The fatty acid synthase inhibitor triclosan: repurposing an anti-microbial agent for targeting prostate cancer

三氯生 脂肪酸合酶 药物重新定位 奥利斯特 前列腺癌 药理学 细胞毒性 生长抑制 癌症研究 癌症 化学 细胞生长 医学 生物化学 药品 内科学 体外 肥胖 病理 减肥
作者
Martin C. Sadowski,Rebecca H. Pouwer,Jennifer H. Gunter,Amy A. Lubik,Ronald J. Quinn,Colleen C. Nelson
出处
期刊:Oncotarget [Impact Journals LLC]
卷期号:5 (19): 9362-9381 被引量:107
标识
DOI:10.18632/oncotarget.2433
摘要

Inhibition of FASN has emerged as a promising therapeutic target in cancer, and numerous inhibitors have been investigated. However, severe pharmacological limitations have challenged their clinical testing. The synthetic FASN inhibitor triclosan, which was initially developed as a topical antibacterial agent, is merely affected by these pharmacological limitations. Yet, little is known about its mechanism in inhibiting the growth of cancer cells. Here we compared the cellular and molecular effects of triclosan in a panel of eight malignant and non-malignant prostate cell lines to the well-known FASN inhibitors C75 and orlistat, which target different partial catalytic activities of FASN. Triclosan displayed a superior cytotoxic profile with a several-fold lower IC50 than C75 or orlistat. Structure-function analysis revealed that alcohol functionality of the parent phenol is critical for inhibitory action. Rescue experiments confirmed that end product starvation was a major cause of cytotoxicity. Importantly, triclosan, C75 and orlistat induced distinct changes to morphology, cell cycle, lipid content and the expression of key enzymes of lipid metabolism, demonstrating that inhibition of different partial catalytic activities of FASN activates different metabolic pathways. These finding combined with its well-documented pharmacological safety profile make triclosan a promising drug candidate for the treatment of prostate cancer.

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