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局部 VEGF-A 阻断可调节角膜移植物床的微环境。

Local VEGF-A blockade modulates the microenvironment of the corneal graft bed.

机构信息

Department of Ophthalmology, University Hospital of Cologne, Cologne, Germany.

Center for Molecular Medicine Cologne (CMMC), University of Cologne, Cologne, Germany.

出版信息

Am J Transplant. 2019 Sep;19(9):2446-2456. doi: 10.1111/ajt.15331. Epub 2019 Apr 3.

DOI:10.1111/ajt.15331
PMID:30821887
Abstract

The microenvironment plays an important role in several immunological processes. Vascular endothelial growth factor-A (VEGF-A) not only regulates angiogenesis, but is known as a modulator of the immune microenvironment. Modulating the site of transplantation might be beneficial for subsequent transplant survival. In this study, we therefore analyzed the effect that a local blockade of VEGF-A in the inflamed cornea as the graft receiving tissue has on the immune system. We used the murine model of suture-induced neovascularization and subsequent high-risk corneal transplantation, which is an optimal model for local drug application. Mice were treated with VEGFR1/R2 trap prior to transplantation. We analyzed corneal gene expression, as well as protein levels in the cornea and serum on the day of transplantation, 2 and 8 weeks later. Local VEGF depletion prior to transplantation increases the expression of pro-inflammatory as well as immune regulatory cytokines only in the corneal microenvironment, but not in the serum. Furthermore, local VEGFR1/R2 trap treatment significantly inhibits the infiltration of CD11c+ dendritic cells into the cornea. Subsequent increased corneal transplantation success was accompanied by a local upregulation of Foxp3 gene expression. This study demonstrates that locally restricted VEGF depletion increases transplantation success by modulating the receiving corneal microenvironment and inducing tolerogenic mechanisms.

摘要

微环境在几个免疫学过程中起着重要作用。血管内皮生长因子-A(VEGF-A)不仅调节血管生成,而且被认为是免疫微环境的调节剂。调节移植部位可能有利于随后的移植物存活。因此,在这项研究中,我们分析了局部阻断炎症角膜(作为移植物接受组织)中的 VEGF-A 对免疫系统的影响。我们使用了缝线诱导的新生血管形成和随后的高风险角膜移植的小鼠模型,这是局部药物应用的最佳模型。在移植前,用 VEGFR1/R2 陷阱处理小鼠。我们分析了移植当天、2 周和 8 周后角膜的基因表达以及角膜和血清中的蛋白水平。移植前局部 VEGF 耗竭仅增加了角膜微环境中促炎和免疫调节细胞因子的表达,而不是在血清中。此外,局部 VEGFR1/R2 陷阱处理显著抑制了 CD11c+树突状细胞浸润到角膜。随后角膜移植成功率的增加伴随着 Foxp3 基因表达的局部上调。这项研究表明,局部限制的 VEGF 耗竭通过调节接受的角膜微环境和诱导耐受机制来增加移植成功率。

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