首页> 外文OA文献 >Involvement of HLA class I alleles in natural killer (NK) cell-specific functions: expression of HLA-Cw3 confers selective protection from lysis by alloreactive NK clones displaying a defined specificity (specificity 2)
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Involvement of HLA class I alleles in natural killer (NK) cell-specific functions: expression of HLA-Cw3 confers selective protection from lysis by alloreactive NK clones displaying a defined specificity (specificity 2)

机译:HLA I类等位基因参与自然杀伤(NK)细胞特异性功能:HLA-Cw3的表达赋予显示出确定的特异性(特异性2)的同种异体反应性NK克隆选择性保护以防止其裂解

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摘要

This study was designed to identify the target molecules of the natural killer (NK) cell-mediated recognition of normal allogeneic target cells. As previously shown, the gene(s) governing the first NK-defined allospecificity (specificity 1) were found to be localized in the major histocompatibility complex region between BF gene and HLA-A. In addition, the analysis of a previously described family revealed that a donor (donor 81) was heterozygous for three distinct NK-defined allospecificities (specificities 1, 2, and 5). HLA variants were derived from the B-Epstein-Barr virus cell line of donor 81 by gamma irradiation followed by negative selection using monoclonal antibodies specific for the appropriate HLA allele. Several variants were derived that lacked one or more class I antigen expressions. These variants were analyzed for the susceptibility to lysis by NK clones recognizing different allospecificities. The loss of HLA-A did not modify the phenotype (i.e., "resistance to lysis"). On the other hand, a variant lacking expression of all class I antigens became susceptible to lysis by all alloreactive clones. Variants characterized by the selective loss of class I antigens coded for by the maternal chromosome became susceptible to lysis by anti-2-specific clones. Conversely, variants selectively lacking class I antigens coded for by paternal chromosome became susceptible to lysis by anti-1 and anti-5 clones (but not by anti-2 clones). Since the Cw3 allele was lost in the variant that acquired susceptibility to lysis by anti-2 clones and, in informative families, it was found to cosegregate with the character "resistance to lysis" by anti-2 clones, we analyzed whether Cw3 could represent the element conferring selective resistance to lysis by anti-2 clones. To this end, murine P815 cells transfected with HLA Cw3 (or with other HLA class I genes) were used as target cells in a cytolytic assay in which effector cells were represented by alloreactive NK clones directed against different specificities. Anti-2-specific clones efficiently lysed untransfected or A2-, A3-, and A24-transfected P815 cells, while they failed to lyse Cw3-transfected cells. NK clones recognizing specificities other than specificity 2 lysed untransfected or Cw3- transfected cells. Thus, the loss of Cw3 resulted in the de novo appearance of susceptibility to lysis, and transfection of the HLA- negative P815 cells with Cw3 resulted in resistance to lysis by anti-2 clones. Therefore, we can infer that Cw3 expression on (both human and murine) target cells confers selective protection from lysis mediated by anti-2 NK clones.
机译:本研究旨在鉴定天然杀伤(NK)细胞介导的正常同种异体靶细胞识别的靶分子。如先前所示,发现第一个由NK定义的同种异体特异性(特异性1)的基因位于BF基因和HLA-A之间的主要组织相容性复合体区域。此外,对先前描述的家族的分析表明,供体(供体81)对于三种不同的NK定义的同种异体(特异性1、2和5)是杂合的。 HLA变体是通过γ射线从供体81的B-Epstein-Barr病毒细胞系衍生而来,然后通过使用对合适的HLA等位基因具有特异性的单克隆抗体进行阴性选择。衍生了几种缺乏一种或多种I类抗原表达的变体。通过识别不同同种异体特异性的NK克隆分析了这些变体的裂解敏感性。 HLA-A的丧失没有改变表型(即“抗裂解性”)。另一方面,缺乏所有I类抗原表达的变体易于被所有同种异体反应性克隆裂解。以母体染色体编码的I类抗原选择性丧失为特征的变体变得易于被抗2特异性克隆裂解。相反,选择性缺乏由父本染色体编码的I类抗原的变体变得易于被抗-1和抗5克隆(而不是抗2克隆)裂解。由于Cw3等位基因在通过抗2克隆获得裂解敏感性的变体中丢失,并且在信息丰富的家族中,发现它与通过抗2克隆获得的“抗裂解性”特征共分离,因此我们分析了Cw3是否可以代表赋予对抗2克隆的裂解具有选择性抗性的元件。为此,用HLA Cw3(或其他HLA I类基因)转染的鼠P815细胞在溶细胞试验中用作靶细胞,其中效应细胞由针对不同特异性的同种反应性NK克隆代表。抗2特异克隆可有效裂解未转染的或A2,A3和A24转染的P815细胞,而它们却无法裂解Cw3转染的细胞。 NK克隆识别除特异性2裂解的未转染或Cw3转染的细胞以外的特异性。因此,Cw3的丧失导致从头出现对裂解的敏感性,并且用Cw3转染HLA-阴性P815细胞对CLA-3的抗裂解性产生抗性。因此,我们可以推断Cw3在(人类和鼠类)靶细胞上的表达赋予了针对抗2 NK克隆介导的裂解的选择性保护。

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