G3BP1 knockdown sensitizes U87 glioblastoma cell line to Bortezomib by inhibiting stress granules assembly and potentializing apoptosis

L. F. F. Bittencourt,Graziele L. Negreiros-Lima,Lirlandia P. Sousa,A. G. Silva,I. B. S. Souza,Rosy Iara Maciel de Azambuja Ribeiro,M. F. Dutra,R.F Silva,Ana Carolina Fialho Dias,Frederico M. Soriani,W. K. Martins,Lucíola S. Barcelos

G3BP1 knockdown sensitizes U87 glioblastoma cell line to Bortezomib by inhibiting stress granules assembly and potentializing apoptosis

2019

L. F. F. Bittencourt
Graziele L. Negreiros-Lima
Lirlandia P. Sousa
A. G. Silva
I. B. S. Souza
Rosy Iara Maciel de Azambuja Ribeiro
M. F. Dutra
R.F Silva
Ana Carolina Fialho Dias
Frederico M. Soriani
W. K. Martins
Lucíola S. Barcelos

Introduction Glioblastoma multiforme (GBM) is the most lethal form of gliomas. New therapies are currently in development to tackle treatment limitations such as chemotherapy resistance. One mechanism of resistance may be the stress granules (SG) assembly, a stress-related cellular response that allows cells to recruit and protect mRNAs during stress. SG are composed of various proteins, being G3BP1 a core element that enucleates and results in SG assembly. Here, we aimed to evaluate the effects of inhibiting the G3PB1 expression in the chemotherapeutical-induced cell death of the U87 glioblastoma cell line.

Keywords:

Angiogenesis
Cancer research
Apoptosis
Programmed cell death
U87
Bortezomib
Medicine
Stress granule
Gene knockdown
Cell culture
Flow cytometry
MTT assay
Temozolomide
Proteasome inhibitor

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