Inhibition of Transcription Elongation by the VHL Tumor Suppressor Protein

Delin Duan; Arnim Pause; Wilson H. Burgess; Teijiro Aso; David Y.T. Chen; Karla P. Garrett; Ronald Conaway; Joan Conaway; W. Marston Linehan; Richard D. Klausner

doi:10.1126/science.7660122

Inhibition of Transcription Elongation by the VHL Tumor Suppressor Protein

Delin Duan(National Institutes of Health), Arnim Pause(National Institutes of Health), Wilson H. Burgess(National Institutes of Health), Teijiro Aso(National Institutes of Health), David Y.T. Chen(National Institutes of Health), Karla P. Garrett(National Institutes of Health), Ronald Conaway(National Institutes of Health), Joan Conaway(National Institutes of Health), W. Marston Linehan(National Institutes of Health), Richard D. Klausner(National Institutes of Health)

Science

September 8, 1995

10.1126/science.7660122

Cited by 577

Abstract

Germline mutations in the von Hippel-Lindau tumor suppressor gene (VHL) predispose individuals to a variety of tumors, including renal carcinoma, hemangioblastoma of the central nervous system, and pheochromocytoma. Here, a cellular transcription factor, Elongin (SIII), is identified as a functional target of the VHL protein. Elongin (SIII) is a heterotrimer consisting of a transcriptionally active subunit (A) and two regulatory subunits (B and C) that activate transcription elongation by RNA polymerase II. The VHL protein was shown to bind tightly and specifically to the Elongin B and C subunits and to inhibit Elongin (SIII) transcriptional activity in vitro. These findings reveal a potentially important transcriptional regulatory network in which the VHL protein may play a key role.

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