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小鼠CD22的免疫球蛋白结构域1和2构成配体结合结构域,并与B细胞和T细胞上表达的多种唾液酸化配体结合。

Ig domains 1 and 2 of murine CD22 constitute the ligand-binding domain and bind multiple sialylated ligands expressed on B and T cells.

作者信息

Law C L, Aruffo A, Chandran K A, Doty R T, Clark E A

机构信息

Department of Microbiology, University of Washington, Seattle 98195, USA.

出版信息

J Immunol. 1995 Oct 1;155(7):3368-76.

PMID:7561031
Abstract

Baby hamster kidney cells transfected with murine CD22 (mCD22) mediate adhesion to B- and T-lineage cells. To further characterize mCD22-mediated cell adhesion, we generated a panel of recombinant globulins (Rg) consisting of different extracellular Ig-like (Ig) domains of mCD22. FACS analysis using these mCD22.Rgs revealed that ligands for mCD22 are expressed on both B and T cell lines and also normal B and T cells. In B-lineage cells, the expression of mCD22 ligands began on sIgM- pre-B cells in bone marrow. The ligand-binding site of mCD22 for ligands was mapped to Ig domains 1 and 2: mCD22.Rgs containing Ig domains 1 and 2 bound target cells and immunoprecipitated sets of glycoproteins similar to Rgs containing Ig domains 1 to 3 or all 7 CD22 Ig domains, whereas Rgs containing Ig domains 2 to 3 or 3 to 7 did not bind either B or T cells. Furthermore, B cells apparently expressed higher levels of mCD22 ligands than that of T cells, suggesting a potential competition for CD22 binding between ligands expressed on the same B cell and those expressed on another B cell or T cells. Immunoprecipitation experiments using the mCD22.Rgs identified mCD22 itself and the B cell-specific isoform of mCD45RA (B220) as two of the mCD22 ligands expressed on B cells. Thus, mCD22 may potentially regulate B cell activation through interactions with itself or mCD45RA/B220.

摘要

用鼠源CD22(mCD22)转染的幼仓鼠肾细胞介导与B细胞系和T细胞系细胞的黏附。为了进一步表征mCD22介导的细胞黏附,我们构建了一组由mCD22不同细胞外免疫球蛋白样(Ig)结构域组成的重组球蛋白(Rg)。使用这些mCD22.Rg进行的流式细胞术分析表明,mCD22的配体在B细胞系和T细胞系以及正常B细胞和T细胞上均有表达。在B细胞系细胞中,mCD22配体的表达始于骨髓中sIgM-前B细胞。mCD22与配体的配体结合位点被定位到Ig结构域1和2:包含Ig结构域1和2的mCD22.Rg与靶细胞结合,并免疫沉淀出一组糖蛋白,类似于包含Ig结构域1至3或所有7个CD22 Ig结构域的Rg,而包含Ig结构域2至3或3至7的Rg既不与B细胞也不与T细胞结合。此外,B细胞表面mCD22配体的表达水平明显高于T细胞,这表明同一B细胞上表达的配体与另一B细胞或T细胞上表达的配体之间可能存在对CD22结合的竞争。使用mCD22.Rg进行的免疫沉淀实验确定mCD22自身以及mCD45RA的B细胞特异性异构体(B220)是B细胞上表达的两种mCD22配体。因此,mCD22可能通过与自身或mCD45RA/B220相互作用来潜在地调节B细胞活化。

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