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Published in: Gastric Cancer 1/2016

01-01-2016 | Original Article

Recurrent amplification of MYC and TNFRSF11B in 8q24 is associated with poor survival in patients with gastric cancer

Authors: Xiaohong Wang, Yiqiang Liu, Duanfang Shao, Ziliang Qian, Zhengwei Dong, Yun Sun, Xiaofang Xing, Xiaojing Cheng, Hong Du, Ying Hu, Yingai Li, Lin Li, Bin Dong, Ziyu Li, Aiwen Wu, Xiaojiang Wu, Zhaode Bu, Xianglong Zong, Guanshan Zhu, Qunsheng Ji, Xian-zi Wen, Lian-hai Zhang, Jia-fu Ji

Published in: Gastric Cancer | Issue 1/2016

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Abstract

Background

Gastric cancer (GC) is an aggressive malignancy whose mechanisms of development and progression are poorly understood. The identification of prognosis-related genomic loci and genes may suffer from the relatively small case numbers and a lack of systematic validation in previous studies.

Methods

Array-based comparative genomic hybridization (aCGH) coupled with patient clinical information was applied to identify prognosis-related loci and genes with high-frequency recurrent gains in 129 GC patients. The candidate loci and genes were then validated using an independent cohort of 384 patients through branched DNA signal amplification analysis (QuantiGene assays).

Results

In the 129 patients, a copy number gain of three chromosome regions—namely, 8q22 (including ESRP1 and CCNE2), 8q24 (including MYC and TNFRSF11B), and 20q11-q13 (including SRC, MMP9, and CSE1L)—conferred poor survival for patients. In addition, the correlation between the branched DNA signal amplification analysis results and the aCGH results was analyzed in 73 of these 129 patients, and MYC, TNFRSF11B, ESRP1, CSE1L, and MMP9 were found to be well correlated. Further validation using an independent cohort (n = 384) verified that only MYC and TNFRSF11B within 8q24 are related to survival. Patients with gains in both MYC and TNFRSF11B had poorer survival than those with no gains, particularly those with noncardia GC. Gains in both of these genes were also a significant independent prognostic indicator.

Conclusions

Our results revealed that copy number gains in MYC and TNFRSF11B located at 8q24 are associated with survival in GC, particularly noncardia GC.
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Metadata
Title
Recurrent amplification of MYC and TNFRSF11B in 8q24 is associated with poor survival in patients with gastric cancer
Authors
Xiaohong Wang
Yiqiang Liu
Duanfang Shao
Ziliang Qian
Zhengwei Dong
Yun Sun
Xiaofang Xing
Xiaojing Cheng
Hong Du
Ying Hu
Yingai Li
Lin Li
Bin Dong
Ziyu Li
Aiwen Wu
Xiaojiang Wu
Zhaode Bu
Xianglong Zong
Guanshan Zhu
Qunsheng Ji
Xian-zi Wen
Lian-hai Zhang
Jia-fu Ji
Publication date
01-01-2016
Publisher
Springer Japan
Published in
Gastric Cancer / Issue 1/2016
Print ISSN: 1436-3291
Electronic ISSN: 1436-3305
DOI
https://doi.org/10.1007/s10120-015-0467-2

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