Computer-Aided Design of Lasso-like Self-Assembling Anticancer Peptides with Multiple Functions for Targeted Self-Delivery and Cancer Treatments

癌症研究 计算生物学 癌症 计算机科学 纳米技术 材料科学 生物 医学 内科学
作者
Pengfei Pei,Long Chen,Ruru Fan,Xirui Zhou,Shan Feng,Hangrui Liu,Quanqiang Guo,Huiwei Yin,Qiang Zhang,Fude Sun,Liang Peng,Peng Wei,Chengzhi He,Renzhong Qiao,Zai Wang,Shi‐Zhong Luo
出处
期刊:ACS Nano [American Chemical Society]
卷期号:16 (9): 13783-13799 被引量:14
标识
DOI:10.1021/acsnano.2c01014
摘要

Anticancer peptides are promising drug candidates for cancer treatment, but the short circulation time and low delivery efficiency limit their clinical applications. Herein, we designed several lasso-like self-assembling anticancer peptides (LASAPs) integrated with multiple functions by a computer-aided approach. Among these LASAPs, LASAP1 (CRGDKGPDCGKAFRRFLGALFKALSHLL, 1–9 disulfide bond) was determined to be superior to the others because it can self-assemble into homogeneous nanoparticles and exhibits improved stability in serum. Thus, LASAP1 was chosen for proving the design idea. LASAP1 can self-assemble into nanoparticles displaying iRGD on the surface because of its amphiphilic structure and accumulate to the tumor site after injection because of the EPR effect and iRGD targeting to αVβ3 integrin. The nanoparticles could disassemble in the acidic microenvironment of the solid tumor, and cleaved by the overexpressed hK2, which was secreted by prostate tumor cells, to release the effector peptide PTP-7b (FLGALFKALSHLL), which was further activated by the acidic pH. Therefore, LASAP1 could target the orthotopic prostate tumor in the model mice after intraperitoneal injection and specifically inhibit tumor growth, with low systematic toxicity. Combining the multiple targeting functions, LASAP1 represents a promising design of self-delivery of peptide drugs for targeted cancer treatments.
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