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光触发原位凝胶化以实现通过重复刺激的稳健光动力免疫治疗。

Light-Triggered In Situ Gelation to Enable Robust Photodynamic-Immunotherapy by Repeated Stimulations.

机构信息

Institute of Functional Nano and Soft Materials (FUNSOM), Jiangsu Key Laboratory for Carbon-Based Functional Materials and Devices, Soochow University, Suzhou, Jiangsu, 215123, China.

出版信息

Adv Mater. 2019 Jun;31(24):e1900927. doi: 10.1002/adma.201900927. Epub 2019 Apr 22.

DOI:10.1002/adma.201900927
PMID:31012164
Abstract

Photodynamic therapy (PDT) has shown the potential of triggering systemic antitumor immune responses. However, while the oxygen-deficient hypoxic tumor microenvironment is a factor that limits the PDT efficacy, the immune responses after conventional PDT usually are not strong enough to eliminate metastatic tumors. Herein, a light-triggered in situ gelation system containing photosensitizer-modified catalase together with poly(ethylene glycol) double acrylate (PEGDA) as the polymeric matrix is designed. Immune adjuvant nanoparticles are further introduced into this system to trigger robust antitumor immune responses after PDT. Following local injection of the mixed precursor solution into tumors and the subsequent light exposure, polymerization of PEGDA can be initiated to induce in situ gelation. Such hybrid hydrogel with long-term tumor retention of various agents and the ability to enable persistent tumor hypoxia relief can enable multiple rounds of PDT, which results in significantly enhanced immune responses by multiround stimulation. Further combination of such gel-based multiround PDT with anticytotoxic T-lymphocyte antigen-4 checkpoint blockade offers not only the abscopal effect to inhibit growth of distant tumors but also effective long-term immune memory protection from rechallenged tumors. Therefore, such a light-triggered in situ gelation system by a single-dose injection can enable greatly enhanced photoimmunotherapy by means of repeated stimulations.

摘要

光动力疗法 (PDT) 已显示出触发全身性抗肿瘤免疫反应的潜力。然而,虽然缺氧的肿瘤微环境是限制 PDT 疗效的因素,但传统 PDT 后的免疫反应通常不足以消除转移性肿瘤。在此,设计了一种包含光敏剂修饰的过氧化氢酶和聚乙二醇二丙烯酸酯 (PEGDA) 作为聚合物基质的光触发原位凝胶系统。进一步将免疫佐剂纳米颗粒引入该系统,以在 PDT 后引发强烈的抗肿瘤免疫反应。将混合前体溶液局部注射到肿瘤中,然后进行光照,即可引发 PEGDA 的聚合,从而诱导原位凝胶形成。这种混合水凝胶具有各种药物在肿瘤中长时间保留的能力,并能够实现持续的肿瘤缺氧缓解,从而能够进行多轮 PDT,通过多轮刺激可显著增强免疫反应。将这种基于凝胶的多轮 PDT 与抗细胞毒性 T 淋巴细胞抗原-4 检查点阻断相结合,不仅可以产生抑制远处肿瘤生长的远隔效应,还可以提供有效的长期免疫记忆保护,防止再次挑战的肿瘤。因此,通过单次注射的光触发原位凝胶系统可以通过重复刺激实现大大增强的光免疫治疗。

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