首页> 外文期刊>Journal of Cell Science >MHC class I molecules are an essential cell surface component involved in Theileria parva sporozoite binding to bovine lymphocytes.
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MHC class I molecules are an essential cell surface component involved in Theileria parva sporozoite binding to bovine lymphocytes.

机译:MHC I类分子是参与Theileria parva子孢子结合牛淋巴细胞的重要细胞表面成分。

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The major histocompatibility complex (MHC) class I molecules are ubiquitous cell surface molecules involved in the cell-mediated immune response. We show here, using a number of different, independent approaches, that these proteins are an essential component of the host cell surface receptor involved in Theileria parva sporozoite invasion. Monoclonal antibodies (mAbs) reactive with common determinants on MHC class I molecules and with beta-2 microglobulin inhibited sporozoite entry by specifically preventing the initial binding event. However, in experiments using lymphocytes from heterozygous cattle in which at least four MHC class I gene products are expressed, mAbs which reacted with only one of these products did not inhibit entry. Using a series of bovine deletion mutant cell lines from which one or both MHC class I haplotypes had been lost, sporozoite binding and entry clearly correlated with the level of class I surface expression. While the level of sporozoite entry into cells in which one of the MHC class I haplotypes was lost was only slightly lower than into the parent cells, in a double deletion cell line having less than 5% of the class I expression of the parent cells the level of infection was only 4.3% of that into the parent cells. Furthermore, sporozoite entry into cells from a spontaneously arising mutant cell line exhibiting low levels of class I expression was correspondingly low. Treatment of lymphocytes with IL-2 produced a significant increase in host cell susceptibility and sporozoite entry and this increase correlated with either an increase in the number of target molecules per host cell, or in the binding of bovine MHC class I molecules to the mAbs. In particular, a significant increase in the level of reactivity with mAb W6/32 was observed. Lastly, we show that parasite entry can be competitively inhibited with an isolated sporozoite surface protein, p67. However, p67 binds weakly to lymphocyte surface molecules and initial attempts to use p67 to isolate the relevant host cellmolecule(s) have not been successful.
机译:主要的组织相容性复合物(MHC)I类分子是参与细胞介导的免疫反应的普遍存在的细胞表面分子。我们在这里使用多种不同的独立方法显示,这些蛋白质是参与泰勒虫幼虫子孢子入侵的宿主细胞表面受体的重要组成部分。与MHC I类分子上的常见决定簇以及与β-2微球蛋白反应的单克隆抗体(mAb)通过特异性地防止初始结合事件而抑制了子孢子的进入。但是,在使用表达至少四个MHC I类基因产物的杂合牛淋巴细胞的实验中,仅与这些产物之一反应的mAb不会抑制进入。使用丢失了一个或两个MHC I类单倍型的一系列牛缺失突变细胞系,子孢子的结合和进入显然与I类表面表达的水平相关。虽然子孢子进入丢失了一种MHC I类单倍型的细胞的水平仅略低于亲代细胞中的水平,但在双缺失细胞系中,其子类I的表达量不到I类的5%。感染水平仅为亲代细胞感染水平的4.3%。此外,子孢子从表现出低水平的I类表达的自发产生的突变细胞系进入细胞的相应地低。用IL-2处理淋巴细胞使宿主细胞的敏感性和子孢子进入显着增加,并且这种增加与每个宿主细胞中靶分子数量的增加或牛MHC I类分子与mAb的结合有关。特别地,观察到与mAb W6 / 32的反应性水平显着增加。最后,我们显示可以通过分离的子孢子表面蛋白p67竞争性抑制寄生虫进入。但是,p67与淋巴细胞表面分子的结合较弱,使用p67分离相关宿主细胞分子的最初尝试并未成功。

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