The Induction of Circulating, ACAID-Inducing Monocytes Requires CCR2/CCL2-Dependent Migration of Circulating F4/80(+) Cells into the Anterior Chamber.

Ophthalmology and eye diseases Pub Date : 2010-11-11 Print Date: 2010-01-01 DOI:10.4137/OED.S6113
Robert E Cone, Subhasis Chattopadhyay, Roshan Pais, Sourojit Bhowmick, Roshanak Sharafieh, Yen Lemire, James O'Rourke
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引用次数: 3

Abstract

To determine the origin of peripheral blood mononulclear cells (PBMC) that activate regulatory T cells in anterior chamber-associated immune deviation (ACAID), fluorescein-labeled PBMC were intravenously injected into mice before the mice received an intracameral injection of antigen. Six-24 hr after intracameral injection, fluorescein-labeled PBMC increased in the iris. Twenty-four-48 hr labeled cells decreased in the iris and increased in the thymus and spleen. The entry of the labeled PBMC into the anterior chamber and subsequent production of PBMC that transfer ACAID required the expression of CCR2 by the PBMC and the production of the chemokine CCL2 by the recipient of the PBMC. The results suggest that the intracameral injection of antigen induces i) the infiltration of F4/80(+) PBMC into the AC, ii) where these PBMC are converted to a regulatory phenotype, and iii) recirculate to activate T cells that suppress cell-mediated immunity.

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诱导循环、诱导acid的单核细胞需要循环F4/80(+)细胞迁移到前房的CCR2/ ccl2依赖性。
为了确定激活前房相关免疫偏差(ACAID)中调节性T细胞的外周血单核细胞(PBMC)的来源,在小鼠接受肠腔内注射抗原之前,将荧光素标记的PBMC静脉注射到小鼠体内。眼内注射6 -24小时后,虹膜中荧光素标记的PBMC增加。24 -48小时标记细胞在虹膜中减少,胸腺和脾脏中增加。标记的PBMC进入前房并随后产生转移ACAID的PBMC需要PBMC表达CCR2和PBMC受体产生趋化因子CCL2。结果表明,ameral内注射抗原诱导i) F4/80(+) PBMC浸润到AC中,ii)这些PBMC转化为调节表型,iii)再循环激活T细胞,抑制细胞介导的免疫。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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