A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets
Objective Gastric cancer is a major gastrointestinal malignancy for which targeted therapies are emerging as treatment options. This study sought to identify the most prevalent molecular targets in gastric cancer and to elucidate systematic patterns of exclusivity and co-occurrence among these targe...
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sg-ntu-dr.10356-1006532022-02-16T16:29:45Z A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets Tao, Jiong Tan, Iain Beehuat Deng, Niantao Goh, Liang-Kee Wang, Hannah Das, Kakoli Zhang, Shenli Lee, Minghui Wu, Jeanie Lim, Kiat Hon Lei, Zhengdeng Goh, Glenn Lim, Qing-Yan Tan, Angie Lay-Keng Poh, Dianne Yu Sin Riahi, Sudep Bell, Sandra Linnartz, Ronald Zhu, Feng Yeoh, Khay Guan Toh, Han Chong Yong, Wei Peng Cheong, Hyun Cheol Rha, Sun Young Boussioutas, Alex Grabsch, Heike Tan, Patrick Shi, Michael M. Rozen, Steve G. School of Biological Sciences DRNTU::Science::Biological sciences Objective Gastric cancer is a major gastrointestinal malignancy for which targeted therapies are emerging as treatment options. This study sought to identify the most prevalent molecular targets in gastric cancer and to elucidate systematic patterns of exclusivity and co-occurrence among these targets, through comprehensive genomic analysis of a large panel of gastric cancers. Design Using high-resolution single nucleotide polymorphism arrays, copy number alterations were profiled in a panel of 233 gastric cancers (193 primary tumours, 40 cell lines) and 98 primary matched gastric non-malignant samples. For selected alterations, their impact on gene expression and clinical outcome were evaluated. Results 22 recurrent focal alterations (13 amplifications and nine deletions) were identified. These included both known targets (FGFR2, ERBB2) and also novel genes in gastric cancer (KLF5, GATA6). Receptor tyrosine kinase (RTK)/RAS alterations were found to be frequent in gastric cancer. This study also demonstrates, for the first time, that these alterations occur in a mutually exclusive fashion, with KRAS gene amplifications highlighting a clinically relevant but previously underappreciated gastric cancer subgroup. FGFR2-amplified gastric cancers were also shown to be sensitive to dovitinib, an orally bioavailable FGFR/VEGFR targeting agent, potentially representing a subtype-specific therapy for FGFR2-amplified gastric cancers. Conclusion The study demonstrates the existence of five distinct gastric cancer patient subgroups, defined by the signature genomic alterations FGFR2 (9% of tumours), KRAS (9%), EGFR (8%), ERBB2 (7%) and MET (4%). Collectively, these subgroups suggest that at least 37% of gastric cancer patients may be potentially treatable by RTK/RAS directed therapies. 2013-10-07T04:03:30Z 2019-12-06T20:25:56Z 2013-10-07T04:03:30Z 2019-12-06T20:25:56Z 2012 2012 Journal Article Deng, N., Goh, L.-K., Wang, H., Das, K., Tao, J., Tan, I. B., et al. (2012). A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets. Gut, 61(5). https://hdl.handle.net/10356/100653 http://hdl.handle.net/10220/16299 10.1136/gutjnl-2011-301839 22315472 en Gut |
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DRNTU::Science::Biological sciences Tao, Jiong Tan, Iain Beehuat Deng, Niantao Goh, Liang-Kee Wang, Hannah Das, Kakoli Zhang, Shenli Lee, Minghui Wu, Jeanie Lim, Kiat Hon Lei, Zhengdeng Goh, Glenn Lim, Qing-Yan Tan, Angie Lay-Keng Poh, Dianne Yu Sin Riahi, Sudep Bell, Sandra Linnartz, Ronald Zhu, Feng Yeoh, Khay Guan Toh, Han Chong Yong, Wei Peng Cheong, Hyun Cheol Rha, Sun Young Boussioutas, Alex Grabsch, Heike Tan, Patrick Shi, Michael M. Rozen, Steve G. A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets |
| description |
Objective Gastric cancer is a major gastrointestinal malignancy for which targeted therapies are emerging as treatment options. This study sought to identify the most prevalent molecular targets in gastric cancer and to elucidate systematic patterns of exclusivity and co-occurrence among these targets, through comprehensive genomic analysis of a large panel of gastric cancers.
