STK33 Kinase Activity is Nonessential in KRAS-dependent Cancer Cells

Overview

Journal Cancer Res

Specialty Oncology

Date 2011 Jul 12

PMID 21742770

Citations 63

Authors

Carol Babij

Yihong Zhang

Robert J Kurzeja

Anke Munzli

Amro Shehabeldin

Manory Fernando

Kim Quon

Paul D Kassner

Astrid A Ruefli-Brasse

Vivienne J Watson

Flordeliza Fajardo

Angela Jackson

James Zondlo

Yu Sun

Aaron R Ellison

Cherylene A Plewa

Miguel Tisha San

John Robinson

John McCarter

Ralf Schwandner

Ted Judd

Josette Carnahan

Isabelle Dussault

Affiliations

Soon will be listed here.

Abstract

Despite the prevalence of KRAS mutations in human cancers, there remain no targeted therapies for treatment. The serine-threonine kinase STK33 has been proposed to be required for the survival of mutant KRAS-dependent cell lines, suggesting that small molecule kinase inhibitors of STK33 may be useful to treat KRAS-dependent tumors. In this study, we investigated the role of STK33 in mutant KRAS human cancer cells using RNA interference, dominant mutant overexpression, and small molecule inhibitors. As expected, KRAS downregulation decreased the survival of KRAS-dependent cells. In contrast, STK33 downregulation or dominant mutant overexpression had no effect on KRAS signaling or survival of these cells. Similarly, a synthetic lethal siRNA screen conducted in a broad panel of KRAS wild-type or mutant cells identified KRAS but not STK33 as essential for survival. We also obtained similar negative results using small molecule inhibitors of the STK33 kinase identified by high-throughput screening. Taken together, our findings refute earlier proposals that STK33 inhibition may be a useful therapeutic approach to target human KRAS mutant tumors.

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