneity, the extent of genomic instability, and the difficulty in acquiring a large sample size in a rare tumor, we used several methods to identify genomic events contributing to osteosarcoma survival. Pathway analysis, a heuristic analytic algorithm, a comparative oncology approach, and an shRNA screen converged on the phosphatidylinositol 3-kinase/mammalian target of rapamycin (PI3K/mTOR) pathway as a central vulnerability for therapeutic exploitation in osteosarcoma. Osteosarcoma cell lines are responsive to pharmacologic and genetic inhibition of the PI3K/mTOR pathway both in vitro and in vivo.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.1419260111

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 2014

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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5

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Discovery and prioritization of somatic mutations in diffuse large B-cell lymphoma (DLBCL) by whole-exome sequencing

Lohr, Jens G. ; Stojanov, Petar ; Lawrence, Michael S. ; [weitere]

Proceedings of the National Academy of Sciences ; 2012

In: Proceedings of the National Academy of Sciences Vol. 109, No. 10 ( 2012-03-06), p. 3879-3884

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 109, No. 10 ( 2012-03-06), p. 3879-3884

Kurzfassung: To gain insight into the genomic basis of diffuse large B-cell lymphoma (DLBCL), we performed massively parallel whole-exome sequencing of 55 primary tumor samples from patients with DLBCL and matched normal tissue. We identified recurrent mutations in genes that are well known to be functionally relevant in DLBCL, including MYD88 , CARD11 , EZH2 , and CREBBP . We also identified somatic mutations in genes for which a functional role in DLBCL has not been previously suspected. These genes include MEF2B , MLL2 , BTG1 , GNA13 , ACTB , P2RY8 , PCLO , and TNFRSF14 . Further, we show that BCL2 mutations commonly occur in patients with BCL2 / IgH rearrangements as a result of somatic hypermutation normally occurring at the IgH locus. The BCL2 point mutations are primarily synonymous, and likely caused by activation-induced cytidine deaminase–mediated somatic hypermutation, as shown by comprehensive analysis of enrichment of mutations in WRCY target motifs. Those nonsynonymous mutations that are observed tend to be found outside of the functionally important BH domains of the protein, suggesting that strong negative selection against BCL2 loss-of-function mutations is at play. Last, by using an algorithm designed to identify likely functionally relevant but infrequent mutations, we identify KRAS , BRAF , and NOTCH1 as likely drivers of DLBCL pathogenesis in some patients. Our data provide an unbiased view of the landscape of mutations in DLBCL, and this in turn may point toward new therapeutic strategies for the disease.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.1121343109

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 2012

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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6

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Systematic investigation of genetic vulnerabilities across cancer cell lines reveals lineage-specific dependencies in ovarian cancer

Cheung, Hiu Wing ; Cowley, Glenn S. ; Weir, Barbara A. ; [weitere]

Proceedings of the National Academy of Sciences ; 2011

In: Proceedings of the National Academy of Sciences Vol. 108, No. 30 ( 2011-07-26), p. 12372-12377

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 108, No. 30 ( 2011-07-26), p. 12372-12377

Kurzfassung: A comprehensive understanding of the molecular vulnerabilities of every type of cancer will provide a powerful roadmap to guide therapeutic approaches. Efforts such as The Cancer Genome Atlas Project will identify genes with aberrant copy number, sequence, or expression in various cancer types, providing a survey of the genes that may have a causal role in cancer. A complementary approach is to perform systematic loss-of-function studies to identify essential genes in particular cancer cell types. We have begun a systematic effort, termed Project Achilles, aimed at identifying genetic vulnerabilities across large numbers of cancer cell lines. Here, we report the assessment of the essentiality of 11,194 genes in 102 human cancer cell lines. We show that the integration of these functional data with information derived from surveying cancer genomes pinpoints known and previously undescribed lineage-specific dependencies across a wide spectrum of cancers. In particular, we found 54 genes that are specifically essential for the proliferation and viability of ovarian cancer cells and also amplified in primary tumors or differentially overexpressed in ovarian cancer cell lines. One such gene, PAX8 , is focally amplified in 16% of high-grade serous ovarian cancers and expressed at higher levels in ovarian tumors. Suppression of PAX8 selectively induces apoptotic cell death of ovarian cancer cells. These results identify PAX8 as an ovarian lineage-specific dependency. More generally, these observations demonstrate that the integration of genome-scale functional and structural studies provides an efficient path to identify dependencies of specific cancer types on particular genes and pathways.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.1109363108

