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C型凝集素受体CD302在小鼠和人类中的表达及功能特征揭示了其在树突状细胞迁移中的作用。

Characterization of the Expression and Function of the C-Type Lectin Receptor CD302 in Mice and Humans Reveals a Role in Dendritic Cell Migration.

作者信息

Lo Tsun-Ho, Silveira Pablo A, Fromm Phillip D, Verma Nirupama D, Vu Phi A, Kupresanin Fiona, Adam Rhonda, Kato Masato, Cogger Victoria C, Clark Georgina J, Hart Derek N J

机构信息

Dendritic Cell Research, ANZAC Research Institute, Sydney, New South Wales 2139, Australia; Sydney Medical School, University of Sydney, Sydney, New South Wales 2006, Australia;

Dendritic Cell Research, ANZAC Research Institute, Sydney, New South Wales 2139, Australia;

出版信息

J Immunol. 2016 Aug 1;197(3):885-98. doi: 10.4049/jimmunol.1600259. Epub 2016 Jun 17.

Abstract

C-type lectin receptors play important roles in immune cell interactions with the environment. We described CD302 as the simplest, single domain, type I C-type lectin receptor and showed it was expressed mainly on the myeloid phagocytes in human blood. CD302 colocalized with podosomes and lamellopodia structures, so we hypothesized that it played a role in cell adhesion or migration. In this study, we used mouse models to obtain further insights into CD302 expression and its potential immunological function. Mouse CD302 transcripts were, as in humans, highest in the liver, followed by lungs, lymph nodes (LN), spleen, and bone marrow. In liver, CD302 was expressed by hepatocytes, liver sinusoidal endothelial cells, and Kupffer cells. A detailed analysis of CD302 transcription in mouse immune cells revealed highest expression by myeloid cells, particularly macrophages, granulocytes, and myeloid dendritic cells (mDC). Interestingly, 2.5-fold more CD302 was found in migratory compared with resident mDC populations and higher CD302 expression in mouse M1 versus M2 macrophages was also noteworthy. CD302 knockout (CD302KO) mice were generated. Studies on the relevant immune cell populations revealed a decrease in the frequency and numbers of migratory mDC within CD302KO LN compared with wild-type LN. In vitro studies showed CD302KO and wild-type DC had an equivalent capacity to undergo maturation, prime T cells, uptake Ags, and migrate toward the CCL19/CCL21 chemokines. Nevertheless, CD302KO migratory DC exhibited reduced in vivo migration into LN, confirming a functional role for CD302 in mDC migration.

摘要

C型凝集素受体在免疫细胞与环境的相互作用中发挥着重要作用。我们将CD302描述为最简单的单结构域I型C型凝集素受体,并表明它主要在人血液中的髓系吞噬细胞上表达。CD302与足体和片状伪足结构共定位,因此我们推测它在细胞黏附或迁移中起作用。在本研究中,我们使用小鼠模型来进一步深入了解CD302的表达及其潜在的免疫功能。与人类一样,小鼠CD302转录本在肝脏中最高,其次是肺、淋巴结(LN)、脾脏和骨髓。在肝脏中,CD302由肝细胞、肝窦内皮细胞和库普弗细胞表达。对小鼠免疫细胞中CD302转录的详细分析显示,髓系细胞,特别是巨噬细胞、粒细胞和髓系树突状细胞(mDC)的表达最高。有趣的是,与驻留mDC群体相比,迁移性mDC中的CD302含量多2.5倍,并且小鼠M1与M2巨噬细胞中较高的CD302表达也值得注意。我们生成了CD302基因敲除(CD302KO)小鼠。对相关免疫细胞群体的研究表明,与野生型LN相比,CD302KO LN中迁移性mDC的频率和数量有所减少。体外研究表明,CD302KO和野生型DC在成熟、激活T细胞、摄取抗原以及向CCL19/CCL21趋化因子迁移方面具有同等能力。然而,CDKO迁移性DC在体内向LN的迁移减少,证实了CD302在mDC迁移中的功能作用。

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