Tamoxifen Dependent Interaction Between the Estrogen Receptor and a Novel P21 Activated Kinase

Abstract

The estrogen receptor alpha (ER(alpha)) plays an important role in breast cancer and a large fraction of ER(alpha) positive breast cancers respond to tamoxifen. We cloned a novel p21 activated kinase (PAK), termed PAK6, which binds to the androgen receptor (AR) and selectively to the tamoxifen liganded ER(alpha). PAKs are a family of seilne/threonine kinases that bind to and are regulated by the Rho family small (p21) GTPases, Cdc42 and Rac. PAKs are involved in translating extracellular signals into cellular responses. Although PAK6 binds to Cdc42, it lacks the Cdc42 regulated autoinhibitory domain found in other PAKs and can instead be activated by steroid receptor binding. Binding is mediated by at least two sites on PAK6, one at the N-terminus and another towards the middle of the protein. PAK6 inhibits ER(alpha) and AR transcriptional activity. PAK6 is highly expressed in brain and testes, is also expressed in mammary epithelium and prostate, and its expression in breast cancer cell lines has been confirmed by a polyclonal antibody. Further studies of PAK6 protein expression in breast cancer are in progress, and breast cancer cell lines expressing wild type and mutant PAK6 have been generated to assess functions in breast cancer.

Document Details

Document Type

Technical Report

Publication Date

Jun 01, 2002

Accession Number

ADA407401

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