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 2011

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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7

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Effects of p 53 mutations on apoptosis in mouse intestinal and human colonic adenomas

Fazeli, Amin ; Steen, Robert G. ; Dickinson, Stephanie L. ; [weitere]

Proceedings of the National Academy of Sciences ; 1997

In: Proceedings of the National Academy of Sciences Vol. 94, No. 19 ( 1997-09-16), p. 10199-10204

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 94, No. 19 ( 1997-09-16), p. 10199-10204

Kurzfassung: We have examined the effects of inactivation of the p53 tumor suppressor gene on the incidence of apoptotic cell death in two stages of the adenoma-to-carcinoma progression in the intestine: in early adenomas where p53 mutations are rare and in highly dysplastic adenomas where loss of p53 occurs frequently. Homozygosity for an inactivating germ-line mutation of p53 had no effect on the incidence or the rate of progression of Apc Min/+ -induced adenomas in mice and also did not affect the frequency of apoptosis in the cells of these adenomas. To examine the effect of p53 loss on apoptosis in late-stage adenomas, we compared the incidence of apoptotic cell death before and after the appearance of highly dysplastic cells in human colonic adenomas. The appearance of highly dysplastic cells, which usually coincides during colon tumor progression with loss of heterozygosity at the p53 locus, did not correlate with a reduction in the incidence of apoptosis. These studies suggest that p53 is only one of the genes that determine the incidence of apoptotic in colon carcinomas and that wild-type p53 retards the progression of many benign colonic adenoma to malignant carcinomas by mechanism(s) other than the promotion of apoptosis.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.94.19.10199

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 1997

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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8

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Systematic dissection of genomic features determining transcription factor binding and enhancer function

Grossman, Sharon R. ; Zhang, Xiaolan ; Wang, Li ; [weitere]

Proceedings of the National Academy of Sciences ; 2017

In: Proceedings of the National Academy of Sciences Vol. 114, No. 7 ( 2017-02-14)

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 114, No. 7 ( 2017-02-14)

Kurzfassung: Enhancers regulate gene expression through the binding of sequence-specific transcription factors (TFs) to cognate motifs. Various features influence TF binding and enhancer function—including the chromatin state of the genomic locus, the affinities of the binding site, the activity of the bound TFs, and interactions among TFs. However, the precise nature and relative contributions of these features remain unclear. Here, we used massively parallel reporter assays (MPRAs) involving 32,115 natural and synthetic enhancers, together with high-throughput in vivo binding assays, to systematically dissect the contribution of each of these features to the binding and activity of genomic regulatory elements that contain motifs for PPARγ, a TF that serves as a key regulator of adipogenesis. We show that distinct sets of features govern PPARγ binding vs. enhancer activity. PPARγ binding is largely governed by the affinity of the specific motif site and higher-order features of the larger genomic locus, such as chromatin accessibility. In contrast, the enhancer activity of PPARγ binding sites depends on varying contributions from dozens of TFs in the immediate vicinity, including interactions between combinations of these TFs. Different pairs of motifs follow different interaction rules, including subadditive, additive, and superadditive interactions among specific classes of TFs, with both spatially constrained and flexible grammars. Our results provide a paradigm for the systematic characterization of the genomic features underlying regulatory elements, applicable to the design of synthetic regulatory elements or the interpretation of human genetic variation.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.1621150114

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 2017

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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9

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Systematic discovery of regulatory motifs in conserved regions of the human genome, including thousands of CTCF insulator sites

