pH-dependent reversibly activatable cell-penetrating peptides improve the antitumor effect of artemisinin-loaded liposomes

纳米载体 脂质体 青蒿素 化学 体内 细胞毒性 药理学 药品 体外 药物输送 细胞穿透肽 细胞 生物化学 医学 免疫学 有机化学 生物技术 生物 疟疾 恶性疟原虫
作者
Yinglan Yu,Chang Zu,Dongsheng He,Yanan Li,Qinying Chen,Qian Chen,Huimin Wang,Ruijuan Wang,Birendra Chaurasiya,Jennica L. Zaro,Yiran Wang,Jiasheng Tu,Chunmeng Sun
出处
期刊:Journal of Colloid and Interface Science [Elsevier BV]
卷期号:586: 391-403 被引量:46
标识
DOI:10.1016/j.jcis.2020.10.103
摘要

Artemisinin (ART) is well known as an antimalarial drug, and it can also be used to treat inflammation as well as cancer. Although many researchers have reported the antitumor activity of ART, most of these studies were investigated in vitro. In addition, ART is sparingly soluble in water, limiting its clinical relevance in drug development. Based on the data from our preliminary study, ART is not cytotoxic at low micromolar concentrations. Thus, we hypothesized that smart nanocarriers are beneficial for not only increasing the solubility of ART but also elevating the concentration of the drug at the target, thereby inducing the ideal antitumor effect. In this article, a reversibly activatable cell-penetrating peptide ((HE)10-G5-R6 or HE-R6) was introduced to modify artemisinin (ART)-loaded liposomes (ART-Lip-HE-R6) against tumors, and in vitro and in vivo performance were investigated. ART-Lip-HE-R6 exhibited sustained release under different pH conditions. The internalization and cytotoxicity of liposomes were enhanced at low pH, i.e., 6.5, after modification with HE-R6 versus nonmodified liposomes. Moreover, a longer retention time in tumors could be observed in the ART-Lip-HE-R6 group, followed by higher efficiency of tumor suppression. In conclusion, Lip-HE-R6 might be a promising delivery system for ART in cancer therapy.
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