TY - JOUR
T1 - Kruppel-Like Factor 6 (KLF6) Is a Tumor-Suppressor Gene Frequently Inactivated in Colorectal Cancer
AU - Reeves, Helen L.
AU - Narla, Goutham
AU - Ogunbiyi, Olagunju
AU - Haq, Asif I.
AU - Katz, Amanda
AU - Benzeno, Sharon
AU - Hod, Eldad
AU - Harpaz, Noam
AU - Goldberg, Shlomit
AU - Tal-Kremer, Sigal
AU - Eng, Francis J.
AU - Arthur, Michael J.P.
AU - Martignetti, John A.
AU - Friedman, Scott L.
N1 - Funding Information:
Supported by grants from the National Institutes of Health (DK37340 to S.L.F.), Mount Sinai School of Medicine Dean’s Research Incentive Fund (to S.L.F.), Child Health Research Center (5 P30 HD28822 to J.A.M.), Charles and ELS Bendheim Foundation, Inc. (to S.L.F.), American Association for the Study of Liver Diseases/Schering (to H.L.R.), Howard Hughes Medical Institute (to G.N.), American Liver Foundation (to G.N. and F.J.E.), and UK-US Fulbright Commission (to M.J.P.A.).
PY - 2004/4
Y1 - 2004/4
N2 - Background & Aims: Kruppel-like factor 6 (KLF6) is a ubiquitous zinc finger tumor suppressor that is often mutated in prostate cancer. Our aims were to establish the frequency of KLF6 inactivation in sporadic and inflammatory bowel disease (IBD)-associated colorectal cancers (CRC); to correlate these abnormalities with mutation and/or loss of TP53, APC, and K-RAS; and to characterize the behavior of mutant KLF6 in colon-derived cell lines. Methods: We analyzed DNA isolated from 50 microdissected CRC cases, including 35 sporadic and 15 IBD-associated tumors. Microsatellite analysis and direct sequencing were used to establish the incidence of microsatellite instability, KLF6 and TP53 allelic imbalance, and KLF6, K-RAS, TP53, and APC mutation. Loss of growth suppressive function of the CRC-derived KLF6 mutants was characterized by in vitro thymidine incorporation assays and Western blotting. Results: KLF6 was inactivated by loss and/or mutation in most sporadic and IBD-related CRCs. The KLF6 locus was deleted in at least 55% of tumors, and mutations were identified in 44%. Rates of KLF6 loss and mutation were similar to those of TP53 and K-RAS in the same samples. KLF6 mutations were present in tumors with either microsatellite or chromosomal instability and were more common, particularly in the IBD-related cancers, in the presence of wild-type APC. Unlike wild-type KLF6, cancer-derived KLF6 mutants neither suppressed growth nor induced p21 following transfection into cultured cells. Conclusions: Deregulation of KLF6 by a combination of allelic imbalance and mutation may play a role in the development of CRC.
AB - Background & Aims: Kruppel-like factor 6 (KLF6) is a ubiquitous zinc finger tumor suppressor that is often mutated in prostate cancer. Our aims were to establish the frequency of KLF6 inactivation in sporadic and inflammatory bowel disease (IBD)-associated colorectal cancers (CRC); to correlate these abnormalities with mutation and/or loss of TP53, APC, and K-RAS; and to characterize the behavior of mutant KLF6 in colon-derived cell lines. Methods: We analyzed DNA isolated from 50 microdissected CRC cases, including 35 sporadic and 15 IBD-associated tumors. Microsatellite analysis and direct sequencing were used to establish the incidence of microsatellite instability, KLF6 and TP53 allelic imbalance, and KLF6, K-RAS, TP53, and APC mutation. Loss of growth suppressive function of the CRC-derived KLF6 mutants was characterized by in vitro thymidine incorporation assays and Western blotting. Results: KLF6 was inactivated by loss and/or mutation in most sporadic and IBD-related CRCs. The KLF6 locus was deleted in at least 55% of tumors, and mutations were identified in 44%. Rates of KLF6 loss and mutation were similar to those of TP53 and K-RAS in the same samples. KLF6 mutations were present in tumors with either microsatellite or chromosomal instability and were more common, particularly in the IBD-related cancers, in the presence of wild-type APC. Unlike wild-type KLF6, cancer-derived KLF6 mutants neither suppressed growth nor induced p21 following transfection into cultured cells. Conclusions: Deregulation of KLF6 by a combination of allelic imbalance and mutation may play a role in the development of CRC.
UR - http://www.scopus.com/inward/record.url?scp=11144357280&partnerID=8YFLogxK
U2 - 10.1053/j.gastro.2004.01.005
DO - 10.1053/j.gastro.2004.01.005
M3 - Article
C2 - 15057748
AN - SCOPUS:11144357280
SN - 0016-5085
VL - 126
SP - 1090
EP - 1103
JO - Gastroenterology
JF - Gastroenterology
IS - 4
ER -