Autophagy Inhibition Improves the Efficacy of Curcumin/temozolomide Combination Therapy in Glioblastomas

Overview

Journal Cancer Lett

Specialty Oncology

Date 2014 Dec 28

PMID 25542083

Citations 85

Authors

Alfeu Zanotto-Filho

Elizandra Braganhol

Karina Klafke

Fabricio Figueiro

Silvia Resende Terra

Francis Jackson Paludo

Maurilio Morrone

Ivi Juliana Bristot

Ana Maria Battastini

Cassiano Mateus Forcelini

Alexander James Roy Bishop

Daniel Pens Gelain

Jose Claudio Fonseca Moreira

Affiliations

Soon will be listed here.

Abstract

Glioblastoma is a devastating primary brain tumor resistant to conventional therapies. In this study, we tested the efficacy of combining temozolomide with curcumin, a phytochemical known to inhibit glioblastoma growth, and investigated the mechanisms involved. The data showed that synergy between curcumin and temozolomide was not achieved due to redundant mechanisms that lead to activating protective autophagy both in vitro and in vivo. Autophagy preceded apoptosis, and blocking this response with autophagy inhibitors (3-methyl-adenine, ATG7 siRNA and chloroquine) rendered cells susceptible to temozolomide and curcumin alone or combinations by increasing apoptosis. While curcumin inhibited STAT3, NFκB and PI3K/Akt to affect survival, temozolomide-induced autophagy relied on the DNA damage response and repair components ATM and MSH6, as well as p38 and JNK1/2. However, the most interesting observation was that both temozolomide and curcumin required ERK1/2 to induce autophagy. Blocking this ERK1/2-mediated temozolomide and curcumin induced autophagy with resveratrol, a blood-brain barrier permeable drug, improved temozolomide/curcumin efficacy in brain-implanted tumors. Overall, the data presented demonstrate that autophagy impairs the efficacy of temozolomide/curcumin, and inhibiting this phenomenon could provide novel opportunities to improve brain tumor treatment.

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