Rapamycin antagonizes angiogenesis and lymphangiogenesis through myeloid-derived suppressor cells in corneal transplantation

IF 8.9 2区 医学 Q1 SURGERY American Journal of Transplantation Pub Date : 2023-09-01 DOI:10.1016/j.ajt.2023.05.017
Yuerong Ren , Xiaonan Dong , Yingyi Liu , Huanmin Kang , Lingling Guan , Yumin Huang , Xinqi Zhu , Jing Tian , Baihua Chen , Bing Jiang , Yan He
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引用次数: 2

Abstract

Rapamycin is an immunosuppressive drug that is widely used in the postsurgery management of transplantation. To date, the mechanism by which rapamycin reduces posttransplant neovascularization has not been fully understood. Given the original avascularity and immune privilege of the cornea, corneal transplantation is considered as an ideal model to investigate neovascularization and its effects on allograft rejection. Previously, we found that myeloid-derived suppressor cells (MDSC) prolong corneal allograft survival through suppression of angiogenesis and lymphangiogenesis. Here, we show that depletion of MDSC abolished rapamycin-mediated suppression of neovascularization and elongation of corneal allograft survival. RNA-sequencing analysis revealed that rapamycin dramatically enhanced the expression of arginase 1 (Arg1). Furthermore, an Arg1 inhibitor also completely abolished the rapamycin-mediated beneficial effects after corneal transplantation. Taken together, these findings indicate that MDSC and elevated Arg1 activity are essential for the immunosuppressive and antiangiogenic functions of rapamycin.

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在角膜移植中,雷帕霉素通过髓源性抑制细胞拮抗血管生成和淋巴管生成
雷帕霉素是一种免疫抑制药物,广泛用于移植术后管理。到目前为止,雷帕霉素减少移植后新生血管形成的机制尚不完全清楚。鉴于角膜的原始无血管性和免疫特权,角膜移植被认为是研究新生血管及其对同种异体移植物排斥反应影响的理想模型。以前,我们发现骨髓来源的抑制细胞(MDSC)通过抑制血管生成和淋巴管生成来延长角膜移植物的存活时间。在这里,我们发现MDSC的耗竭消除了雷帕霉素介导的对新生血管形成的抑制和角膜移植存活率的延长。RNA测序分析显示雷帕霉素显著增强精氨酸酶1(Arg1)的表达。此外,Arg1抑制剂也完全消除了雷帕霉素介导的角膜移植后的有益作用。总之,这些发现表明MDSC和Arg1活性的升高对雷帕霉素的免疫抑制和抗血管生成功能至关重要。
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来源期刊
CiteScore
18.70
自引率
4.50%
发文量
346
审稿时长
26 days
期刊介绍: The American Journal of Transplantation is a leading journal in the field of transplantation. It serves as a forum for debate and reassessment, an agent of change, and a major platform for promoting understanding, improving results, and advancing science. Published monthly, it provides an essential resource for researchers and clinicians worldwide. The journal publishes original articles, case reports, invited reviews, letters to the editor, critical reviews, news features, consensus documents, and guidelines over 12 issues a year. It covers all major subject areas in transplantation, including thoracic (heart, lung), abdominal (kidney, liver, pancreas, islets), tissue and stem cell transplantation, organ and tissue donation and preservation, tissue injury, repair, inflammation, and aging, histocompatibility, drugs and pharmacology, graft survival, and prevention of graft dysfunction and failure. It also explores ethical and social issues in the field.
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