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存在一系列新的B细胞抗原分离株的证据,这些抗原由HLA - D区域编码,并刺激二次同种异体增殖和细胞毒性反应。

Evidence for a new segregant series of B cell antigens that are encoded in the HLA-D region and that stimulate secondary allogenic proliferative and cytotoxic responses.

作者信息

Shaw S, Johnson A H, Shearer G M

出版信息

J Exp Med. 1980 Sep 1;152(3):565-80. doi: 10.1084/jem.152.3.565.

Abstract

Five new histocompatibility antigens, designated secondary B cell or (SB) antigens, have been identified by secondary allogeneic proliferative and cytotoxic responses. The reagents used to define the SB antigents are lymphocytes primed between donors matched for all known HLA antigens. The SB antigens stimulate weak primary allogeneic proliferative responses (a mean relative response of 8%) but strong secondary proliferative responses. Strong secondary cell-mediated cytotoxicity is generated against target antigens that are distinguishable from the SB antigens defined by proliferation. Studies by direct lysis and by cold-target inhibition indicate that these target antigens are preferentially expressed on B cells relative to T cells. The SB antigens segregate with HLA, and the gene(s) encoding the SB1, 3, and 4 antigens maps centromeric to HLA-B. The SB antigens are major histocompatibility antigens not only because they are encoded by major histocompatibility complex (MHC) genes, but also by the functional criteria that the proliferative and cytotoxic responses to SB antigens are not restricted by HLA-DR or HLA-A,-B. Parallel studies of the SB antigens and the DR antigens with respect to: (a) their preferential expression on B cells, (b) their function in secondary allogeneic proliferative and cytotoxic respones, and (c) the location of their structural gene within the MHC. However, the SB antigens and the DR antigens are clearly distinct antigens, because population studies indicate that they can occur independently, and family studies indicate that specific SB antigens segregate with HLA haplotypes having different D and DR specificities. Our data are consistent with the hypotheses that the SB antigens are a new segregant series of B cell alloantigens, and that the SB gene and the DR gene derive from a duplicated ancestral gene.

摘要

通过二次同种异体增殖和细胞毒性反应,已鉴定出五种新的组织相容性抗原,称为二级B细胞或(SB)抗原。用于定义SB抗原的试剂是在所有已知HLA抗原相匹配的供体之间引发的淋巴细胞。SB抗原刺激较弱的初次同种异体增殖反应(平均相对反应率为8%),但刺激较强的二次增殖反应。针对与通过增殖定义的SB抗原不同的靶抗原,可产生强烈的二次细胞介导的细胞毒性。直接裂解和冷靶抑制研究表明,相对于T细胞,这些靶抗原在B细胞上优先表达。SB抗原与HLA连锁,编码SB1、3和4抗原的基因定位于HLA - B的着丝粒侧。SB抗原是主要组织相容性抗原,这不仅是因为它们由主要组织相容性复合体(MHC)基因编码,还因为对SB抗原的增殖和细胞毒性反应不受HLA - DR或HLA - A、- B的限制。对SB抗原和DR抗原进行了平行研究,涉及:(a)它们在B细胞上的优先表达,(b)它们在二次同种异体增殖和细胞毒性反应中的功能,以及(c)它们的结构基因在MHC中的位置。然而,SB抗原和DR抗原显然是不同的抗原,因为群体研究表明它们可以独立出现,而家系研究表明特定的SB抗原与具有不同D和DR特异性的HLA单倍型连锁。我们的数据与以下假设一致:SB抗原是B细胞同种异体抗原的一个新的分离系列,并且SB基因和DR基因源自一个重复的祖先基因。

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