| Literature DB >> 26880715 |
Stephanie Zdanov1, Magis Mandapathil2, Rasha Abu Eid3, Saudat Adamson-Fadeyi1, Willie Wilson4, Jiahua Qian1, Andrea Carnie1, Nadya Tarasova5, Mikayel Mkrtichyan3, Jay A Berzofsky6, Theresa L Whiteside2, Samir N Khleif7.
Abstract
Constitutive activation of the KRAS oncogene in human malignancies is associated with aggressive tumor growth and poor prognosis. Similar to other oncogenes, KRAS acts in a cell-intrinsic manner to affect tumor growth or survival. However, we describe here a different, cell-extrinsic mechanism through which mutant KRAS contributes to tumor development. Tumor cells carrying mutated KRAS induced highly suppressive T cells, and silencing KRAS reversed this effect. Overexpression of the mutant KRAS(G12V)gene in wild-type KRAS tumor cells led to regulatory T-cell (Treg) induction. We also demonstrate that mutant KRAS induces the secretion of IL10 and transforming growth factor-β1 (both required for Treg induction) by tumor cells through the activation of the MEK-ERK-AP1 pathway. Finally, we report that inhibition of KRAS reduces the infiltration of Tregs in KRAS-driven lung tumorigenesis even before tumor formation. This cell-extrinsic mechanism allows tumor cells harboring a mutant KRAS oncogene to escape immune recognition. Thus, an oncogene can promote tumor progression independent of its transforming activity by increasing the number and function of Tregs. This has a significant clinical potential, in which targeting KRAS and its downstream signaling pathways could be used as powerful immune modulators in cancer immunotherapy. ©2016 American Association for Cancer Research.Entities:
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Year: 2016 PMID: 26880715 PMCID: PMC4884020 DOI: 10.1158/2326-6066.CIR-15-0241
Source DB: PubMed Journal: Cancer Immunol Res ISSN: 2326-6066 Impact factor: 11.151