Functional Genomics Identifies Novel Genes Essential for Clear Cell Renal Cell Carcinoma Tumor Cell Proliferation and Migration

Overview

Journal Oncotarget

Specialty Oncology

Date 2014 Jul 1

PMID 24979721

Citations 18

Authors

Christina A von Roemeling

Laura A Marlow

Derek C Radisky

Austin Rohl

Hege Ekeberg Larsen

Johnny Wei

Heather Sasinowska

Heng Zhu

Richard Drake

Maciek Sasinowski

Han W Tun

John A Copland

Affiliations

Soon will be listed here.

Abstract

Currently there is a lack of targeted therapies that lead to long-term attenuation or regression of disease in patients with advanced clear cell renal cell carcinoma (ccRCC). Our group has implemented a high-throughput genetic analysis coupled with a high-throughput proliferative screen in order to investigate the genetic contributions of a large cohort of overexpressed genes at the functional level in an effort to better understand factors involved in tumor initiation and progression. Patient gene array analysis identified transcripts that are consistently elevated in patient ccRCC as compared to matched normal renal tissues. This was followed by a high-throughput lentivirus screen, independently targeting 195 overexpressed transcripts identified in the gene array in four ccRCC cell lines. This revealed 31 'hits' that contribute to ccRCC cell proliferation. Many of the hits identified are not only presented in the context of ccRCC for the first time, but several have not been previously linked to cancer. We further characterize the function of a group of hits in tumor cell invasion. Taken together these findings reveal pathways that may be critical in ccRCC tumorigenicity, and identifies novel candidate factors that could serve as targets for therapeutic intervention or diagnostic/prognostic biomarkers for patients with advanced ccRCC.

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