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IL-33 的修复作用。

The Reparative Roles of IL-33.

机构信息

Thomas E. Starzl Transplantation Institute, University of Pittsburgh School of Medicine, Pittsburgh, PA.

Department of Surgery, University of Pittsburgh School of Medicine, Pittsburgh, PA.

出版信息

Transplantation. 2023 May 1;107(5):1069-1078. doi: 10.1097/TP.0000000000004447. Epub 2023 Apr 22.

Abstract

When discovered in the early 2000s, interleukin-33 (IL-33) was characterized as a potent driver of type 2 immunity and implicated in parasite clearance, as well as asthma, allergy, and lung fibrosis. Yet research in other models has since revealed that IL-33 is a highly pleiotropic molecule with diverse functions. These activities are supported by elusive release mechanisms and diverse expression of the IL-33 receptor, STimulation 2 (ST2), on both immune and stromal cells. Interestingly, IL-33 also supports type 1 immune responses during viral and tumor immunity and after allogeneic hematopoietic stem cell transplantation. Yet the IL-33-ST2 axis is also critical to the establishment of systemic homeostasis and tissue repair and regeneration. Despite these recent findings, the mechanisms by which IL-33 governs the balance between immunity and homeostasis or can support both effective repair and pathogenic fibrosis are poorly understood. As such, ongoing research is trying to understand the potential reparative and regulatory versus pro-inflammatory and pro-fibrotic roles for IL-33 in transplantation. This review provides an overview of the emerging regenerative role of IL-33 in organ homeostasis and tissue repair as it relates to transplantation immunology. It also outlines the known impacts of IL-33 in commonly transplanted solid organs and covers the envisioned roles for IL-33 in ischemia-reperfusion injury, rejection, and tolerance. Finally, we give a comprehensive summary of its effects on different cell populations involved in these processes, including ST2 + regulatory T cells, innate lymphoid cell type 2, as well as significant myeloid cell populations.

摘要

当白细胞介素-33 (IL-33) 在 21 世纪初被发现时,它被描述为 2 型免疫的有力驱动因子,并与寄生虫清除以及哮喘、过敏和肺纤维化有关。然而,此后其他模型的研究表明,IL-33 是一种具有多种功能的高度多功能分子。这些活性得到了难以捉摸的释放机制和 IL-33 受体 STimulation 2 (ST2) 在免疫细胞和基质细胞上的多样化表达的支持。有趣的是,IL-33 在病毒和肿瘤免疫以及异基因造血干细胞移植后也支持 1 型免疫反应。然而,IL-33-ST2 轴对于建立全身稳态和组织修复和再生也至关重要。尽管有这些最近的发现,但 IL-33 调节免疫和稳态之间平衡或支持有效修复和病理性纤维化的机制仍知之甚少。因此,正在进行的研究试图了解 IL-33 在移植中作为潜在的修复和调节因子与促炎和促纤维化因子的作用。这篇综述概述了 IL-33 在器官稳态和组织修复中的新兴再生作用,以及它与移植免疫学的关系。它还概述了 IL-33 在常见移植实体器官中的已知影响,并涵盖了 IL-33 在缺血再灌注损伤、排斥和耐受中的预期作用。最后,我们全面总结了它对涉及这些过程的不同细胞群体的影响,包括 ST2+调节性 T 细胞、先天淋巴细胞 2 以及重要的髓样细胞群体。

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