Genomics

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Whole-Genome and Epigenomic Landscapes of Etiologically Distinct Subtypes of Cholangiocarcinoma


ABSTRACT: Cholangiocarcinoma (CCA) is a hepatobiliary malignancy exhibiting high incidence in countries with endemic liver-fluke infection. We analyzed 489 CCAs from 10 countries, combining whole-genome (71 cases), targeted/exome, copy-number, gene expression, and DNA methylation information. Integrative clustering defined 4 CCA clusters-fluke-positive CCAs (clusters 1/2) are enriched in ERBB2 amplifications and TP53 mutations; conversely, fluke-negative CCAs (clusters 3/4) exhibit high copy-number alterations and PD-1/PD-L2 expression, or epigenetic mutations (IDH1/2, BAP1) and FGFR/PRKA-related gene rearrangements. Whole-genome analysis highlighted FGFR2 3' untranslated region deletion as a mechanism of FGFR2 upregulation. Integration of noncoding promoter mutations with protein-DNA binding profiles demonstrates pervasive modulation of H3K27me3-associated sites in CCA. Clusters 1 and 4 exhibit distinct DNA hypermethylation patterns targeting either CpG islands or shores-mutation signature and subclonality analysis suggests that these reflect different mutational pathways. Our results exemplify how genetics, epigenetics, and environmental carcinogens can interplay across different geographies to generate distinct molecular subtypes of cancer.SIGNIFICANCE: Integrated whole-genome and epigenomic analysis of CCA on an international scale identifies new CCA driver genes, noncoding promoter mutations, and structural variants. CCA molecular landscapes differ radically by etiology, underscoring how distinct cancer subtypes in the same organ may arise through different extrinsic and intrinsic carcinogenic processes.

PROVIDER: EGAS00001001653 | EGA |

REPOSITORIES: EGA

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Whole-Genome and Epigenomic Landscapes of Etiologically Distinct Subtypes of Cholangiocarcinoma.

Jusakul Apinya A   Cutcutache Ioana I   Yong Chern Han CH   Lim Jing Quan JQ   Huang Mi Ni MN   Padmanabhan Nisha N   Nellore Vishwa V   Kongpetch Sarinya S   Ng Alvin Wei Tian AWT   Ng Ley Moy LM   Choo Su Pin SP   Myint Swe Swe SS   Thanan Raynoo R   Nagarajan Sanjanaa S   Lim Weng Khong WK   Ng Cedric Chuan Young CCY   Boot Arnoud A   Liu Mo M   Ong Choon Kiat CK   Rajasegaran Vikneswari V   Lie Stefanus S   Lim Alvin Soon Tiong AST   Lim Tse Hui TH   Tan Jing J   Loh Jia Liang JL   McPherson John R JR   Khuntikeo Narong N   Bhudhisawasdi Vajaraphongsa V   Yongvanit Puangrat P   Wongkham Sopit S   Totoki Yasushi Y   Nakamura Hiromi H   Arai Yasuhito Y   Yamasaki Satoshi S   Chow Pierce Kah-Hoe PK   Chung Alexander Yaw Fui AYF   Ooi London Lucien Peng Jin LLPJ   Lim Kiat Hon KH   Dima Simona S   Duda Dan G DG   Popescu Irinel I   Broet Philippe P   Hsieh Sen-Yung SY   Yu Ming-Chin MC   Scarpa Aldo A   Lai Jiaming J   Luo Di-Xian DX   Carvalho André Lopes AL   Vettore André Luiz AL   Rhee Hyungjin H   Park Young Nyun YN   Alexandrov Ludmil B LB   Gordân Raluca R   Rozen Steven G SG   Shibata Tatsuhiro T   Pairojkul Chawalit C   Teh Bin Tean BT   Tan Patrick P  

Cancer discovery 20170630 10


Cholangiocarcinoma (CCA) is a hepatobiliary malignancy exhibiting high incidence in countries with endemic liver-fluke infection. We analyzed 489 CCAs from 10 countries, combining whole-genome (71 cases), targeted/exome, copy-number, gene expression, and DNA methylation information. Integrative clustering defined 4 CCA clusters-fluke-positive CCAs (clusters 1/2) are enriched in <i>ERBB2</i> amplifications and <i>TP53</i> mutations; conversely, fluke-negative CCAs (clusters 3/4) exhibit high copy  ...[more]

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