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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >DARC extracellular domain remodeling in maturating reticulocytes explains Plasmodium vivax tropism
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DARC extracellular domain remodeling in maturating reticulocytes explains Plasmodium vivax tropism

机译:成熟网状细胞中的DARC细胞外结构域改造解释了疟原虫vivax rootism

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Plasmodium vivax is the most prevalent parasite species that causes malaria in humans and exclusively infects reticulocytes. Reticulocyte infection is facilitated by P vivax Duffy binding protein (DBP), which utilizes DARC (Duffy antigen receptor for chemokines) as an entry point. However, the selective tropismofPvivax for transferrin receptor (CD71)-positive reticulocytes remained unexplained, given the constitutive expression of DARC during reticulocyte maturation. CD71/RNA double staining of reticulocytes enriched from adult peripheral blood reveals 4 distinct reticulocyte populations: CD71 (high)/RNAhigh (similar to 0.016%), CD71(low)/RNA(high) (similar to 0.059%), CD71(neg)/RNA(high) (similar to 0.37%), CD71(neg)/RNA(low) (similar to 0.55%), and erythrocytes CD71(neg)/RNA(neg) (similar to 99%). Wehypothesized that selective association of DBP with as mall population of immature reticulocytes could explain the preference of P vivax for reticulocytes. Binding of specific monoclonal anti-DARC antibodies and recombinant DBP to CD71(high)/RNA(high) reticulocytes was significantly higher compared with other reticulocyte populations and erythrocytes. Interestingly, the total DARC protein throughout reticulocyte maturation was constant. The data suggest that selective exposure of the DBP binding site within DARC is key to the preferential binding of DBP to immature reticulocytes, which is the potential mechanism underlying the preferential infection of a reticulocyte subset by P vivax.
机译:疟原虫疟原虫是最常见的寄生虫物种,导致人类疟疾,并专门感染网状细胞。通过P Vivax Duffy结合蛋白(DBP)促进了网状细胞感染,其利用DARC(Duffy抗原受体用于趋化因子)作为入口点。然而,鉴于在网状细胞成熟期间DARC的组成型表达,对转铁蛋白受体(CD71)的选择性Tropismofpvivax仍然是未解释的。从成年外周血中富集的网状细胞的CD71 / RNA双染色显示出4种不同的网状细胞群:CD71(高)/ Rnahigh(类似于0.016%),CD71(低)/ RNA(高)(类似于0.059%)CD71(Neg )/ RNA(高)(类似于0.37%),CD71(NEG)/ RNA(低)(类似于0.55%),和红细胞CD71(NEC)/ RNA(NEG)(类似于99%)。 Wehypothesized认为DBP的选择性与未成熟的网状细胞的商场群体可以解释P vivax用于网状细胞的偏好。与其他网状细胞群和红细胞相比,特异性单克隆抗DARC抗体和重组DBP对CD71(高)/ RNA(高)网(高)网的结合显着高得多。有趣的是,整个网状细胞成熟的总DARC蛋白是恒定的。该数据表明,DARC内的DBP结合位点的选择性暴露是DBP对未成熟括约肌细胞的优先结合的关键,这是PVivax括号子集优先感染的潜在机制。

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