Orlistat As a FASN Inhibitor and Multitargeted Agent for Cancer Therapy

Overview

Journal Expert Opin Investig Drugs

Specialty Pharmacology

Date 2018 May 4

PMID 29723075

Citations 55

Authors

Alejandro Schcolnik-Cabrera

Alma Chavez-Blanco

Guadalupe Dominguez-Gomez

Lucia Taja-Chayeb

Rocio Morales-Barcenas

Catalina Trejo-Becerril

Enrique Perez-Cardenas

Aurora Gonzalez-Fierro

Alfonso Duenas-Gonzalez

Affiliations

Soon will be listed here.

Abstract

Introduction: Cancer cells have increased glycolysis and glutaminolysis. Their third feature is increased de novo lipogenesis. As such, fatty acid (FA) synthesis enzymes are over-expressed in cancer and their depletion causes antitumor effects. As fatty acid synthase (FASN) plays a pivotal role in this process, it is an attractive target for cancer therapy.

Areas Covered: This is a review of the lipogenic phenotype of cancer and how this phenomenon can be exploited for cancer therapy using inhibitors of FASN, with particular emphasis on orlistat as a repurposing drug.

Expert Opinion: Disease stabilization only has been observed with a highly selective FASN inhibitor used as a single agent in clinical trials. It is too early to say whether the absence of tumor responses other than stabilization results because even full inhibition of FASN is not enough to elicit antitumor responses. The FASN inhibitor orlistat is a 'dirty' drug with target-off actions upon at least seven targets with a proven role in tumor biology. The development of orlistat formulations suited for its intravenous administration is a step ahead to shed light on the concept that drug promiscuity can or not be a virtue.

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