Inhibition of estrogen receptor action by a naturally occurring variant in human breast tumors.

Suzanne A.W. Fuqua; Fitzgerald Sd; Allred Dc; Elledge Rm; Zafar Nawaz; McDonnell Dp; O'Malley Bw; GL Greene; McGuire Wl

Inhibition of estrogen receptor action by a naturally occurring variant in human breast tumors.

Suzanne A.W. Fuqua, Fitzgerald Sd(The University of Texas Health Science Center at San Antonio), Allred Dc(The University of Texas Health Science Center at San Antonio), Elledge Rm, Zafar Nawaz(Baylor College of Medicine), McDonnell Dp(Baylor College of Medicine), O'Malley Bw(Baylor College of Medicine), GL Greene(University of Chicago), McGuire Wl(The University of Texas Health Science Center at San Antonio)

PubMed

January 15, 1992

Cited by 251

Abstract

It is fairly well accepted that the presence of estrogen receptor (ER) and progesterone receptor (PgR) identifies breast cancer patients with a lower risk of relapse and better overall survival. But patients with discordant receptors, the ER+/PgR- phenotype, are often intermediate in clinical response. We focused upon this group of patients and have identified a truncated ER which is abundant in some ER+/PgR- breast tumors and which inhibits the binding of wild-type ER to its cognate response element. This variant interferes in a dominant negative manner with wild-type ER function and may represent a mechanism for modulation of estrogen responsiveness.

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