Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model

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Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model Publisher Pubmed

Ramezani S² ; Vousooghi N^{1, 3, 4} ; Ramezani Kapourchali F⁵ ; Joghataei MT^{6, 7}

Source: Apoptosis Published:2017

Abstract

Bevacizumab (BVZ) as an antiangiogenesis therapy leads to a transient therapeutic efficacy in high-grade glioma. However, the proapoptotic potential of BVZ has not been well elucidated, yet. There is also a tumor resistance to BVZ that is linked to post-treatment metalloproteinases and AKT activities. Herein, the association between therapeutic efficacy and putative proapoptotic activity of low-dose BVZ either alone or in combination with a specific inhibitor of AKT called perifosine (PRF), in a glioma model was investigated. BALB/c mice bearing C6 glioma tumor were treated with BVZ and PRF either alone or combined for 13 days (n = 11/group). At the end of treatments, apoptosis, proliferation and vascular density, in the xenografts (3/group) were detected by TUNEL staining, Ki67 and CD31 markers, respectively. Relative levels of cleaved-caspase3, phospho-AKT (Ser473) and matrix metalloproteinase2 (MMP2) were measured using western blotting. PRF and BVZ separately slowed down tumor growth along with the cell apoptosis induction associated with a profound increase in caspase3 activity through an AKT inhibition-related pathway for PRF but not BVZ. Unlike PRF, BVZ significantly increased the intratumor MMP2 and phospho-AKT (Ser473) levels coupled with the slight antiproliferative and significant antivascular effects. Co-administration of PRF and BVZ versus monotherapies potentiated the proapoptotic effects and reversed the BVZ-induced upregulation of phospho-AKT (Ser473) and MMP2 levels in C6 xenografts, leading to the optimal antiproliferative activity and tumor growth regression and longer survival. In conclusion, BVZ plus PRF renders a paramount proapoptotic effect, leading to a major therapeutic efficacy and might be a new substitute for GBM therapy in the clinic. © 2017, Springer Science+Business Media, LLC.

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Style	Citing Format
MLA	Ramezani S, et al.. "Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model." Apoptosis, vol. 22, no. 8, 2017, pp. 1025-1034.
APA	Ramezani S, Vousooghi N, Ramezani Kapourchali F, Joghataei MT (2017). Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model. Apoptosis, 22(8), 1025-1034.
Chicago	Ramezani S, Vousooghi N, Ramezani Kapourchali F, Joghataei MT. "Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model." Apoptosis 22, no. 8 (2017): 1025-1034.
Harvard	Ramezani S et al. (2017) 'Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model', Apoptosis, 22(8), pp. 1025-1034.
Vancouver	Ramezani S, Vousooghi N, Ramezani Kapourchali F, Joghataei MT. Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model. Apoptosis. 2017;22(8):1025-1034.
BibTex	@article{ author = {Ramezani S and Vousooghi N and Ramezani Kapourchali F and Joghataei MT}, title = {Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model}, journal = {Apoptosis}, volume = {22}, number = {8}, pages = {1025-1034}, year = {2017} }
RIS	TY - JOUR AU - Ramezani S AU - Vousooghi N AU - Ramezani Kapourchali F AU - Joghataei MT TI - Perifosine Enhances Bevacizumab-Induced Apoptosis and Therapeutic Efficacy by Targeting Pi3k/Akt Pathway in a Glioblastoma Heterotopic Model JO - Apoptosis VL - 22 IS - 8 SP - 1025 EP - 1034 PY - 2017 ER -

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