EphB4单体在主动脉移植模型中抑制慢性移植物血管病变

Q3 Medicine
John T. Langford MD , Luis Gonzalez PhD , Ryosuke Taniguchi MD, PhD , Anand Brahmandam MD , Weichang Zhang MD, PhD , Alan Dardik MD, PhD
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引用次数: 0

摘要

T细胞和巨噬细胞在同种异体移植物血管病变的形成中起重要作用,这是心脏移植慢性排斥反应的主要形式。动脉表达Ephrin-B2作为动脉身份的标志,而循环单核细胞表达同源受体EphB4,促进单核细胞粘附到内皮表面。附着的单核细胞转移并分化为巨噬细胞,巨噬细胞激活T细胞,是排斥反应中组织损伤的主要来源。我们假设抑制Ephrin-B2-EphB4结合可以减少移植移植物内免疫细胞的积累,防止同种异体移植物血管病变。我们利用EphB4单体抑制Ephrin-B2-EphB4在大鼠肾下主动脉移植模型中的结合。经EphB4单体处理的大鼠在移植主动脉28天后巨噬细胞和T细胞减少,新生内膜形成明显减少。这些数据表明Ephin-B2-EphB4轴可能是预防或治疗同种异体移植物血管病变的重要靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

EphB4 monomer inhibits chronic graft vasculopathy in an aortic transplant model

EphB4 monomer inhibits chronic graft vasculopathy in an aortic transplant model

EphB4 monomer inhibits chronic graft vasculopathy in an aortic transplant model

EphB4 monomer inhibits chronic graft vasculopathy in an aortic transplant model

T cells and macrophages play an important role in the formation of allograft vasculopathy, which is the predominant form of chronic rejection in cardiac transplants. Arteries express Ephrin-B2 as a marker of arterial identity, whereas circulating monocytes express the cognate receptor EphB4, which facilitates monocyte adhesion to the endothelial surface. Adherent monocytes transmigrate and differentiate into macrophages that activate T cells and are a main source of tissue damage during rejection. We hypothesized that inhibition of Ephrin-B2-EphB4 binding would decrease immune cell accumulation within a transplanted graft and prevent allograft vasculopathy. We used EphB4 monomer to inhibit Ephrin-B2-EphB4 binding in a rat infrarenal aortic transplant model. Rats treated with EphB4 monomer had fewer macrophages and T cells in the aortic allografts at 28 days, as well as significantly less neointima formation. These data show that the Ephin-B2-EphB4 axis may be an important target for prevention or treatment of allograft vasculopathy.

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来源期刊
CiteScore
4.20
自引率
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审稿时长
28 weeks
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