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马CD89的克隆与特性分析以及黑猩猩和恒河猴中CD89基因的鉴定。

Cloning and characterization of equine CD89 and identification of the CD89 gene in chimpanzees and rhesus macaques.

作者信息

Morton H Craig, Pleass Richard J, Storset Anne K, Brandtzaeg Per, Woof Jenny M

机构信息

Laboratory for Immunohistochemistry and Immunopathology (LIIPAT), Institute of Pathology, Rikshospitalet, University Hospital, Oslo, Norway.

出版信息

Immunology. 2005 May;115(1):74-84. doi: 10.1111/j.1365-2567.2005.02129.x.

Abstract

Immunoglobulin A (IgA) is the major antibody class present in external secretions of mammals. At the vulnerable mucosal surfaces, IgA provides a crucial first-line defence by neutralizing pathogens. Primates also have a substantial level of IgA in serum and although not well understood, the biological role of this IgA depends, at least partly, on its ability to interact with specific receptors (FcalphaRs) on the surface of leucocytes. The human FcalphaR, CD89, was the first IgA Fc receptor to be identified and binding of IgA-coated particles to CD89 triggers numerous cellular effector functions, including phagocytosis, antibody-dependent cellular cytotoxicity, and release of inflammatory mediators, all of which may play an important role in both systemic and mucosal immunity. For many years humans were the only species known to express CD89, however, it has recently been cloned from cows and rats. Here, we describe the identification of the CD89 gene in three additional species: horses, chimpanzees, and Rhesus macaques. Equine CD89 was identified at the cDNA level, whereas the chimpanzee and Rhesus macaque genes were identified from the available draft genomic sequence. Interestingly, when compared with humans and other primates, horses, cows and rats have a relatively low concentration of serum IgA, so the role of CD89 in these species is of particular interest. The identification and characterization of CD89 in different species will contribute to a greater understanding of the biological role of IgA and CD89 in mucosal and systemic immunity throughout evolution.

摘要

免疫球蛋白A(IgA)是哺乳动物外分泌液中存在的主要抗体类别。在易受侵害的黏膜表面,IgA通过中和病原体提供关键的一线防御。灵长类动物血清中也有相当水平的IgA,尽管其生物学作用尚未完全明确,但这种IgA的生物学作用至少部分取决于其与白细胞表面特定受体(FcalphaRs)相互作用的能力。人类FcalphaR即CD89是首个被鉴定出的IgA Fc受体,IgA包被颗粒与CD89的结合会触发多种细胞效应功能,包括吞噬作用、抗体依赖性细胞毒性以及炎症介质的释放,所有这些在全身免疫和黏膜免疫中都可能发挥重要作用。多年来,人类是已知唯一表达CD89的物种,然而,最近已从牛和大鼠中克隆出该基因。在此,我们描述了在另外三个物种:马、黑猩猩和恒河猴中CD89基因的鉴定情况。马的CD89是在cDNA水平上鉴定出来的,而黑猩猩和恒河猴的基因则是从可用的基因组序列草图中鉴定出来的。有趣的是,与人类和其他灵长类动物相比,马、牛和大鼠的血清IgA浓度相对较低,因此CD89在这些物种中的作用尤其令人感兴趣。不同物种中CD89的鉴定和表征将有助于更深入地了解IgA和CD89在整个进化过程中在黏膜免疫和全身免疫中的生物学作用。

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