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凋亡小体介导的细胞内递药策略增强 STING 激活和改善肿瘤免疫原性

Apoptotic Body-Mediated Intracellular Delivery Strategy for Enhanced STING Activation and Improved Tumor Immunogenicity.

机构信息

Key Laboratory of Biomedical Polymers of Ministry of Education & Department of Chemistry, Wuhan University, Wuhan 430072, P. R. China.

出版信息

Nano Lett. 2022 Mar 23;22(6):2217-2227. doi: 10.1021/acs.nanolett.1c03996. Epub 2022 Mar 7.

Abstract

Agonists of stimulators of interferon genes (STING) are a promising class of immunotherapeutics that trigger potent innate immunity. However, the therapeutic efficacy of conventional STING agonists, such as 2',3'-cyclic guanosine monophosphate-adenosine monophosphate (cGAMP), is severely restricted to poor cytosolic delivery and lacks the capacity to promote the recognition of tumor-specific antigens. Here, we tackle these challenges through a nanovaccine platform based on Fenton-reactive and STING-activating nanoparticles, synergistically contributing to the generation of tumor-cell-derived apoptotic bodies (ABs). ABs loaded with exogenous cGAMP are readily phagocytosed by antigen-presenting cells (APCs), as a Trojan horse for rendering tumor cells with high immunogenicity instead of a noninflammatory response. This leads to enhanced STING activation and an improved tumor-specific antigen presentation ability, boosting the adaptive immunity in collaboration with innate immune. The strategy of exploiting a metal-based nanovaccine platform possesses great potential to be clinically translated into a trinitarian system of diagnosis, treatment, and prognosis.

摘要

激动剂的干扰素基因刺激物(STING)是一类很有前途的免疫治疗药物,能引发强烈的先天免疫。然而,传统的 STING 激动剂,如 2',3'-环鸟苷单磷酸-腺苷单磷酸(cGAMP)的治疗效果受到严重限制,主要是由于它们在细胞质内的递送效果不佳,并且缺乏促进肿瘤特异性抗原识别的能力。在这里,我们通过基于芬顿反应和 STING 激活纳米粒子的纳米疫苗平台来解决这些挑战,这些纳米粒子协同作用,有助于生成肿瘤细胞来源的凋亡小体(ABs)。ABs 负载外源性 cGAMP 后,很容易被抗原呈递细胞(APCs)吞噬,作为一种特洛伊木马,使肿瘤细胞具有高免疫原性,而不是产生非炎症反应。这导致 STING 的激活增强,以及肿瘤特异性抗原呈递能力的提高,与先天免疫协同增强适应性免疫。利用基于金属的纳米疫苗平台的策略具有很大的潜力,可以在临床上转化为诊断、治疗和预后三位一体的系统。

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