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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >The CXCR4 mutations in WHIM syndrome impair the stability of the T-cell immunologic synapse.
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The CXCR4 mutations in WHIM syndrome impair the stability of the T-cell immunologic synapse.

机译:WHIM综合征中的CXCR4突变会损害T细胞免疫突触的稳定性。

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WHIM (warts, hypogammaglobulinemia, infections, myelokathexis) syndrome is a rare disease characterized by diverse symptoms indicative of aberrantly functioning immunity. It is caused by mutations in the chemokine receptor CXCR4, which impair its intracellular trafficking, leading to increased responsiveness to chemokine ligand and retention of neutrophils in bone marrow. Yet WHIM symptoms related to adaptive immunity, such as delayed IgG switching and impaired memory B-cell function, remain largely unexplained. We hypothesized that the WHIM-associated mutations in CXCR4 may affect the formation of immunologic synapses between T cells and antigen-presenting cells (APCs). We show that, in the presence of competing external chemokine signals, the stability of T-APC conjugates from patients with WHIM-mutant CXCR4 is disrupted as a result of impaired recruitment of the mutant receptor to the immunologic synapse. Using retrogenic mice that develop WHIM-mutant T cells, we show that WHIM-mutant CXCR4 inhibits the formation of long-lasting T-APC interactions in ex vivo lymph node slice time-lapse microscopy. These findings demonstrate that chemokine receptors can affect T-APC synapse stability and allow us to propose a novel mechanism that contributes to the adaptive immune response defects in WHIM patients.
机译:WHIM(疣,低聚球蛋白血症,感染,骨髓病)综合征是一种罕见的疾病,其特征是多种多样的症状表明免疫功能异常。它是由趋化因子受体CXCR4的突变引起的,该突变削弱了它的细胞内运输,导致对趋化因子配体的反应性增强以及中性粒细胞在骨髓中的滞留。然而,与适应性免疫相关的WHIM症状,如延迟的IgG转换和记忆B细胞功能受损,仍然无法解释。我们假设CXCR4中WHIM相关的突变可能影响T细胞和抗原呈递细胞(APC)之间的免疫突触的形成。我们显示,在存在竞争性外部趋化因子信号的情况下,由于突变受体向免疫突触的募集受损,来自WHIM突变CXCR4患者的T-APC缀合物的稳定性受到破坏。使用开发WHIM突变T细胞的逆转录小鼠,我们显示WHIM突变CXCR4抑制离体淋巴结切片延时显微镜中的持久T-APC相互作用的形成。这些发现表明趋化因子受体可以影响T-APC突触的稳定性,并允许我们提出一种新的机制,有助于WHIM患者的适应性免疫应答缺陷。

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