The long tail of oncogenic drivers in prostate cancer

Armenia Joshua; Wankowicz Stephanie A. M.; Liu David; Gao Jianjiong; Kundra Ritika; Reznik Ed; Chatila Walid K.; Chakravarty Debyani; Han G. Celine; Coleman Ilsa; Montgomery Bruce; Pritchard Colin; Morrissey Colm; Barbieri Christopher E.; Beltran Himisha; Sboner Andrea; Zafeiriou Zafeiris; Miranda Susana; Bielski Craig M.; Penson Alexander V.; Tolonen Charlotte; Huang Franklin W.; Robinson Dan; Wu Yi Mi; Lonigro Robert; Garraway Levi A.; Demichelis Francesca; Kantoff Philip W.; Taplin Mary-Ellen; Abida Wassim; Taylor Barry S.; Scher Howard I.; Nelson Peter S.; de Bono Johann S.; Rubin Mark A.; Sawyers Charles L.; Chinnaiyan Arul M.; Schultz Nikolaus; Van Allen Eliezer M.

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The long tail of oncogenic drivers in prostate cancer

机译：前列腺癌中的致癌司机的长尾

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Comprehensive genomic characterization of prostate cancer has identified recurrent alterations in genes involved in androgen signaling, DNA repair, and PI3K signaling, among others. However, larger and uniform genomic analysis may identify additional recurrently mutated genes at lower frequencies. Here we aggregate and uniformly analyze exome sequencing data from 1,013 prostate cancers. We identify and validate a new class of E26 transformation-specific (ETS)-fusion-negative tumors defined by mutations in epigenetic regulators, as well as alterations in pathways not previously implicated in prostate cancer, such as the spliceosome pathway. We find that the incidence of significantly mutated genes (SMGs) follows a long-tail distribution, with many genes mutated in less than 3% of cases. We identify a total of 97 SMGs, including 70 not previously implicated in prostate cancer, such as the ubiquitin ligase CUL3 and the transcription factor SPEN. Finally, comparing primary and metastatic prostate cancer identifies a set of genomic markers that may inform risk stratification.

机译：前列腺癌的综合基因组表征已经确定了雄激素信号，DNA修复和PI3K信号传导中参与的基因的复发性改变。然而，较大且均匀的基因组分析可以在较低频率下识别额外的常规突变基因。在这里，我们汇总并统一分析来自1,013个前列腺癌的Exome测序数据。我们识别并验证通过表观遗传调节剂中的突变定义的新类别的E26转化特异性（ETS） - 熔母，以及以前没有涉及前列腺癌的途径的变化，例如抗缩肌瘤途径。我们发现显着突变的基因（SMG）的发病率遵循长尾分布，许多基因在不到3％的情况下突变。我们共识别总共97个SMG，其中70例以前没有涉及前列腺癌，例如泛素连接酶CUL3和转录因子均匀。最后，比较原发性和转移性前列腺癌鉴定了一组可能向风险分层提供信息的基因组标记。

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《Nature Genetics》 |2018年第5期|共9页
作者
Armenia Joshua; Wankowicz Stephanie A. M.; Liu David; Gao Jianjiong; Kundra Ritika; Reznik Ed; Chatila Walid K.; Chakravarty Debyani; Han G. Celine; Coleman Ilsa; Montgomery Bruce; Pritchard Colin; Morrissey Colm; Barbieri Christopher E.; Beltran Himisha; Sboner Andrea; Zafeiriou Zafeiris; Miranda Susana; Bielski Craig M.; Penson Alexander V.; Tolonen Charlotte; Huang Franklin W.; Robinson Dan; Wu Yi Mi; Lonigro Robert; Garraway Levi A.; Demichelis Francesca; Kantoff Philip W.; Taplin Mary-Ellen; Abida Wassim; Taylor Barry S.; Scher Howard I.; Nelson Peter S.; de Bono Johann S.; Rubin Mark A.; Sawyers Charles L.; Chinnaiyan Arul M.; Schultz Nikolaus; Van Allen Eliezer M.;
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作者单位

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Dana Farber Canc Inst Dept Med Oncol Boston MA 02115 USA;

Dana Farber Canc Inst Dept Med Oncol Boston MA 02115 USA;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Dana Farber Canc Inst Dept Med Oncol Boston MA 02115 USA;