Design Using high-resolution single nucleotide polymorphism arrays, copy number alterations were profiled in a panel of 233 gastric cancers (193 primary tumours, 40 cell lines) and 98 primary matched gastric non-malignant samples. For selected alterations, their impact on gene expression and clinical outcome were evaluated.
Results 22 recurrent focal alterations (13 amplifications and nine deletions) were identified. These included both known targets (FGFR2, ERBB2) and also novel genes in gastric cancer (KLF5, GATA6). Receptor tyrosine kinase (RTK)/RAS alterations were found to be frequent in gastric cancer. This study also demonstrates, for the first time, that these alterations occur in a mutually exclusive fashion, with KRAS gene amplifications highlighting a clinically relevant but previously underappreciated gastric cancer subgroup. FGFR2-amplified gastric cancers were also shown to be sensitive to dovitinib, an orally bioavailable FGFR/VEGFR targeting agent, potentially representing a subtype-specific therapy for FGFR2-amplified gastric cancers.
Conclusion The study demonstrates the existence of five distinct gastric cancer patient subgroups, defined by the signature genomic alterations FGFR2 (9% of tumours), KRAS (9%), EGFR (8%), ERBB2 (7%) and MET (4%). Collectively, these subgroups suggest that at least 37% of gastric cancer patients may be potentially treatable by RTK/RAS directed therapies. |
| author2 |
School of Biological Sciences |
| author_facet |
School of Biological Sciences Tao, Jiong Tan, Iain Beehuat Deng, Niantao Goh, Liang-Kee Wang, Hannah Das, Kakoli Zhang, Shenli Lee, Minghui Wu, Jeanie Lim, Kiat Hon Lei, Zhengdeng Goh, Glenn Lim, Qing-Yan Tan, Angie Lay-Keng Poh, Dianne Yu Sin Riahi, Sudep Bell, Sandra Linnartz, Ronald Zhu, Feng Yeoh, Khay Guan Toh, Han Chong Yong, Wei Peng Cheong, Hyun Cheol Rha, Sun Young Boussioutas, Alex Grabsch, Heike Tan, Patrick Shi, Michael M. Rozen, Steve G. |
| format |
Article |
| author |
Tao, Jiong Tan, Iain Beehuat Deng, Niantao Goh, Liang-Kee Wang, Hannah Das, Kakoli Zhang, Shenli Lee, Minghui Wu, Jeanie Lim, Kiat Hon Lei, Zhengdeng Goh, Glenn Lim, Qing-Yan Tan, Angie Lay-Keng Poh, Dianne Yu Sin Riahi, Sudep Bell, Sandra Linnartz, Ronald Zhu, Feng Yeoh, Khay Guan Toh, Han Chong Yong, Wei Peng Cheong, Hyun Cheol Rha, Sun Young Boussioutas, Alex Grabsch, Heike Tan, Patrick Shi, Michael M. Rozen, Steve G. |
| author_sort |
Tao, Jiong |
| title |
A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets |
| title_short |
A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets |
| title_full |
A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets |
| title_fullStr |
A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets |
| title_full_unstemmed |
A comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets |
| title_sort |
comprehensive survey of genomic alterations in gastric cancer reveals systematic patterns of molecular exclusivity and co-occurrence among distinct therapeutic targets |
| publishDate |
2013 |
| url |
https://hdl.handle.net/10356/100653 http://hdl.handle.net/10220/16299 |
| _version_ |
1725985652307132416 |