基于多肽自组装的仿生纳米材料在免疫治疗中的应用。

Zhuan Wen, Zhang-Zhi Song, Ming-Ze Cai, Ni-Yuan Zhang, Hao-Ze Li, Yang Yang, Qian-Ting Wang, Muhammad Hamza Ghafoor, Hong-Wei An, Hao Wang
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引用次数: 0

摘要

癌症仍然是全世界患者死亡的主要原因,其发病率继续上升。由于免疫治疗在作用机制上与常规放疗和靶向抗肿瘤药物有很大的不同,因此正在迅速发展。在过去的几十年里,许多生物材料被设计和制备用于构建调节免疫系统对抗癌症的治疗平台。利用生物材料的免疫治疗平台可以通过优化治疗剂的递送、减少循环过程中的药物损失和放大免疫调节作用来显着提高治疗效果。肿瘤复杂的生理屏障,加上不良的免疫环境,如浸润不足、脱靶效应和免疫抑制,已经成为阻碍肿瘤药物治疗有效性的重要障碍。然而,目前的研究大多致力于开发复杂的免疫调节剂,通过装载药物或佐剂来发挥免疫调节功能,而忽略了肿瘤复杂的生理屏障和不良的免疫环境。与传统的生物材料相比,基于多肽原位自组装的仿生纳米材料具有良好的生物相容性、生物可降解性和生物活性等功能特征,已成为一种新的有效的癌症免疫治疗工具。本文综述了基于多肽原位自组装的仿生纳米材料在肿瘤免疫治疗中的最新研究进展。首先,我们对仿生肽纳米材料的结构类型进行了分类,并阐明了其内在驱动力。随后,我们深入研究了这些肽仿生纳米材料的原位自组装策略,突出了它们在免疫治疗中的优势。此外,我们详细介绍了这些仿生纳米材料在抗原呈递和免疫微环境调节中的应用。最后,我们总结了基于多肽原位自组装的仿生纳米材料在免疫治疗中的临床翻译的挑战和前景发展。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Biomimetic Nanomaterials Based on Peptide In Situ Self-Assembly for Immunotherapy Applications.

Cancer remains the leading cause of patient death worldwide and its incidence continues to rise. Immunotherapy is rapidly developing due to its significant differences in the mechanism of action from conventional radiotherapy and targeted antitumor drugs. In the past decades, many biomaterials have been designed and prepared to construct therapeutic platforms that modulate the immune system against cancer. Immunotherapeutic platforms utilizing biomaterials can markedly enhance therapeutic efficacy by optimizing the delivery of therapeutic agents, minimizing drug loss during circulation, and amplifying immunomodulatory effects. The intricate physiological barriers of tumors, coupled with adverse immune environments such as inadequate infiltration, off-target effects, and immunosuppression, have emerged as significant obstacles impeding the effectiveness of oncology drug therapy. However, most of the current studies are devoted to the development of complex immunomodulators that exert immunomodulatory functions by loading drugs or adjuvants, ignoring the complex physiological barriers and adverse immune environments of tumors. Compared with conventional biomaterials, biomimetic nanomaterials based on peptide in situ self-assembly with excellent functional characteristics of biocompatibility, biodegradability, and bioactivity have emerged as a novel and effective tool for cancer immunotherapy. This article presents a comprehensive review of the latest research findings on biomimetic nanomaterials based on peptide in situ self-assembly in tumor immunotherapy. Initially, we categorize the structural types of biomimetic peptide nanomaterials and elucidate their intrinsic driving forces. Subsequently, we delve into the in situ self-assembly strategies of these peptide biomimetic nanomaterials, highlighting their advantages in immunotherapy. Furthermore, we detail the applications of these biomimetic nanomaterials in antigen presentation and modulation of the immune microenvironment. In conclusion, we encapsulate the challenges and prospective developments of biomimetic nanomaterials based on peptide in situ self-assembly for clinical translation in immunotherapy.

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