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犬类CD1基因座拓扑结构的优化及抗体与重组犬类CD1亚型结合的研究。

Refinement of the canine CD1 locus topology and investigation of antibody binding to recombinant canine CD1 isoforms.

作者信息

Schjaerff Mette, Keller Stefan M, Fass Joseph, Froenicke Lutz, Grahn Robert A, Lyons Leslie, Affolter Verena K, Kristensen Annemarie T, Moore Peter F

机构信息

Department of Veterinary Clinical and Animal Sciences, Faculty of Health and Medical Sciences, University of Copenhagen, Dyrlaegevej 16, 1870, Frederiksberg C, Denmark.

Department of Veterinary Pathology, Microbiology and Immunology, University of California, One Shields Avenue, Davis, CA, 95616, USA.

出版信息

Immunogenetics. 2016 Mar;68(3):191-204. doi: 10.1007/s00251-015-0889-3. Epub 2015 Dec 21.

Abstract

CD1 molecules are antigen-presenting glycoproteins primarily found on dendritic cells (DCs) responsible for lipid antigen presentation to CD1-restricted T cells. Despite their pivotal role in immunity, little is known about CD1 protein expression in dogs, notably due to lack of isoform-specific antibodies. The canine (Canis familiaris) CD1 locus was previously found to contain three functional CD1A genes: canCD1A2, canCD1A6, and canCD1A8, where two variants of canCD1A8, canCD1A8.1 and canCD1A8.2, were assumed to be allelic variants. However, we hypothesized that these rather represented two separate genes. Sequencing of three overlapping bacterial artificial chromosomes (BACs) spanning the entire canine CD1 locus revealed canCD1A8.2 and canCD1A8.1 to be located in tandem between canCD1A7 and canCD1C, and canCD1A8.1 was consequently renamed canCD1A9. Green fluorescent protein (GFP)-fused canine CD1 transcripts were recombinantly expressed in 293T cells. All proteins showed a highly positive GFP expression except for canine CD1d and a splice variant of canine CD1a8 lacking exon 3. Probing with a panel of anti-CD1 monoclonal antibodies (mAbs) showed that Ca13.9H11 and Ca9.AG5 only recognized canine CD1a8 and CD1a9 isoforms, and Fe1.5F4 mAb solely recognized canine CD1a6. Anti-CD1b mAbs recognized the canine CD1b protein, but also bound CD1a2, CD1a8, and CD1a9. Interestingly, Ca9.AG5 showed allele specificity based on a single nucleotide polymorphism (SNP) located at position 321. Our findings have refined the structure of the canine CD1 locus and available antibody specificity against canine CD1 proteins. These are important fundamentals for future investigation of the role of canine CD1 in lipid immunity.

摘要

CD1分子是主要存在于树突状细胞(DCs)上的抗原呈递糖蛋白,负责将脂质抗原呈递给受CD1限制的T细胞。尽管它们在免疫中起关键作用,但关于犬类中CD1蛋白的表达却知之甚少,尤其是由于缺乏亚型特异性抗体。先前发现犬(犬科动物)CD1基因座包含三个功能性CD1A基因:canCD1A2、canCD1A6和canCD1A8,其中canCD1A8的两个变体canCD1A8.1和canCD1A8.2被认为是等位基因变体。然而,我们推测这些更像是两个独立的基因。对跨越整个犬类CD1基因座的三个重叠细菌人工染色体(BACs)进行测序后发现,canCD1A8.2和canCD1A8.1串联位于canCD1A7和canCD1C之间,因此canCD1A8.1被重新命名为canCD1A9。绿色荧光蛋白(GFP)融合的犬类CD1转录本在293T细胞中重组表达。除了犬类CD1d和缺少外显子3的犬类CD1a8剪接变体之外,所有蛋白质均显示出高度阳性的GFP表达。用一组抗CD1单克隆抗体(mAbs)进行检测表明,Ca13.9H11和Ca9.AG5仅识别犬类CD1a8和CD1a9亚型,而Fe1.5F4单克隆抗体仅识别犬类CD1a6。抗CD1b单克隆抗体识别犬类CD1b蛋白,但也与CD1a2、CD1a8和CD1a9结合。有趣的是,Ca9.AG5基于位于321位的单核苷酸多态性(SNP)表现出等位基因特异性。我们的研究结果完善了犬类CD1基因座的结构以及针对犬类CD1蛋白的现有抗体特异性。这些是未来研究犬类CD1在脂质免疫中作用的重要基础。

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