Two Antagonistic Microtubule Targeting Drugs Act Synergistically to Kill Cancer Cells

Author:

Peronne LauralieORCID,Denarier EricORCID,Rai AnkitORCID,Prudent Renaud,Vernet Audrey,Suzanne Peggy,Ramirez-Rios Sacnicté,Michallet Sophie,Guidetti Mélanie,Vollaire Julien,Lucena-Agell DanielORCID,Ribba Anne-Sophie,Josserand Véronique,Coll Jean-LucORCID,Dallemagne PatrickORCID,Díaz J. FernandoORCID,Oliva María ÁngelaORCID,Sadoul Karin,Akhmanova AnnaORCID,Andrieux AnnieORCID,Lafanechère LaurenceORCID

Abstract

Paclitaxel is a microtubule stabilizing agent and a successful drug for cancer chemotherapy inducing, however, adverse effects. To reduce the effective dose of paclitaxel, we searched for pharmaceutics which could potentiate its therapeutic effect. We screened a chemical library and selected Carba1, a carbazole, which exerts synergistic cytotoxic effects on tumor cells grown in vitro, when co-administrated with a low dose of paclitaxel. Carba1 targets the colchicine binding-site of tubulin and is a microtubule-destabilizing agent. Catastrophe induction by Carba1 promotes paclitaxel binding to microtubule ends, providing a mechanistic explanation of the observed synergy. The synergistic effect of Carba1 with paclitaxel on tumor cell viability was also observed in vivo in xenografted mice. Thus, a new mechanism favoring paclitaxel binding to dynamic microtubules can be transposed to in vivo mouse cancer treatments, paving the way for new therapeutic strategies combining low doses of microtubule targeting agents with opposite mechanisms of action.

Funder

Institut National Du Cancer

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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