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外源性非编码 dsDNA 依赖性吞噬细胞转激活增强抗肿瘤免疫。

Exogenous non-coding dsDNA-dependent trans-activation of phagocytes augments anti-tumor immunity.

机构信息

Department of Cell Biology, Sylvester Cancer Center, University of Miami Miller School of Medicine, Miami, FL, USA.

Georgia Cancer Center, Augusta University Medical Center, Augusta, GA, USA.

出版信息

Cell Rep Med. 2024 May 21;5(5):101528. doi: 10.1016/j.xcrm.2024.101528. Epub 2024 Apr 26.

Abstract

Stimulator of interferon genes (STING)-dependent signaling is requisite for effective anti-microbial and anti-tumor activity. STING signaling is commonly defective in cancer cells, which enables tumor cells to evade the immunosurveillance system. We evaluate here whether intrinsic STING signaling in such tumor cells could be reconstituted by creating recombinant herpes simplex viruses (rHSVs) that express components of the STING signaling pathway. We observe that rHSVs expressing STING and/or cGAS replicate inefficiently yet retain in vivo anti-tumor activity, independent of oncolytic activity requisite on the trans-activation of extrinsic STING signaling in phagocytes by engulfed microbial dsDNA species. Accordingly, the in vivo effects of virotherapy could be simulated by nanoparticles incorporating non-coding dsDNA species, which comparably elicit the trans-activation of phagocytes and augment the efficacy of established cancer treatments including checkpoint inhibition and radiation therapy. Our results help elucidate mechanisms of virotherapeutic anti-tumor activity as well as provide alternate strategies to treat cancer.

摘要

干扰素基因刺激物 (STING) 依赖性信号转导对于有效的抗微生物和抗肿瘤活性是必需的。STING 信号转导在癌细胞中通常存在缺陷,这使肿瘤细胞能够逃避免疫监视系统。我们在这里评估是否可以通过创建表达 STING 信号通路成分的重组单纯疱疹病毒 (rHSV) 来重建此类肿瘤细胞中的固有 STING 信号。我们观察到表达 STING 和/或 cGAS 的 rHSV 复制效率低下,但保留体内抗肿瘤活性,而无需吞噬细胞吞噬微生物 dsDNA 后通过外在 STING 信号转导所必需的溶瘤活性。因此,通过包含非编码 dsDNA 物质的纳米颗粒可以模拟病毒治疗的体内作用,该物质可比照激活吞噬细胞并增强包括检查点抑制和放射治疗在内的既定癌症治疗方法的疗效。我们的结果有助于阐明病毒治疗抗肿瘤活性的机制,并提供了治疗癌症的替代策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1cf4/11148645/89e6aac7a55e/fx1.jpg

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