The CNS-penetrating taxane drug TPI 287 potentiates antiglioma activity of the AURKA inhibitor alisertib in vivo.

Müge SakBrian J WilliamsCory T ZumbarLandon TeerMustafa N G Al-KawaazAastha KakarAndrew J HeyMegan J WilsonLeslie M SchierJoseph ChenNorman L Lehman

Published in: Cancer chemotherapy and pharmacology (2023)

Results suggest that apoptosis is the dominant mechanism of potentiation of GBM growth inhibition by alisertib + TPI 287, in part through effects on Bcl-2 family proteins, providing a rationale for further laboratory testing of an AURKA inhibitor plus TPI 287 as a potential therapy against GBM.

Keyphrases

oxidative stress
endoplasmic reticulum stress
cell death
blood brain barrier
clinical trial
cell cycle arrest
risk assessment
mesenchymal stem cells
metastatic breast cancer
signaling pathway
chemotherapy induced