Authors
Goutham Narla, Analisa DiFeo, Helen L Reeves, Daniel J Schaid, Jennifer Hirshfeld, Eldad Hod, Amanda Katz, William B Isaacs, Scott Hebbring, Akira Komiya, Shannon K McDonnell, Kathleen E Wiley, Steven J Jacobsen, Sarah D Isaacs, Patrick C Walsh, S Lilly Zheng, Bao-Li Chang, Danielle M Friedrichsen, Janet L Stanford, Elaine A Ostrander, Arul M Chinnaiyan, Mark A Rubin, Jianfeng Xu, Stephen N Thibodeau, Scott L Friedman, John A Martignetti
Publication date
2005/2/15
Journal
Cancer research
Volume
65
Issue
4
Pages
1213-1222
Publisher
American Association for Cancer Research
Description
Prostate cancer is a leading and increasingly prevalent cause of cancer death in men. Whereas family history of disease is one of the strongest prostate cancer risk factors and suggests a hereditary component, the predisposing genetic factors remain unknown. We first showed that KLF6 is a tumor suppressor somatically inactivated in prostate cancer and since then, its functional loss has been further established in prostate cancer cell lines and other human cancers. Wild-type KLF6, but not patient-derived mutants, suppresses cell growth through p53-independent transactivation of p21. Here we show that a germline KLF6 single nucleotide polymorphism, confirmed in a tri-institutional study of 3,411 men, is significantly associated with an increased relative risk of prostate cancer in men, regardless of family history of disease. This prostate cancer–associated allele generates a novel functional SRp40 DNA …
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Scholar articles
G Narla, A DiFeo, HL Reeves, DJ Schaid, J Hirshfeld… - Cancer research, 2005