CeMM Research Center for Molecular Medicine, Austrian Academy of Sciences, Vienna, Austria.
Haematologica. 2013 Mar;98(3):473-8. doi: 10.3324/haematol.2012.068791. Epub 2012 Jul 16.
CD27, a tumor necrosis factor receptor family member, interacts with CD70 and influences T-, B- and NK-cell functions. Disturbance of this axis impairs immunity and memory generation against viruses including Epstein Barr virus (EBV), influenza, and others. CD27 is commonly used as marker of memory B cells for the classification of B-cell deficiencies including common variable immune deficiency. Flow cytometric immunophenotyping including expression analysis of CD27 on lymphoid cells was followed by capillary sequencing of CD27 in index patients, their parents, and non-affected siblings. More comprehensive genetic analysis employed single nucleotide polymorphism-based homozygosity mapping and whole exome sequencing. Analysis of exome sequencing data was performed at two centers using slightly different data analysis pipelines, each based on the Genome Analysis ToolKit Best Practice version 3 recommendations. A comprehensive clinical characterization was correlated to genotype. We report the simultaneous confirmation of human CD27 deficiency in 3 independent families (8 patients) due to a homozygous mutation (p. Cys53Tyr) revealed by whole exome sequencing, leading to disruption of an evolutionarily conserved cystein knot motif of the transmembrane receptor. Phenotypes varied from asymptomatic memory B-cell deficiency (n=3) to EBV-associated hemophagocytosis and lymphoproliferative disorder (LPD; n=3) and malignant lymphoma (n=2; +1 after LPD). Following EBV infection, hypogammaglobulinemia developed in at least 3 of the affected individuals, while specific anti-viral and anti-polysaccharide antibodies and EBV-specific T-cell responses were detectable. In severely affected patients, numbers of iNKT cells and NK-cell function were reduced. Two of 8 patients died, 2 others underwent allogeneic hematopoietic stem cell transplantation successfully, and one received anti-CD20 (rituximab) therapy repeatedly. Since homozygosity mapping and exome sequencing did not reveal additional modifying factors, our findings suggest that lack of functional CD27 predisposes towards a combined immunodeficiency associated with potentially fatal EBV-driven hemo-phagocytosis, lymphoproliferation, and lymphoma development.
CD27 是肿瘤坏死因子受体家族的一员,与 CD70 相互作用,影响 T、B 和 NK 细胞的功能。该轴的紊乱会损害针对包括 EBV(爱泼斯坦-巴尔病毒)、流感在内的病毒的免疫和记忆生成。CD27 通常被用作记忆 B 细胞的标志物,用于分类包括常见可变免疫缺陷在内的 B 细胞缺陷。首先对淋巴细胞进行流式细胞免疫表型分析,包括 CD27 的表达分析,然后对索引患者、其父母和无病兄弟姐妹进行 CD27 的毛细管测序。更全面的遗传分析采用基于单核苷酸多态性的纯合性映射和全外显子组测序。使用稍微不同的数据分析管道在两个中心分析外显子组测序数据,每个管道都基于基因组分析工具包最佳实践版本 3 的建议。对基因型进行了全面的临床特征分析。我们报告了由于全外显子组测序揭示的纯合突变(p.Cys53Tyr),在 3 个独立的家庭(8 名患者)中同时确认了人类 CD27 缺陷,该突变导致跨膜受体的进化保守半胱氨酸结基序中断。表型从无症状记忆 B 细胞缺陷(n=3)到 EBV 相关噬血细胞和淋巴组织增生性疾病(LPD;n=3)和恶性淋巴瘤(n=2;+1 后 LPD)不等。在 EBV 感染后,至少 3 名受影响的个体出现低丙种球蛋白血症,而可检测到针对特定病毒和多糖的抗体以及 EBV 特异性 T 细胞反应。在严重受影响的患者中,iNKT 细胞数量和 NK 细胞功能减少。8 名患者中有 2 名死亡,2 名患者成功接受了同种异体造血干细胞移植,1 名患者反复接受抗 CD20(利妥昔单抗)治疗。由于纯合性映射和外显子组测序未发现其他修饰因子,我们的研究结果表明,缺乏功能性 CD27 易导致与潜在致命 EBV 驱动的噬血细胞、淋巴增生和淋巴瘤发展相关的联合免疫缺陷。