Xie, Xiaohui ; Mikkelsen, Tarjei S. ; Gnirke, Andreas ; [weitere]

Proceedings of the National Academy of Sciences ; 2007

In: Proceedings of the National Academy of Sciences Vol. 104, No. 17 ( 2007-04-24), p. 7145-7150

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 104, No. 17 ( 2007-04-24), p. 7145-7150

Kurzfassung: Conserved noncoding elements (CNEs) constitute the majority of sequences under purifying selection in the human genome, yet their function remains largely unknown. Experimental evidence suggests that many of these elements play regulatory roles, but little is known about regulatory motifs contained within them. Here we describe a systematic approach to discover and characterize regulatory motifs within mammalian CNEs by searching for long motifs (12–22 nt) with significant enrichment in CNEs and studying their biochemical and genomic properties. Our analysis identifies 233 long motifs (LMs), matching a total of ≈60,000 conserved instances across the human genome. These motifs include 16 previously known regulatory elements, such as the histone 3′-UTR motif and the neuron-restrictive silencer element, as well as striking examples of novel functional elements. The most highly enriched motif (LM1) corresponds to the X-box motif known from yeast and nematode. We show that it is bound by the RFX1 protein and identify thousands of conserved motif instances, suggesting a broad role for the RFX family in gene regulation. A second group of motifs (LM2*) does not match any previously known motif. We demonstrate by biochemical and computational methods that it defines a binding site for the CTCF protein, which is involved in insulator function to limit the spread of gene activation. We identify nearly 15,000 conserved sites that likely serve as insulators, and we show that nearby genes separated by predicted CTCF sites show markedly reduced correlation in gene expression. These sites may thus partition the human genome into domains of expression.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.0701811104

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 2007

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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10

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Chromatin extrusion explains key features of loop and domain formation in wild-type and engineered genomes

Sanborn, Adrian L. ; Rao, Suhas S. P. ; Huang, Su-Chen ; [weitere]

Proceedings of the National Academy of Sciences ; 2015

In: Proceedings of the National Academy of Sciences Vol. 112, No. 47 ( 2015-11-24)

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In: Proceedings of the National Academy of Sciences, Proceedings of the National Academy of Sciences, Vol. 112, No. 47 ( 2015-11-24)

Kurzfassung: We recently used in situ Hi-C to create kilobase-resolution 3D maps of mammalian genomes. Here, we combine these maps with new Hi-C, microscopy, and genome-editing experiments to study the physical structure of chromatin fibers, domains, and loops. We find that the observed contact domains are inconsistent with the equilibrium state for an ordinary condensed polymer. Combining Hi-C data and novel mathematical theorems, we show that contact domains are also not consistent with a fractal globule. Instead, we use physical simulations to study two models of genome folding. In one, intermonomer attraction during polymer condensation leads to formation of an anisotropic “tension globule.” In the other, CCCTC-binding factor (CTCF) and cohesin act together to extrude unknotted loops during interphase. Both models are consistent with the observed contact domains and with the observation that contact domains tend to form inside loops. However, the extrusion model explains a far wider array of observations, such as why loops tend not to overlap and why the CTCF-binding motifs at pairs of loop anchors lie in the convergent orientation. Finally, we perform 13 genome-editing experiments examining the effect of altering CTCF-binding sites on chromatin folding. The convergent rule correctly predicts the affected loops in every case. Moreover, the extrusion model accurately predicts in silico the 3D maps resulting from each experiment using only the location of CTCF-binding sites in the WT. Thus, we show that it is possible to disrupt, restore, and move loops and domains using targeted mutations as small as a single base pair.

Materialart: Online-Ressource

ISSN: 0027-8424 , 1091-6490

URL: Article

DOI: 10.1073/pnas.1518552112

RVK:

TA 1000

RVK:

WA 15000

Sprache: Englisch

Verlag: Proceedings of the National Academy of Sciences

Publikationsdatum: 2015

ZDB Id: 209104-5

ZDB Id: 1461794-8

SSG: 11

SSG: 12

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