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A Point Mutation in DNA Polymerase β (POLB) Gene Is Associated with Increased Progesterone Receptor (PR) Expression and Intraperitoneal Metastasis in Gastric Cancer

Increased expression of progesterone receptor (PR) has been reported in gastric cancer (GC). We have previously identified a functional T889C point mutation in DNA polymerase beta (POLB), a DNA repair gene in GC. To provide a detailed analysis of molecular changes associated with the mutation, human...

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Autores principales: Tan, Xiaohui, Wu, Xiaoling, Ren, Shuyang, Wang, Hongyi, Li, Zhongwu, Alshenawy, Weaam, Li, Wenmei, Cui, Jiantao, Luo, Guangbin, Siegel, Robert S., Fu, Sidney W., Lu, Youyong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4964131/
https://www.ncbi.nlm.nih.gov/pubmed/27471563
http://dx.doi.org/10.7150/jca.14844
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author Tan, Xiaohui
Wu, Xiaoling
Ren, Shuyang
Wang, Hongyi
Li, Zhongwu
Alshenawy, Weaam
Li, Wenmei
Cui, Jiantao
Luo, Guangbin
Siegel, Robert S.
Fu, Sidney W.
Lu, Youyong
author_facet Tan, Xiaohui
Wu, Xiaoling
Ren, Shuyang
Wang, Hongyi
Li, Zhongwu
Alshenawy, Weaam
Li, Wenmei
Cui, Jiantao
Luo, Guangbin
Siegel, Robert S.
Fu, Sidney W.
Lu, Youyong
author_sort Tan, Xiaohui
collection PubMed
description Increased expression of progesterone receptor (PR) has been reported in gastric cancer (GC). We have previously identified a functional T889C point mutation in DNA polymerase beta (POLB), a DNA repair gene in GC. To provide a detailed analysis of molecular changes associated with the mutation, human cDNA microarrays focusing on 18 signal transduction pathways were used to analyze differential gene expression profiles between GC tissues with T889C mutant in POLB gene and those with wild type. Among the differentially expressed genes, notably, PR was one of the significantly up-regulated genes in T889C mutant POLB tissues, which were subsequently confirmed in POLB gene transfected AGS cell line. Interestingly, patients with T889C mutation and PR positivity were associated with higher incidence of intraperitoneal metastasis (IM). In vitro studies indicate that PR expression was upregulated in AGS cell line when transfected with T889C mutant expression vector. Cotransfection of T889C mutant allele and PR gene induced cell migration in the cell line. These data demonstrated that T889C mutation-associated PR overexpression results in increased IM. Therefore, T889C mutation-associated PR overexpression may serve as a biomarker for an adverse prognosis for human GC.
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spelling pubmed-49641312016-07-28 A Point Mutation in DNA Polymerase β (POLB) Gene Is Associated with Increased Progesterone Receptor (PR) Expression and Intraperitoneal Metastasis in Gastric Cancer Tan, Xiaohui Wu, Xiaoling Ren, Shuyang Wang, Hongyi Li, Zhongwu Alshenawy, Weaam Li, Wenmei Cui, Jiantao Luo, Guangbin Siegel, Robert S. Fu, Sidney W. Lu, Youyong J Cancer Research Paper Increased expression of progesterone receptor (PR) has been reported in gastric cancer (GC). We have previously identified a functional T889C point mutation in DNA polymerase beta (POLB), a DNA repair gene in GC. To provide a detailed analysis of molecular changes associated with the mutation, human cDNA microarrays focusing on 18 signal transduction pathways were used to analyze differential gene expression profiles between GC tissues with T889C mutant in POLB gene and those with wild type. Among the differentially expressed genes, notably, PR was one of the significantly up-regulated genes in T889C mutant POLB tissues, which were subsequently confirmed in POLB gene transfected AGS cell line. Interestingly, patients with T889C mutation and PR positivity were associated with higher incidence of intraperitoneal metastasis (IM). In vitro studies indicate that PR expression was upregulated in AGS cell line when transfected with T889C mutant expression vector. Cotransfection of T889C mutant allele and PR gene induced cell migration in the cell line. These data demonstrated that T889C mutation-associated PR overexpression results in increased IM. Therefore, T889C mutation-associated PR overexpression may serve as a biomarker for an adverse prognosis for human GC. Ivyspring International Publisher 2016-07-05 /pmc/articles/PMC4964131/ /pubmed/27471563 http://dx.doi.org/10.7150/jca.14844 Text en © Ivyspring International Publisher. Reproduction is permitted for personal, noncommercial use, provided that the article is in whole, unmodified, and properly cited. See http://ivyspring.com/terms for terms and conditions.
spellingShingle Research Paper
Tan, Xiaohui
Wu, Xiaoling
Ren, Shuyang
Wang, Hongyi
Li, Zhongwu
Alshenawy, Weaam
Li, Wenmei
Cui, Jiantao
Luo, Guangbin
Siegel, Robert S.
Fu, Sidney W.
Lu, Youyong
A Point Mutation in DNA Polymerase β (POLB) Gene Is Associated with Increased Progesterone Receptor (PR) Expression and Intraperitoneal Metastasis in Gastric Cancer
title A Point Mutation in DNA Polymerase β (POLB) Gene Is Associated with Increased Progesterone Receptor (PR) Expression and Intraperitoneal Metastasis in Gastric Cancer
title_full A Point Mutation in DNA Polymerase β (POLB) Gene Is Associated with Increased Progesterone Receptor (PR) Expression and Intraperitoneal Metastasis in Gastric Cancer
title_fullStr A Point Mutation in DNA Polymerase β (POLB) Gene Is Associated with Increased Progesterone Receptor (PR) Expression and Intraperitoneal Metastasis in Gastric Cancer
title_full_unstemmed A Point Mutation in DNA Polymerase β (POLB) Gene Is Associated with Increased Progesterone Receptor (PR) Expression and Intraperitoneal Metastasis in Gastric Cancer
title_short A Point Mutation in DNA Polymerase β (POLB) Gene Is Associated with Increased Progesterone Receptor (PR) Expression and Intraperitoneal Metastasis in Gastric Cancer
title_sort point mutation in dna polymerase β (polb) gene is associated with increased progesterone receptor (pr) expression and intraperitoneal metastasis in gastric cancer
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4964131/
https://www.ncbi.nlm.nih.gov/pubmed/27471563
http://dx.doi.org/10.7150/jca.14844
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