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通过雌激素受体递送米托蒽醌的雌酮靶向脂质体:体内靶向效果、抗肿瘤活性、急性毒性和药代动力学。

Estrone-targeted liposomes for mitoxantrone delivery via estrogen receptor: In vivo targeting efficacy, antitumor activity, acute toxicity and pharmacokinetics.

作者信息

Xu Guoxing, Tang Huan, Chen Jinglin, Zhu Ming, Xie Yizhuo, Li Yao, Hao Qiang, Sun Yuxin, Cong Dengli, Meng Qin, Ren Zhihui, Li Qianwen, Bao Han, Lv Zhe, Li Yan, Pei Jin

机构信息

School of Pharmaceutical Sciences, Jilin University, Changchun130021, Jilin, China.

School of Pharmaceutical Sciences, Jilin University, Changchun130021, Jilin, China.

出版信息

Eur J Pharm Sci. 2021 Jun 1;161:105780. doi: 10.1016/j.ejps.2021.105780. Epub 2021 Mar 2.

DOI:10.1016/j.ejps.2021.105780
PMID:33667664
Abstract

Estrogen receptor (ER) is a potential target receptor for ER-positive cancer therapy including breast cancers, gastric cancers, and human acute myeloblastic leukaemia. In order to reduce the side-effects of mitoxantrone (MTO), estrone-targeted liposomes for MTO delivery via ER were designed for selectively targeting cancer cells. In previous studies, MTO-loaded estrogen receptor targeted and sterically stabilized liposome (ES-SSL-MTO; ES: estrone, is known to bind the ER) had been synthesized and showed a very high antiproliferative effect with IC value of 0.7 ng/mL. Based on these, further studies including in vivo targeting efficacy and antitumor activity, acute toxicity and pharmacokinetics of MTO liposomes were carried out. The results showed SSL (sterically stabilized liposome, PEGylated liposome, PEG: Polyethylene Glycol) could reduce drug metabolism, improve the stability of liposomes, prolong in vivo circulation time of drugs, reduce the toxicity of MTO. But SSL could not be enriched in tumor tissues. However, estrone (ES)-targeted liposomes could be delivered to tumor sites. ES-SSL could effectively enter into ER-expressing tumor cellsand be accumulated, prolong the circulation time in vivo, reduce side effects of drug. ES-SSL-MTO could provide higher bioavailability than MTO, enhance the anti-tumor effect and the safety of MTO, reduce the toxicity and side effects of MTO and improve the therapeutic effect of MTO. These facts proved ES-SSL is a useful tumor-targeting drug delivery system for MTO.

摘要

雌激素受体(ER)是雌激素受体阳性癌症治疗的潜在靶点,这些癌症包括乳腺癌、胃癌和人类急性髓细胞白血病。为了降低米托蒽醌(MTO)的副作用,设计了通过雌激素受体将米托蒽醌靶向递送至肿瘤部位的雌酮靶向脂质体。在先前的研究中,已合成了负载米托蒽醌的雌激素受体靶向且空间稳定的脂质体(ES-SSL-MTO;ES:雌酮,已知可与雌激素受体结合),其IC值为0.7 ng/mL,显示出非常高的抗增殖作用。基于此,进一步开展了包括米托蒽醌脂质体的体内靶向效果和抗肿瘤活性、急性毒性及药代动力学等研究。结果表明,空间稳定脂质体(SSL,聚乙二醇化脂质体,PEG:聚乙二醇)可减少药物代谢,提高脂质体稳定性,延长药物在体内的循环时间,降低米托蒽醌的毒性。但空间稳定脂质体无法在肿瘤组织中富集。然而,雌酮(ES)靶向脂质体可被递送至肿瘤部位。ES-SSL可有效进入表达雌激素受体的肿瘤细胞并蓄积,延长其在体内的循环时间,降低药物副作用。ES-SSL-MTO比米托蒽醌具有更高的生物利用度,增强了米托蒽醌的抗肿瘤效果和安全性,降低了米托蒽醌的毒性和副作用,提高了米托蒽醌的治疗效果。这些事实证明,ES-SSL是一种用于米托蒽醌的有效的肿瘤靶向给药系统。

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