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zadetkov: 167
1.
  • GISTIC2.0 facilitates sensi... GISTIC2.0 facilitates sensitive and confident localization of the targets of focal somatic copy-number alteration in human cancers
    Mermel, Craig H; Schumacher, Steven E; Hill, Barbara ... Genome biology, 04/2011, Letnik: 12, Številka: 4
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    We describe methods with enhanced power and specificity to identify genes targeted by somatic copy-number alterations (SCNAs) that drive cancer growth. By separating SCNA profiles into underlying ...
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2.
  • β-Catenin-Driven Cancers Re... β-Catenin-Driven Cancers Require a YAP1 Transcriptional Complex for Survival and Tumorigenesis
    Rosenbluh, Joseph; Nijhawan, Deepak; Cox, Andrew G. ... Cell, 12/2012, Letnik: 151, Številka: 7
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    Wnt/β-catenin signaling plays a key role in the pathogenesis of colon and other cancers; emerging evidence indicates that oncogenic β-catenin regulates several biological processes essential for ...
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3.
  • Pan-cancer patterns of soma... Pan-cancer patterns of somatic copy number alteration
    Zack, Travis I; Schumacher, Stephen E; Carter, Scott L ... Nature genetics, 10/2013, Letnik: 45, Številka: 10
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    Determining how somatic copy number alterations (SCNAs) promote cancer is an important goal. We characterized SCNA patterns in 4,934 cancers from The Cancer Genome Atlas Pan-Cancer data set. ...
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4.
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5.
  • Widespread Genetic Heteroge... Widespread Genetic Heterogeneity in Multiple Myeloma: Implications for Targeted Therapy
    Lohr, Jens G.; Stojanov, Petar; Carter, Scott L. ... Cancer cell, 01/2014, Letnik: 25, Številka: 1
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    We performed massively parallel sequencing of paired tumor/normal samples from 203 multiple myeloma (MM) patients and identified significantly mutated genes and copy number alterations and discovered ...
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6.
  • Cancer Vulnerabilities Unve... Cancer Vulnerabilities Unveiled by Genomic Loss
    Nijhawan, Deepak; Zack, Travis I.; Ren, Yin ... Cell, 08/2012, Letnik: 150, Številka: 4
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    Due to genome instability, most cancers exhibit loss of regions containing tumor suppressor genes and collateral loss of other genes. To identify cancer-specific vulnerabilities that are the result ...
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7.
  • Landscape of Genomic Altera... Landscape of Genomic Alterations in Pituitary Adenomas
    Bi, Wenya Linda; Horowitz, Peleg; Greenwald, Noah F ... Clinical cancer research, 04/2017, Letnik: 23, Številka: 7
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    Pituitary adenomas are the second most common primary brain tumor, yet their genetic profiles are incompletely understood. We performed whole-exome sequencing of 42 pituitary macroadenomas and ...
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8.
  • BET bromodomain inhibition of MYC-amplified medulloblastoma
    Bandopadhayay, Pratiti; Bergthold, Guillaume; Nguyen, Brian ... Clinical cancer research, 02/2014, Letnik: 20, Številka: 4
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    MYC-amplified medulloblastomas are highly lethal tumors. Bromodomain and extraterminal (BET) bromodomain inhibition has recently been shown to suppress MYC-associated transcriptional activity in ...
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9.
  • Gastrointestinal adenocarcinomas of the esophagus, stomach, and colon exhibit distinct patterns of genome instability and oncogenesis
    Dulak, Austin M; Schumacher, Steven E; van Lieshout, Jasper ... Cancer research (Chicago, Ill.), 09/2012, Letnik: 72, Številka: 17
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    A more detailed understanding of the somatic genetic events that drive gastrointestinal adenocarcinomas is necessary to improve diagnosis and therapy. Using data from high-density genomic profiling ...
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10.
  • Tumor-suppressor genes that escape from X-inactivation contribute to cancer sex bias
    Dunford, Andrew; Weinstock, David M; Savova, Virginia ... Nature genetics, 01/2017, Letnik: 49, Številka: 1
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    There is a striking and unexplained male predominance across many cancer types. A subset of X-chromosome genes can escape X-inactivation, which would protect females from complete functional loss by ...
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zadetkov: 167

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