Smart stimuli-responsive carrier-free nanoassembly of SN38 prodrug as efficient chemotherapeutic nanomedicine

Guanting Li, Qianhui Jin, Fengli Xia, Shuwen Fu, Xuanbo Zhang, Hongying Xiao, Chutong Tian, Qingzhi Lv, J. Sun, Zhonggui He, Bingjun Sun
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引用次数: 2

Abstract

The compound 7-ethyl-10-hydroxy-camptothecin (SN38) is a broad-spectrum antitumor agent whose applications are greatly limited by its poor solubility. Therefore, irinotecan, the hydrophilic derived prodrug of SN38, has been developed as the commercial formulation Campto® for colorectal cancer. However, only 1% to 0.1% of irinotecan is converted to active SN38 in vivo, thus leading to unsatisfactory antitumor activity in clinical settings. Herein, we report a smart stimuli-responsive SN38 prodrug nanoassembly for efficient cancer therapy. First, SN38 was conjugated with an endogenous lipid, cholesterol (CST), via a redox dual-responsive disulfide bond (namely SN38-SS-CST). The prodrug self-assembled into uniform prodrug nanoassemblies with good colloidal stability and ultrahigh drug loading. SN38-SS-CST NPs released sufficient SN38 in the redox environments of tumor cells but remained intact in normal tissues. Finally, SN38-SS-CST NPs potently inhibited the growth of colon cancer without causing systemic toxicity, thus indicating their promise as a translational chemotherapeutic nanomedicine.
SN38前药作为高效化疗纳米药物的智能刺激响应无载体纳米组装
化合物7-乙基-10-羟基喜树碱(SN38)是一种广谱抗肿瘤剂,其溶解度低,应用受到很大限制。因此,SN38的亲水性前药伊立替康已被开发为用于结直肠癌癌症的商业制剂Campto®。然而,只有1%至0.1%的伊立替康在体内转化为活性SN38,因此在临床环境中导致不令人满意的抗肿瘤活性。在此,我们报道了一种用于有效癌症治疗的智能刺激响应SN38前药纳米组件。首先,通过氧化还原双反应二硫键(即SN38-SS-CST)将SN38与内源性脂质胆固醇(CST)偶联。前药自组装成均匀的前药纳米组装体,具有良好的胶体稳定性和超高的载药量。SN38-SS-CST NP在肿瘤细胞的氧化还原环境中释放了足够的SN38,但在正常组织中保持完整。最后,SN38-SS-CST NP有效抑制结肠癌的生长,而不会引起全身毒性,因此表明其有望成为转化化疗纳米药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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