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超越负调控:IL-1R8和IL-1R2作为新型免疫检查点

Beyond Negative Regulation: IL-1R8 and IL-1R2 as Novel Immune Checkpoints.

作者信息

Supino Domenico, Garuti Roberto, Garlanda Cecilia

机构信息

IRCCS Humanitas Research Hospital, Milan, Italy.

Department of Biomedical Sciences, Humanitas University, Milan, Italy.

出版信息

Eur J Immunol. 2025 Sep;55(9):e70050. doi: 10.1002/eji.70050.

Abstract

IL-1 family members and their signaling receptors are key drivers of inflammation in sterile or infectious conditions, as well as polarization of the innate and adaptive immunity. Deregulated or excessive activation of the IL-1 system is associated with detrimental inflammatory reactions. Beside signaling receptors, IL-1-family receptors comprise decoy or negative regulatory receptors, which regulate cell activation mediated by IL-1 family ligands. IL-1-family negative regulatory receptors, which include IL-1R8 and IL-1R2, have peculiar structural features and functions essential to the self-regulation of the IL-1 system. IL-1R8 and IL-1R2 emerge as regulatory molecules whose function is context-dependent, spanning from negative regulation of inflammation in infections or conditions of sterile inflammation and cell damage, including cancer-related inflammation, to skewing of myeloid and lymphoid cells, modulation of anti-tumor immunity, and immune checkpoint activity. This review reports new insights into the physio-pathological roles of these two negative regulatory IL-1 family members, emphasizing their mechanisms of action and potential for innovative therapeutic interventions.

摘要

白细胞介素-1(IL-1)家族成员及其信号受体是无菌或感染性炎症以及先天性和适应性免疫极化的关键驱动因素。IL-1系统的失调或过度激活与有害的炎症反应相关。除了信号受体外,IL-1家族受体还包括诱饵受体或负调节受体,它们调节由IL-1家族配体介导的细胞激活。IL-1家族负调节受体,包括IL-1R8和IL-1R2,具有独特的结构特征和功能,对IL-1系统的自我调节至关重要。IL-1R8和IL-1R2作为调节分子出现,其功能取决于具体情况,范围从感染或无菌性炎症及细胞损伤(包括癌症相关炎症)中的炎症负调节,到骨髓和淋巴细胞的偏向、抗肿瘤免疫调节以及免疫检查点活性。本综述报告了对这两个负调节IL-1家族成员生理病理作用的新见解,强调了它们的作用机制以及创新治疗干预的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0126/12412433/fb6a53781314/EJI-55-e70050-g002.jpg

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