Pediatric Department A and Immunology Service, Jeffrey Modell Foundation Center, Edmond and Lily Safra Children's Hospital, Sheba Medical Center, Tel Hashomer, Israel.
The Mina and Everard Goodman Faculty of Life Sciences, Advanced Materials and Nanotechnology Institute, Bar-Ilan University, Ramat Gan, Israel.
J Exp Med. 2021 Mar 1;218(3). doi: 10.1084/jem.20201062.
The T cell receptor (TCR) signaling pathway is an ensemble of numerous proteins that are crucial for an adequate immune response. Disruption of any protein involved in this pathway leads to severe immunodeficiency and unfavorable clinical outcomes. Here, we describe an infant with severe immunodeficiency who was found to have novel biallelic mutations in SLP76. SLP76 is a key protein involved in TCR signaling and in other hematopoietic pathways. Previous studies of this protein were performed using Jurkat-derived human leukemic T cell lines and SLP76-deficient mice. Our current study links this gene, for the first time, to a human immunodeficiency characterized by early-onset life-threatening infections, combined T and B cell immunodeficiency, severe neutrophil defects, and impaired platelet aggregation. Hereby, we characterized aspects of the patient's immune phenotype, modeled them with an SLP76-deficient Jurkat-derived T cell line, and rescued some consequences using ectopic expression of wild-type SLP76. Understanding human diseases due to SLP76 deficiency is helpful in explaining the mixed T cell and neutrophil defects, providing a guide for exploring human SLP76 biology.
T 细胞受体 (TCR) 信号通路是一组对适当免疫反应至关重要的众多蛋白质。该通路中任何蛋白的破坏都会导致严重的免疫缺陷和不良的临床结局。在这里,我们描述了一名患有严重免疫缺陷的婴儿,他被发现存在 SLP76 的新型双等位基因突变。SLP76 是 TCR 信号转导和其他造血途径中的关键蛋白。以前对该蛋白的研究是使用 Jurkat 衍生的人类白血病 T 细胞系和 SLP76 缺陷型小鼠进行的。我们目前的研究首次将该基因与一种以早期发生危及生命的感染、联合 T 和 B 细胞免疫缺陷、严重的中性粒细胞缺陷和血小板聚集受损为特征的人类免疫缺陷联系起来。在此,我们对患者的免疫表型进行了特征描述,使用 SLP76 缺陷型 Jurkat 衍生 T 细胞系对其进行建模,并通过外源性表达野生型 SLP76 挽救了一些后果。了解 SLP76 缺陷导致的人类疾病有助于解释混合性 T 细胞和中性粒细胞缺陷,为探索人类 SLP76 生物学提供指导。
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