用于重置巨噬细胞极化的多肽免疫调节剂的De Novo设计和合成。

Q2 Agricultural and Biological Sciences
生物设计研究(英文) Pub Date : 2023-02-07 eCollection Date: 2023-01-01 DOI:10.34133/bdr.0006
Na Kong, Hongru Ma, Zhongji Pu, Fengju Wan, Dongfang Li, Lei Huang, Jiazhang Lian, Xingxu Huang, Shengjie Ling, Haoran Yu, Yuan Yao
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引用次数: 0

摘要

在免疫研究或肿瘤治疗中,调节细胞外基质微环境对于实现所需的巨噬细胞表型至关重要。结合从头蛋白质设计和生物合成技术,我们设计了一种仿生多肽自组装纳米免疫调节剂,以触发特定巨噬细胞表型的激活。它是由(​GGS​GGP​GGG​帕斯​AAA​NSA​SRA​TSN​SP)n、来自胶原的RGD基序和来自层粘连蛋白的IKVAV基序。这些结构域的组合使仿生多肽能够组装成细胞外基质样纳米纤维,为巨噬细胞创造细胞外基质状环境。此外,改变浓度进一步提供了微调巨噬细胞极化的简单途径,这通过将肿瘤相关的巨噬细胞免疫反应精确重置为M1样表型来增强抗肿瘤免疫反应,M1样表型通常被认为是杀瘤巨噬细胞,主要是抗肿瘤和免疫促进。与基于金属或合成聚合物的纳米颗粒不同,这种基于多肽的纳米材料表现出优异的生物相容性、高效性和免疫调节效果的精确可调性。这些令人鼓舞的发现激励我们在未来继续研究癌症免疫疗法的应用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
De Novo Design and Synthesis of Polypeptide Immunomodulators for Resetting Macrophage Polarization.

Modulating the extracellular matrix microenvironment is critical for achieving the desired macrophage phenotype in immune investigations or tumor therapy. Combining de novo protein design and biosynthesis techniques, herein, we designed a biomimetic polypeptide self-assembled nano-immunomodulator to trigger the activation of a specific macrophage phenotype. It was intended to be made up of (​GGS​GGP​GGG​PAS​AAA​NSA​SRA​TSN​SP)n, the RGD motif from collagen, and the IKVAV motif from laminin. The combination of these domains allows the biomimetic polypeptide to assemble into extracellular matrix-like nanofibrils, creating an extracellular matrix-like milieu for macrophages. Furthermore, changing the concentration further provides a facile route to fine-tune macrophage polarization, which enhances antitumor immune responses by precisely resetting tumor-associated macrophage immune responses into an M1-like phenotype, which is generally considered to be tumor-killing macrophages, primarily antitumor, and immune-promoting. Unlike metal or synthetic polymer-based nanoparticles, this polypeptide-based nanomaterial exhibits excellent biocompatibility, high efficacy, and precise tunability in immunomodulatory effectiveness. These encouraging findings motivate us to continue our research into cancer immunotherapy applications in the future.

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来源期刊
CiteScore
3.90
自引率
0.00%
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审稿时长
12 weeks
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