| Literature DB >> 26242912 |
Sanguine Byun1, Semi Lim2, Ji Young Mun3, Ki Hyun Kim4, Timothy R Ramadhar5, Lee Farrand6, Seung Ho Shin7, N R Thimmegowda8, Hyong Joo Lee2, David A Frank9, Jon Clardy10, Sam W Lee11, Ki Won Lee12.
Abstract
Bioactive phytochemicals can suppress the growth of malignant cells, and investigation of the mechanisms responsible can assist in the identification of novel therapeutic strategies for cancer therapy. Ginger has been reported to exhibit potent anti-cancer effects, although previous reports have often focused on a narrow range of specific compounds. Through a direct comparison of various ginger compounds, we determined that gingerenone A selectively kills cancer cells while exhibiting minimal toxicity toward normal cells. Kinase array screening revealed JAK2 and S6K1 as the molecular targets primarily responsible for gingerenone A-induced cancer cell death. The effect of gingerenone A was strongly associated with relative phosphorylation levels of JAK2 and S6K1, and administration of gingerenone A significantly suppressed tumor growth in vivo. More importantly, the combined inhibition of JAK2 and S6K1 by commercial inhibitors selectively induced apoptosis in cancer cells, whereas treatment with either agent alone did not. These findings provide rationale for dual targeting of JAK2 and S6K1 in cancer for a combinatorial therapeutic approach.Entities:
Keywords: JAK2 signaling; S6K1 signaling; anticancer; cancer biology; cell death; cell signaling; chemoprevention; gingerenone A; small molecule
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Year: 2015 PMID: 26242912 PMCID: PMC4583007 DOI: 10.1074/jbc.M115.662445
Source DB: PubMed Journal: J Biol Chem ISSN: 0021-9258 Impact factor: 5.157