Enhanced anti-tumor activity in mice with temozolomide-resistant human glioblastoma cell line-derived xenograft using sn-38-incorporated polymeric microparticle

Tao Chieh Yang, Shih Jung Liu, Wei Lun Lo, Shu Mei Chen, Ya Ling Tang, Yuan Yun Tseng*

*此作品的通信作者

研究成果: 期刊稿件文章同行評審

4 引文 斯高帕斯(Scopus)

摘要

Glioblastoma multiforme (GBM) has remained one of the most lethal and challenging cancers to treat. Previous studies have shown encouraging results when irinotecan was used in combination with temozolomide (TMZ) for treating GBM. However, irinotecan has a narrow therapeutic index: a slight dose increase in irinotecan can induce toxicities that outweigh its therapeutic benefits. SN-38 is the active metabolite of irinotecan that accounts for both its anti-tumor efficacy and toxicity. In our previous paper, we showed that SN-38 embedded into 50:50 biodegradable poly[(d,l)-lactide-co-glycolide] (PLGA) microparticles (SMPs) provides an efficient delivery and sustained release of SN-38 from SMPs in the brain tissues of rats. These properties of SMPs give them potential for therapeutic application due to their high efficacy and low toxicity. In this study, we tested the anti-tumor activity of SMP-based interstitial chemotherapy combined with TMZ using TMZ-resistant human glioblastoma cell line-derived xenograft models. Our data suggest that treatment in which SMPs are combined with TMZ reduces tumor growth and extends survival in mice bearing xenograft tumors derived from both TMZ-resistant and TMZ-sensitive human glioblastoma cell lines. Our findings demonstrate that combining SMPs with TMZ may have potential as a promising strategy for the treatment of GBM.

原文英語
文章編號5557
期刊International Journal of Molecular Sciences
22
發行號11
DOIs
出版狀態已出版 - 01 06 2021

文獻附註

Publisher Copyright:
© 2021 by the authors. Licensee MDPI, Basel, Switzerland.

指紋

深入研究「Enhanced anti-tumor activity in mice with temozolomide-resistant human glioblastoma cell line-derived xenograft using sn-38-incorporated polymeric microparticle」主題。共同形成了獨特的指紋。

引用此