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利用长读 RNA 测序定义恒河猴 Fcγ 受体的遗传多样性。

Defining genetic diversity of rhesus macaque Fcγ receptors with long-read RNA sequencing.

机构信息

Department of Surgery, Duke University School of Medicine, Duke University, Durham, NC, United States.

Duke Human Vaccine Institute, Duke University School of Medicine, Duke University, Durham, NC, United States.

出版信息

Front Immunol. 2024 Jan 9;14:1306292. doi: 10.3389/fimmu.2023.1306292. eCollection 2023.

Abstract

Fcγ receptors (FcγRs) are membrane-bound glycoproteins that bind to the fragment crystallizable (Fc) constant regions of IgG antibodies. Interactions between IgG immune complexes and FcγRs can initiate signal transduction that mediates important components of the immune response including activation of immune cells for clearance of opsonized pathogens or infected host cells. In humans, many studies have identified associations between FcγR gene polymorphisms and risk of infection, or progression of disease, suggesting a gene-level impact on FcγR-dependent immune responses. Rhesus macaques are an important translational model for most human health interventions, yet little is known about the breadth of rhesus macaque FcγR genetic diversity. This lack of knowledge prevents evaluation of the impact of FcγR polymorphisms on outcomes of preclinical studies performed in rhesus macaques. In this study we used long-read RNA sequencing to define the genetic diversity of FcγRs in 206 Indian-origin Rhesus macaques, . We describe the frequency of single nucleotide polymorphisms, insertions, deletions, frame-shift mutations, and isoforms. We also index the identified diversity using predicted and known rhesus macaque FcγR and Fc-FcγR structures. Future studies that define the functional significance of this genetic diversity will facilitate a better understanding of the correlation between human and macaque FcγR biology that is needed for effective translation of studies with antibody-mediated outcomes performed in rhesus macaques.

摘要

Fcγ 受体 (FcγRs) 是一种膜结合糖蛋白,可与 IgG 抗体的片段结晶区 (Fc) 恒定区结合。IgG 免疫复合物与 FcγRs 之间的相互作用可以启动信号转导,介导免疫反应的重要组成部分,包括激活免疫细胞清除调理病原体或感染宿主细胞。在人类中,许多研究已经确定了 FcγR 基因多态性与感染风险或疾病进展之间的关联,这表明基因水平对 FcγR 依赖性免疫反应有影响。恒河猴是大多数人类健康干预措施的重要转化模型,但对恒河猴 FcγR 遗传多样性的广泛程度知之甚少。这种知识的缺乏阻止了评估 FcγR 多态性对恒河猴临床前研究结果的影响。在这项研究中,我们使用长读 RNA 测序来定义 206 只印度起源的恒河猴 FcγR 的遗传多样性。我们描述了单核苷酸多态性、插入、缺失、移码突变和同工型的频率。我们还使用预测的和已知的恒河猴 FcγR 和 Fc-FcγR 结构对鉴定出的多样性进行索引。未来定义这种遗传多样性的功能意义的研究将有助于更好地理解人类和猕猴 FcγR 生物学之间的相关性,这对于有效转化恒河猴体内抗体介导的研究结果是必要的。

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