Reduction-sensitive platinum (IV)-prodrug nano-sensitizer with an ultra-high drug loading for efficient chemo-radiotherapy of Pt-resistant cervical cancer in vivo

Cisplatin is widely used in the chemoradiotherapy (CRT) of cervical cancers. However, despite the severe systemic side effects, the therapeutic efficacy of cisplatin is often compromised by the development of drug resistance, which is closely related to the elevated intracellular thiol-containing sp...

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Bibliographic Details
Published in:Journal of controlled release 2020-10, Vol.326, p.25-37
Main Authors: Luo, Kejun, Guo, Wenxuan, Yu, Yanting, Xu, Simeng, Zhou, Min, Xiang, Keqi, Niu, Kun, Zhu, Xianqi, Zhu, Guangying, An, Zheng, Yu, Qingsong, Gan, Zhihua
Format: Article
Language:English
Subjects:
Cervical cancer
Chemoradiotherapy
Cisplatin resistance
Glutathione
Pt(IV)-prodrug NPs
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Summary:Cisplatin is widely used in the chemoradiotherapy (CRT) of cervical cancers. However, despite the severe systemic side effects, the therapeutic efficacy of cisplatin is often compromised by the development of drug resistance, which is closely related to the elevated intracellular thiol-containing species (especially glutathione (GSH)) and the adenosine triphosphate (ATP)-dependent glutathione S-conjugate pumps. The construction of a safe and redox-sensitive nano-sensitizer with high disulfide density and high Pt(IV) prodrug loading capacity (up to 16.50% Pt and even higher), as described herein, is a promising way to overcome the cisplatin resistance and enhance the CRT efficacy. The optimized nanoparticles (NPs) (referred to as SSCV5) with moderate Pt loading (7.62% Pt) and median size (c.a. 40 nm) was screened out and used for further biological evaluation. Compared with free cisplatin, more drugs could be transported and released inside the cisplatin resistant cells (Hela-CDDP) by SSCV5 NPs. With the synergistic effect of GSH scavenging and mitochondrial damage, SSCV5 NPs can easily reverse the cisplatin resistance. Moreover, the higher nucleus DNA binding Pt content of SSCV5 NPs not only caused the DNA damage and apoptosis of Hela-CDDP cells but also sensitized these cells to X-Ray radiation. The in vivo safety and efficacy results showed that SSCV5 NPs effectively accumulated inside tumor and inhibited the growth of cisplatin resistant xenograft models while alleviating the serious side effect associated with cisplatin (the maximum tolerated cisplatin equivalent of single injection is higher than 20 mg/kg body weight). The intervention of exogenous radiation further improved the anticancer efficacy of SSCV5 NPs and caused the shrinkage of tumor volume, thus making this safe and facile nano-sensitizer a promising route for the neoadjuvant CRT of cervical cancers. [Display omitted] •Reduction sensitive nano-carrier quantitatively encapsulated prodrug molecules;•Prodrug nanomedicine greatly improved the safety profiles of cisplatin;•Prodrug strategies overcame cisplatin resistance by GSH consumption and mitochondrial targeting;•Prodrug nano-sensitizer enabled efficient chemoradiotherapy in cisplatin-resistant cancer model.
ISSN:0168-3659
1873-4995
DOI:10.1016/j.jconrel.2020.06.005