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首页> 外文期刊>The Journal of Experomental Medicine >The natural killer cell receptor specific for HLA-A allotypes: a novel member of the p58/p70 family of inhibitory receptors that is characterized by three immunoglobulin-like domains and is expressed as a 140-kD disulphide-linked dimer.
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The natural killer cell receptor specific for HLA-A allotypes: a novel member of the p58/p70 family of inhibitory receptors that is characterized by three immunoglobulin-like domains and is expressed as a 140-kD disulphide-linked dimer.

机译:对HLA-A同质型特异性的天然杀伤细胞受体:P58 / P70系列抑制受体的新型成员,其特征在于三种免疫球蛋白样结构域,表示为140kd二硫键连接二聚体。

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Human natural killer (NK) cells express inhibitory receptors that are specific for different groups of HLA-C or HLA-B alleles. The majority of these receptors belong to the immunoglobulin (Ig) superfamily and are characterized by two or three extracellular Ig-like domains. Here we describe a novel inhibitory NK receptor that is specific for a group of HLA-A alleles. The HLA-A3-specific NK cell clone DP7 has been used for mice immunization. Two mAbs, termed Q66 and Q241, bound to the immunizing clone and stained only a subset of NK cell populations or clones. Among Q66 mAb-reactive clones, we further selected those that did not express any of the previously identified HLA-class I-specific NK receptors. These clones did not lyse HLA-A3+ (or -A11+) target cells, but lysis of these targets could be detected in the presence of Q66 or Q241 mAbs. On the other hand, target cells expressing other HLA-A alleles, including -A1, -A2, and -A24, were efficiently lysed. Moreover, none of the HLA-C or HLA-B alleles that were tested exerted a protective effect. Q66+, but not Q66- NK cell clones, expressed messenger RNA coding for a novel 3 Ig domain protein homologous to the HLA-C (p58) and HLA-B (p70) receptors. The corresponding cDNA (cl.1.1) was used to generate transient and stable transfectants in COS7 and NIH3T3 cell lines, respectively. Both types of transfectants were specifically stained by Q66 and Q241 mAbs. Since the cytoplasmic tail of Q66-reactive molecules was at least 11 amino acid longer than the other known p58/p70 molecules, we could generate an antiserum specific for the COOH-terminus of Q66-reactive molecules, termed PGP-3. PGP-3 immunoprecipitated, only from Q66+ NK cells, molecules displaying a molecular mass of 140 kD, under nonreducing conditions, which resolved, under reducing conditions, in a 70-kD band. Thus, differently from the other p58/p70 receptors, Q66-reactive molecules appear to be expressed as disulphide-linked dimers and were thus termed p140. The comparative analysis of the amino acid sequences of p58, p70, and p140 molecules revealed the existence of two cysteins proximal to the transmembrane region, only in the amino acid sequence of p140 molecules.
机译:人类自然杀伤(NK)细胞表达特异于不同基团的HLA-C或HLA-B等位基因的抑制受体。这些受体中的大多数属于免疫球蛋白(Ig)超家族,其特征在于两种或三个细胞外IG样结构域。在这里,我们描述了一种新的抑制性NK受体,其特异于一组HLA-A等位基因。 HLA-A3特异性NK细胞克隆DP7已用于小鼠免疫。两种MAb,称为Q66和Q241,与免疫克隆结合并仅染色NK细胞群或克隆的子集。在Q66 MAB反应克隆中,我们进一步选择了那些未表达任何先前鉴定的HLA类I特异性NK受体的那些。这些克隆没有Lyse HLA-A3 +(或-A11 +)靶细胞,但可以在Q66或Q241 MAb的存在下检测这些靶标的裂解。另一方面,有效地裂解表达其他HLA-A等位基因的靶细胞,包括-A1,-A2和-A24。此外,没有测试的HLA-C或HLA-B等位基因施加了保护作用。 Q66 +,但不是Q66-NK细胞克隆,表达了对HLA-C(P58)和HLA-B(P70)受体同源的新型3 Ig结构域蛋白的信使RNA编码。相应的cDNA(Cl.1.1)分别用于分别在COS7和NIH3T3细胞系中产生瞬时和稳定的转染剂。两种类型的转染剂由Q66和Q241 mAb具体染色。由于Q66-反应性分子的细胞质尾部比其他已知的P58 / P70分子长为至少11个氨基酸,因此我们可以产生对Q66-反应分子的COOH-末端的抗血清,称为PGP-3。 PGP-3免疫沉淀,仅来自Q66 + NK细胞,在未添加的条件下显示分子量为140kd的分子,该分子在降低条件下在70kd带中分离。因此,与其他P58 / P70受体不同,Q66-反应性分子似乎表示为二硫键连接的二聚体,因此被称为P140。 P58,P70和P140分子的氨基酸序列的对比分析显示,仅在跨膜区近端的两个半胱氨酸存在,仅在P140分子的氨基酸序列中。

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