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孤儿受体RDC1及其假定配体在人树突状细胞和B细胞中的表达与调控。

Expression and regulation of the orphan receptor RDC1 and its putative ligand in human dendritic and B cells.

作者信息

Infantino Simona, Moepps Barbara, Thelen Marcus

机构信息

Institute for Research in Biomedicine, Bellinzona, Switzerland.

出版信息

J Immunol. 2006 Feb 15;176(4):2197-207. doi: 10.4049/jimmunol.176.4.2197.

Abstract

Based on phylogenetic analysis and chromosomal mapping, the orphan receptor RDC1 was proposed to be a chemokine receptor. In this study we examined the expression of RDC1 on leukocytes by measuring mRNA levels and receptor expression using a new specific mAb. Both mRNA and protein levels were high in monocytes and B cells, relatively low on immature dendritic cells (DC), and up-regulated during final stages of maturation. Strikingly, in mature plasmacytoid DC the mRNA was up-regulated, but did not correlate with protein surface expression. We indeed report that CpG-activated plasmacytoid DC produce a putative ligand for RDC1, which selectively down-regulates RDC1, but not CXCR4 on primary human B cells. RDC1 expression was found to be tightly regulated during B cell development and differentiation. In blood-derived switch memory B cells, the expression of RDC1 appeared to correlate with the ability to differentiate into plasma cells upon activation, suggesting that RDC1 is a marker for memory B cells, which are competent to become Ab-secreting cells.

摘要

基于系统发育分析和染色体定位,孤儿受体RDC1被认为是一种趋化因子受体。在本研究中,我们通过使用一种新的特异性单克隆抗体测量mRNA水平和受体表达,来检测RDC1在白细胞上的表达。单核细胞和B细胞中的mRNA和蛋白质水平均较高,在未成熟树突状细胞(DC)上相对较低,并在成熟的最后阶段上调。引人注目的是,在成熟的浆细胞样DC中,mRNA上调,但与蛋白质表面表达无关。我们确实报告了CpG激活的浆细胞样DC产生一种RDC1的假定配体,该配体选择性地下调RDC1,但不影响原代人B细胞上的CXCR4。发现RDC1的表达在B细胞发育和分化过程中受到严格调控。在血液来源的转换记忆B细胞中,RDC1的表达似乎与激活后分化为浆细胞的能力相关,这表明RDC1是有能力成为抗体分泌细胞的记忆B细胞的标志物。

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