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CD22(一种B淋巴细胞限制性黏附分子)小鼠同源物的鉴定与特性分析。

Identification and characterization of the murine homologue of CD22, a B lymphocyte-restricted adhesion molecule.

作者信息

Torres R M, Law C L, Santos-Argumedo L, Kirkham P A, Grabstein K, Parkhouse R M, Clark E A

机构信息

Department of Microbiology, University of Washington, Seattle 98195.

出版信息

J Immunol. 1992 Oct 15;149(8):2641-9.

PMID:1401903
Abstract

The human B lymphocyte-specific Ag, CD22, is a cell adhesion molecule expressed on the surface during a narrow window of B cell development, coincident with surface IgD. A ligand for CD22 has recently been identified on human T cells as the low molecular mass isoform of the leukocyte common Ag, CD45RO. CD22 has been reported to function in the regulation of both T and B cell activation in vitro. In this study, we report the isolation and expression of a molecular cDNA clone encoding the murine homologue of CD22, mCD22. Within their predicted protein sequences, murine and human sequences overall have 62% identity, which includes 18 of 20 extracellular cysteines and six of six cytoplasmic tyrosines. BHK cells transfected with mCD22 cDNA specifically adhere to resting and activated T lymphocytes and in addition bound activated, but not resting, B cells. Five Th clones were analyzed for their ability to adhere to mCD22; two Th0 clones and one Th1 clone bound CD22+ BHK transfectants, but not all T cell clones bound CD22+ cells: another Th1 clone and a Th2 clone did not. mCD22+ BHK transfectants were also specifically bound by the B cell-specific mAb, NIM-R6, demonstrating that this mAb is specific for murine CD22. Human cell lines expressing the counter-receptors for human CD22 were also examined for adhesion to the murine CD22 homologue; the epitope responsible for B cell adhesion to CD22 is conserved, whereas the T cell epitope binding to CD22 is not. The cDNA and mAb to murine CD22 will be useful for defining the in vivo function of CD22.

摘要

人类B淋巴细胞特异性抗原CD22是一种细胞黏附分子,在B细胞发育的狭窄窗口期表达于细胞表面,与表面IgD同时出现。最近在人类T细胞上鉴定出CD22的一种配体,即白细胞共同抗原CD45RO的低分子量异构体。据报道,CD22在体外对T细胞和B细胞的激活均有调节作用。在本研究中,我们报告了编码小鼠CD22同源物mCD22的分子cDNA克隆的分离和表达。在其预测的蛋白质序列中,小鼠和人类序列总体上有62%的同一性,其中包括20个细胞外半胱氨酸中的18个和6个细胞质酪氨酸中的6个。用mCD22 cDNA转染的BHK细胞特异性黏附于静止和活化的T淋巴细胞,此外还结合活化的B细胞,但不结合静止的B细胞。分析了五个Th克隆黏附mCD22的能力;两个Th0克隆和一个Th1克隆结合CD22+BHK转染细胞,但并非所有T细胞克隆都结合CD22+细胞:另一个Th1克隆和一个Th2克隆不结合。mCD22+BHK转染细胞也被B细胞特异性单克隆抗体NIM-R6特异性结合,表明该单克隆抗体对小鼠CD22具有特异性。还检测了表达人类CD22反受体的人类细胞系对小鼠CD22同源物的黏附情况;负责B细胞黏附到CD22的表位是保守的,而与CD22结合的T细胞表位则不是。针对小鼠CD22的cDNA和单克隆抗体将有助于确定CD22在体内的功能。

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