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纳米壳介导的 STING 激动剂胞内递送诱导的合成免疫细胞死亡增强了抗癌化疗免疫治疗。

Synthetic Immunogenic Cell Death Mediated by Intracellular Delivery of STING Agonist Nanoshells Enhances Anticancer Chemo-immunotherapy.

机构信息

Taiwan International Graduate Program in Molecular Medicine, National Yang-Ming University and Academia Sinica, Taipei 11529, Taiwan.

Institute of Biomedical Sciences, Academia Sinica, Taipei 11529, Taiwan.

出版信息

Nano Lett. 2020 Apr 8;20(4):2246-2256. doi: 10.1021/acs.nanolett.9b04094. Epub 2020 Mar 17.

Abstract

Many favorable anticancer treatments owe their success to the induction immunogenic cell death (ICD) in cancer cells, which results in the release of endogenous danger signals along with tumor antigens for effective priming of anticancer immunity. We describe a strategy to artificially induce ICD by delivering the agonist of stimulator of interferon genes (STING) into tumor cells using hollow polymeric nanoshells. Following intracellular delivery of exogenous adjuvant, subsequent cytotoxic treatment creates immunogenic cellular debris that spatiotemporally coordinate tumor antigens and STING agonist in a process herein termed synthetic immunogenic cell death (sICD). sICD is indiscriminate to the type of chemotherapeutics and enables colocalization of exogenously administered immunologic adjuvants and tumor antigens for enhanced antigen presentation and anticancer adaptive response. In three mouse tumor models, sICD enhances therapeutic efficacy and restrains tumor progression. The study highlights the benefit of delivering STING agonists to cancer cells, paving ways to new chemo-immunotherapeutic designs.

摘要

许多有利的抗癌治疗方法归功于诱导癌细胞免疫原性细胞死亡(ICD),这导致内源性危险信号与肿瘤抗原一起释放,从而有效地启动抗癌免疫。我们描述了一种通过使用中空聚合物纳米壳将干扰素基因刺激物(STING)激动剂递送至肿瘤细胞中来人为诱导 ICD 的策略。在细胞内递外源性佐剂后,随后的细胞毒性治疗会产生免疫原性细胞碎片,在本文中称为合成免疫原性细胞死亡(sICD),从而在时空上协调肿瘤抗原和 STING 激动剂。sICD 对化疗药物的类型没有选择性,并能够使外源性给予的免疫佐剂和肿瘤抗原共定位,以增强抗原呈递和抗癌适应性反应。在三种小鼠肿瘤模型中,sICD 增强了治疗效果并抑制了肿瘤进展。该研究强调了向癌细胞递送 STING 激动剂的益处,为新的化疗免疫治疗设计铺平了道路。

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