Fred Hutchinson Canc Res Ctr Div Human Biol 1124 Columbia St Seattle WA 98104 USA;

Univ Washington Dept Med Seattle WA USA;

Univ Washington Dept Lab Med Seattle WA 98195 USA;

Univ Washington Dept Urol Seattle WA 98195 USA;

Weill Cornell Med Dept Pathol &

Lab Med New York NY USA;

Weill Cornell Med Dept Med Div Med Oncol New York NY USA;

Weill Cornell Med Dept Pathol &

Lab Med New York NY USA;

Inst Canc Res Div Clin Studies Biomarkers Team London England;

Inst Canc Res Div Clin Studies Biomarkers Team London England;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Broad Inst MIT &

Harvard Canc Program Cambridge MA 02142 USA;

Dana Farber Canc Inst Dept Med Oncol Boston MA 02115 USA;

Univ Michigan Michigan Ctr Translat Pathol Ann Arbor MI 48109 USA;

Univ Michigan Michigan Ctr Translat Pathol Ann Arbor MI 48109 USA;

Univ Michigan Michigan Ctr Translat Pathol Ann Arbor MI 48109 USA;

Dana Farber Canc Inst Dept Med Oncol Boston MA 02115 USA;

Univ Trento Ctr Integrated Biol Trento Italy;

Mem Sloan Kettering Canc Ctr Dept Med 1275 York Ave New York NY 10021 USA;

Dana Farber Canc Inst Dept Med Oncol Boston MA 02115 USA;

Mem Sloan Kettering Canc Ctr Dept Med 1275 York Ave New York NY 10021 USA;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Mem Sloan Kettering Canc Ctr Dept Med 1275 York Ave New York NY 10021 USA;

Fred Hutchinson Canc Res Ctr Div Human Biol 1124 Columbia St Seattle WA 98104 USA;

Inst Canc Res Div Clin Studies Biomarkers Team London England;

New York Presbyterian Hosp Weill Cornell Med Coll Englander Inst Precis Med New York NY USA;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Univ Michigan Michigan Ctr Translat Pathol Ann Arbor MI 48109 USA;

Mem Sloan Kettering Canc Ctr Human Oncol &

Pathogenesis Program 1275 York Ave New York NY 10021;

Dana Farber Canc Inst Dept Med Oncol Boston MA 02115 USA;

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正文语种 eng
中图分类医学遗传学;
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专利

1. The long tail of oncogenic drivers in prostate cancer (vol 50, pg 645, 2018) [J] . Armenia Joshua, Wankowicz Stephanie A. M., Liu David, Nature Genetics . 2019,第7期

机译：前列腺癌中致癌司机的长尾（第50 Vol 50，PG 645,2018）
2. Defining and Targeting the Oncogenic Drivers of Neuroendocrine Prostate Cancer [J] . Carver Brett S. Cancer Cell . 2016,第4期

机译：定义和靶向神经内分泌前列腺癌的致癌驱动因素
3. Wagging the long tail of drivers of prostate cancer [J] . Vincent L. Cannataro, Jeffrey P. Townsend PLoS Genetics . 2019,第1期

机译：摇摆着前列腺癌司机的长尾巴
4. Discovery of Human Prostate Cancer Biomarkers From a Xenograft Mouse Model and Formalin-fixed, Paraffin-embedded Prostate Cancer Tissue [C] . Hsin-Yao Tang, Lynn Beer, Tony Chang-Wong, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2010

机译：从异种移植小鼠模型和福尔马林固定，石蜡嵌入前列腺癌组织中发现人前列腺癌生物标志物
5. EGFR Rearrangements as Oncogenic Drivers and Therapeutic Targets in Lung Cancer [D] . Gallant, Jean-Nicolas. 2017

机译：EGFR重排作为肺癌的致癌驱动因子和治疗靶标
6. The long tail of oncogenic drivers in prostate cancer [O] . Joshua Armenia, Stephanie A.M. Wankowicz, David Liu, -1

机译：前列腺癌致癌驱动因子的长尾巴
7. The long tail of oncogenic drivers in prostate cancer [O] . Joshua Armenia, Stephanie A. M. Wankowicz, David Liu, 2018

机译：前列腺癌中致癌司机的长尾

The long tail of oncogenic drivers in prostate cancer

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