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Data from An Immune-Inflammation Gene Expression Signature in Prostate Tumors of Smokers

Authors :
Stefan Ambs
Arthur A. Hurwitz
Arun Sreekumar
Nagireddy Putluri
Dong H. Lee
Christopher A. Loffredo
Robert M. Stephens
Richard B. Alexander
Michael J. Naslund
James F. Borin
Symone V. Jordan
Damali N. Martin
Misop Han
Harris G. Yfantis
Diana C. Haines
Jennifer L. Shoe
Atsushi Terunuma
Robert S. Hudson
John W. Gillespie
Katherine E. Stagliano
Tiffany H. Dorsey
Jun Luo
Wei Tang
Ming Yi
Sharon A. Glynn
Tiffany A. Wallace
Robyn L. Prueitt
Publication Year :
2023
Publisher :
American Association for Cancer Research (AACR), 2023.

Abstract

Smokers develop metastatic prostate cancer more frequently than nonsmokers, suggesting that a tobacco-derived factor is driving metastatic progression. To identify smoking-induced alterations in human prostate cancer, we analyzed gene and protein expression patterns in tumors collected from current, past, and never smokers. By this route, we elucidated a distinct pattern of molecular alterations characterized by an immune and inflammation signature in tumors from current smokers that were either attenuated or absent in past and never smokers. Specifically, this signature included elevated immunoglobulin expression by tumor-infiltrating B cells, NF-κB activation, and increased chemokine expression. In an alternate approach to characterize smoking-induced oncogenic alterations, we also explored the effects of nicotine in human prostate cancer cells and prostate cancer–prone TRAMP mice. These investigations showed that nicotine increased glutamine consumption and invasiveness of cancer cells in vitro and accelerated metastatic progression in tumor-bearing TRAMP mice. Overall, our findings suggest that nicotine is sufficient to induce a phenotype resembling the epidemiology of smoking-associated prostate cancer progression, illuminating a novel candidate driver underlying metastatic prostate cancer in current smokers. Cancer Res; 76(5); 1055–65. ©2015 AACR.

Details

Database :
OpenAIRE
Accession number :
edsair.doi...........52f8c36b2991100a26ed3b9f308e6b3d
Full Text :
https://doi.org/10.1158/0008-5472.c.6508259.v1