TY - JOUR
T1 - Allelic imbalance in gastric cancer
T2 - An affected site on chromosome arm 3p
AU - Schneider, Barbara G.
AU - Pulitzer, Donald R.
AU - Brown, Rhonda D.
AU - Prihoda, Thomas J.
AU - Bostwick, David G.
AU - Saldivar, Victor
AU - Rodriguez‐Martinez, Hector A.
AU - Gutiérrez‐Diaz C., M. Esther
AU - O'Connell, Peter
PY - 1995/8
Y1 - 1995/8
N2 - In order to detect regions of DNA containing tumor suppressor genes involved in the development of gastric cancer, we performed an allelotype study on 78 gastric adenocarcinomas from a population composed largely of Texan Hispanics and Anglos, two ethnic groups that have a ratio of incidence rates of gastric cancer of approximately 2: 1. In total, 42 microsatellite markers were employed, which detected at least one site per arm of each autosome in the human genome. These included several markers linked to known tumor suppressor genes (TP53, APC, DCC, RBI, and BRCAI). Sites showing quantitative allelic imbalance (Al) greater than 30% were located on 3p (36%), 11q (31%), 12q (38%), 13q (33%), 17p near TP53 (74%), and 17q near BRCAI (32%). Among the 22% of cases showing microsatellite instability (MI), a subset (4 of 17) showed instability at 59% or more of sites tested. No ethnic bias was detected in cases showing MI or in cases with Al at sites with rates of AI above 30%. Tumors of the intestinal subtype were significantly more likely than diffuse tumors to show AI at D 135170 (P = 0.01). A deletion map of chromosome arm 3p was prepared for tumors with Al at D3S1478. These data indicate that a tumor suppressor gene on chromosome arm 3p is involved in the development of a subset of gastric cancers. © 1995 Wiley‐Liss, Inc.
AB - In order to detect regions of DNA containing tumor suppressor genes involved in the development of gastric cancer, we performed an allelotype study on 78 gastric adenocarcinomas from a population composed largely of Texan Hispanics and Anglos, two ethnic groups that have a ratio of incidence rates of gastric cancer of approximately 2: 1. In total, 42 microsatellite markers were employed, which detected at least one site per arm of each autosome in the human genome. These included several markers linked to known tumor suppressor genes (TP53, APC, DCC, RBI, and BRCAI). Sites showing quantitative allelic imbalance (Al) greater than 30% were located on 3p (36%), 11q (31%), 12q (38%), 13q (33%), 17p near TP53 (74%), and 17q near BRCAI (32%). Among the 22% of cases showing microsatellite instability (MI), a subset (4 of 17) showed instability at 59% or more of sites tested. No ethnic bias was detected in cases showing MI or in cases with Al at sites with rates of AI above 30%. Tumors of the intestinal subtype were significantly more likely than diffuse tumors to show AI at D 135170 (P = 0.01). A deletion map of chromosome arm 3p was prepared for tumors with Al at D3S1478. These data indicate that a tumor suppressor gene on chromosome arm 3p is involved in the development of a subset of gastric cancers. © 1995 Wiley‐Liss, Inc.
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U2 - 10.1002/gcc.2870130406
DO - 10.1002/gcc.2870130406
M3 - Article
C2 - 7547634
AN - SCOPUS:0029088784
SN - 1045-2257
VL - 13
SP - 263
EP - 271
JO - Genes Chromosomes and Cancer
JF - Genes Chromosomes and Cancer
IS - 4
ER -