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增强源自伴孢菌素-2 的变体(Mpp46Aa1)对癌细胞系的细胞毒性和促凋亡作用。

Enhancing the Cytotoxicity and Apoptotic Efficacy of Parasporin-2-Derived Variants (Mpp46Aa1) on Cancer Cell Lines.

机构信息

Facultad de Ciencias Médicas y de la Salud, Instituto de Investigación MASIRA, Universidad de Santander, Bucaramanga 680002, Colombia.

Department of Pathology and Medical Biology, University Medical Center Groningen, University of Groningen, 9700 AB Groningen, The Netherlands.

出版信息

Toxins (Basel). 2024 Sep 25;16(10):415. doi: 10.3390/toxins16100415.

DOI:10.3390/toxins16100415
PMID:39453191
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11511244/
Abstract

Parasporin PS2Aa1, recently renamed Mpp46Aa1, is an anti-cancer protein known for its selectivity against various human cancer cell lines. We genetically modified native PS2Aa1 to create a library of approximately 100 mutants. From this library, we selected promising mutants based on their half-maximal inhibitory concentration (IC) and sequence variations. In this study, Variant 3-35, with the G257V substitution, demonstrated increased cytotoxicity and selectivity against the colon cancer cell line SW480. Conversely, Variant N65, featuring substitutions N92D, K175R, and S218G, yielded the most favorable results against the cancer cell lines SW-620, MOLT-4, and Jurkat. The caspase 3/7 and 9, Annexin V-Cy3 and 6-GFDA activities, and, most notably, mitochondrial membrane permeabilization assays confirmed the apoptotic marker elevation. These findings indicate that residues 92, 175, 218, and 257 may play a critical role in the cytotoxic activity and selectivity. We successfully obtained genetically improved variants with substitutions at these key amino acid positions. Additionally, we conducted molecular dynamic simulations to explore the potential interactions between PS2Aa1 and the CD59 GPI-anchored protein. The simulation results revealed that residues 57, 92, and 101 were consistently present, suggesting their possible significance in the interactions between parasporin and the CD59 protein.

摘要

副杀菌肽 PS2Aa1(最近更名为 Mpp46Aa1)是一种抗癌蛋白,因其对多种人类癌细胞系具有选择性而闻名。我们对天然 PS2Aa1 进行基因改造,创建了一个大约 100 个突变体的文库。从这个文库中,我们根据半抑制浓度(IC)和序列变化选择了有前途的突变体。在这项研究中,具有 G257V 取代的变体 3-35 对结肠癌 SW480 细胞系表现出增强的细胞毒性和选择性。相反,具有 N92D、K175R 和 S218G 取代的变体 N65 对 SW-620、MOLT-4 和 Jurkat 癌细胞系产生了最有利的结果。Caspase 3/7 和 9、Annexin V-Cy3 和 6-GFDA 活性,特别是线粒体膜通透性测定证实了凋亡标志物的升高。这些发现表明残基 92、175、218 和 257 可能在细胞毒性活性和选择性中发挥关键作用。我们成功获得了在这些关键氨基酸位置具有取代的遗传改良变体。此外,我们进行了分子动力学模拟,以探索 PS2Aa1 与 CD59 GPI-锚定蛋白之间的潜在相互作用。模拟结果表明残基 57、92 和 101 始终存在,这表明它们在副杀菌肽与 CD59 蛋白之间的相互作用中可能具有重要意义。

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