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针对HLA-DP、DQ和DR决定簇的单克隆抗体:对正常和EB病毒转化的B细胞激活和增殖的功能影响

Monoclonal antibodies to HLA-DP, DQ, and DR determinants: functional effects on the activation and proliferation of normal and EBV-transformed B cells.

作者信息

Howard D R, Eaves A C, Takei F

出版信息

Exp Hematol. 1986 Oct;14(9):887-95.

PMID:2428652
Abstract

To investigate the function of HLA class II molecules in B-cell activation, we generated three new anti-HLA class II monoclonal antibodies with differing specificities for DP, DQ, and DR determinants. These were tested for their ability to inhibit various B- and T-lymphocyte responses. Each of these antibodies (NB-29, DH-84, and DH-224) immunoprecipitates a heterodimer of approximately 35,000 and 28,000 mol wt from 125I-surface-labeled B-lymphoma cells, as shown by SDS-PAGE. NB-29 (IgG1) detects a polymorphic DQ determinant, while DH-224 (IgG1) is reactive with monomorphic DR determinants, and DH-84 (IgG2a) has specificity for DP, DQ, and DR. Both DH-224 and DH-84, but not NB-29, were found to inhibit significantly the stimulation of peripheral blood mononuclear cells (PBMC) by anti-mu (70%-90% inhibition) and by lipopolysaccharide (80%-90% inhibition), as measured by incorporation of tritiated thymidine. When added to highly purified populations of peripheral blood B cells, none of these anti-class II monoclonal antibodies inhibited anti-mu-induced stimulation. This suggests that the inhibitory effect that DH-224 and DH-84 have on the stimulation of unfractionated PBMC may be due to their ability to interfere with the action of accessory cells. Epstein-Barr-virus (EBV)-transformed B-cell lines, in contrast, showed substantial inhibition of growth when cultured in the presence of any of the three antibodies. With respect to T cells, DH-84 and DH-224 strongly inhibited the mixed lymphocyte response; NB-29 did not. None of these antibodies inhibited stimulation of PBMC by phytohemagglutinin (PHA). These findings suggest that DQ and DR HLA class II molecules have differing roles in B-cell activation and document a direct antiproliferative effect of anti-HLA class II monoclonal antibodies on the growth of EBV-transformed cell lines.

摘要

为了研究人类白细胞抗原(HLA)Ⅱ类分子在B细胞活化中的作用,我们制备了三种新的抗HLAⅡ类单克隆抗体,它们对DP、DQ和DR决定簇具有不同的特异性。检测了它们抑制各种B淋巴细胞和T淋巴细胞反应的能力。如十二烷基硫酸钠-聚丙烯酰胺凝胶电泳(SDS-PAGE)所示,这些抗体(NB-29、DH-84和DH-224)中的每一种都能从125I表面标记的B淋巴瘤细胞中免疫沉淀出一个分子量约为35000和28000道尔顿的异二聚体。NB-29(IgG1)检测到一个多态性的DQ决定簇,而DH-224(IgG1)与单态性的DR决定簇反应,DH-84(IgG2a)对DP、DQ和DR具有特异性。通过掺入氚化胸腺嘧啶核苷来测量,发现DH-224和DH-84,但不是NB-29,能显著抑制抗μ(70%-90%抑制)和脂多糖(80%-90%抑制)对外周血单个核细胞(PBMC)的刺激。当添加到高度纯化的外周血B细胞群体中时,这些抗Ⅱ类单克隆抗体均未抑制抗μ诱导的刺激。这表明DH-224和DH-84对未分级PBMC刺激的抑制作用可能是由于它们干扰辅助细胞作用的能力。相比之下,当在三种抗体中的任何一种存在的情况下培养时,爱泼斯坦-巴尔病毒(EBV)转化的B细胞系显示出显著的生长抑制。关于T细胞,DH-84和DH-224强烈抑制混合淋巴细胞反应;NB-29则没有。这些抗体均未抑制植物血凝素(PHA)对PBMC的刺激。这些发现表明,DQ和DR HLAⅡ类分子在B细胞活化中具有不同的作用,并证明了抗HLAⅡ类单克隆抗体对EBV转化细胞系生长的直接抗增殖作用。

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