microRNA-155 对心脏异体移植免疫反应的调控。

IF 1.6 4区 医学 Q4 IMMUNOLOGY Transplant immunology Pub Date : 2024-08-31 DOI:10.1016/j.trim.2024.102113
Sandhya Bansal, Yoshihiro Itabashi, Alexa Guerrero-Alba, Timothy Fleming, Michael A. Smith, Ross M. Bremner, T. Mohanakumar
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引用次数: 0

摘要

导言:为了改善患者的预后,迫切需要更好地了解移植后异体移植物排斥反应所涉及的免疫机制。由于microRNA-155(miR155)在炎症中起着至关重要的作用,我们推测miR155的缺乏将提高心脏移植后心脏异体移植的存活率并增强耐受性诱导:我们通过将异位 BALB/c 心脏移植给 C57BL/6(野生型)和 C57BL/6 miR155 基因敲除(miR155KO)小鼠,建立了急性排斥小鼠模型。此外,我们还使用CTLA4-Ig(200 μg;移植后第2天)和MRI抗体(250 μg;移植后第0天)分别针对CD28/B7和CD40/CD154信号进行成本刺激阻断,从而诱导两组小鼠产生耐受。最后,我们研究了向耐受miR155KO小鼠注射100微克从发生排斥反应的野生型小鼠体内分离出的细胞外小泡(sEVs)的效果:结果:野生型小鼠和 miR155KO 小鼠心脏同种异体移植物的平均存活时间(MST)分别为 7 天和 15 天(野生型和 miR155KO 受体分别为 100 天(p 100 天;p 结论:miR155KO 小鼠可提高心脏同种异体移植物的存活率,并增强异位心脏移植后的耐受性诱导。向 miR155KO 小鼠注射发生排斥反应的野生型小鼠的 sEV 可逆转这些益处。
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Regulation of cardiac allograft immune responses by microRNA-155

Introduction

A better understanding of the immune mechanisms involved in allograft rejection after transplantation is urgently needed to improve patient outcomes. As microRNA-155 (miR155) plays a critical role in inflammation, we postulated that a deficiency of miR155 will improve cardiac allograft survival and enhance tolerance induction after heart transplantation.

Methods

We developed an acute rejection mouse model through heterotopic BALB/c cardiac transplantation to C57BL/6 (wild-type) and C57BL/6 miR155 knock-out (miR155KO) mice. Further, we induced tolerance in both groups through a costimulatory blockade with CTLA4-Ig (200 μg; post-transplant day 2) and MRI antibodies (250 μg; post-transplant day 0), targeting CD28/B7 and CD40/CD154 signals, respectively. Finally, we examined the effects of injecting 100 μg of small extracellular vesicles (sEVs) isolated from wild-type mice undergoing rejection into tolerant miR155KO mice.

Results

Mean survival time (MST) of the cardiac allografts in wild-type and miR155KO mice was 7 and 15 days, respectively (p < 0.0001). Costimulatory blockade increased MST to 65 days and > 100 days in the wild-type and miR155KO recipients, respectively (p < 0.001). Injection of sEVs isolated from wild-type mice undergoing rejection into tolerant miR155KO mice decreased the allograft survival to 9 days, significantly lower than the tolerant miR155KO mice without injection of sEVs (>100 days; p < 0.0001).

Conclusion

miR155KO mice have improved cardiac allograft survival and enhanced induction of tolerance after heterotopic cardiac transplantation. Injection of sEVs from wild-type mice undergoing rejection into the miR155KO mice reversed these benefits.

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来源期刊
Transplant immunology
Transplant immunology 医学-免疫学
CiteScore
2.10
自引率
13.30%
发文量
198
审稿时长
48 days
期刊介绍: Transplant Immunology will publish up-to-date information on all aspects of the broad field it encompasses. The journal will be directed at (basic) scientists, tissue typers, transplant physicians and surgeons, and research and data on all immunological aspects of organ-, tissue- and (haematopoietic) stem cell transplantation are of potential interest to the readers of Transplant Immunology. Original papers, Review articles and Hypotheses will be considered for publication and submitted manuscripts will be rapidly peer-reviewed and published. They will be judged on the basis of scientific merit, originality, timeliness and quality.
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