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Genome and transcriptome sequencing of lung cancers reveal diverse mutational and splicing events.


ABSTRACT: Lung cancer is a highly heterogeneous disease in terms of both underlying genetic lesions and response to therapeutic treatments. We performed deep whole-genome sequencing and transcriptome sequencing on 19 lung cancer cell lines and three lung tumor/normal pairs. Overall, our data show that cell line models exhibit similar mutation spectra to human tumor samples. Smoker and never-smoker cancer samples exhibit distinguishable patterns of mutations. A number of epigenetic regulators, including KDM6A, ASH1L, SMARCA4, and ATAD2, are frequently altered by mutations or copy number changes. A systematic survey of splice-site mutations identified 106 splice site mutations associated with cancer specific aberrant splicing, including mutations in several known cancer-related genes. RAC1b, an isoform of the RAC1 GTPase that includes one additional exon, was found to be preferentially up-regulated in lung cancer. We further show that its expression is significantly associated with sensitivity to a MAP2K (MEK) inhibitor PD-0325901. Taken together, these data present a comprehensive genomic landscape of a large number of lung cancer samples and further demonstrate that cancer-specific alternative splicing is a widespread phenomenon that has potential utility as therapeutic biomarkers. The detailed characterizations of the lung cancer cell lines also provide genomic context to the vast amount of experimental data gathered for these lines over the decades, and represent highly valuable resources for cancer biology.

SUBMITTER: Liu J 

PROVIDER: S-EPMC3514662 | biostudies-literature | 2012 Dec

REPOSITORIES: biostudies-literature

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Genome and transcriptome sequencing of lung cancers reveal diverse mutational and splicing events.

Liu Jinfeng J   Lee William W   Jiang Zhaoshi Z   Chen Zhongqiang Z   Jhunjhunwala Suchit S   Haverty Peter M PM   Gnad Florian F   Guan Yinghui Y   Gilbert Houston N HN   Stinson Jeremy J   Klijn Christiaan C   Guillory Joseph J   Bhatt Deepali D   Vartanian Steffan S   Walter Kimberly K   Chan Jocelyn J   Holcomb Thomas T   Dijkgraaf Peter P   Johnson Stephanie S   Koeman Julie J   Minna John D JD   Gazdar Adi F AF   Stern Howard M HM   Hoeflich Klaus P KP   Wu Thomas D TD   Settleman Jeff J   de Sauvage Frederic J FJ   Gentleman Robert C RC   Neve Richard M RM   Stokoe David D   Modrusan Zora Z   Seshagiri Somasekar S   Shames David S DS   Zhang Zemin Z  

Genome research 20121002 12


Lung cancer is a highly heterogeneous disease in terms of both underlying genetic lesions and response to therapeutic treatments. We performed deep whole-genome sequencing and transcriptome sequencing on 19 lung cancer cell lines and three lung tumor/normal pairs. Overall, our data show that cell line models exhibit similar mutation spectra to human tumor samples. Smoker and never-smoker cancer samples exhibit distinguishable patterns of mutations. A number of epigenetic regulators, including KD  ...[more]

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