Mou Wenjun, He Jianxin, Chen Xi, Zhang Hui, Ren Xiaoya, Wu Xunyao, Ni Xin, Xu Baoping, Gui Jingang
Key Laboratory of Major Diseases in Children, Ministry of Education, Beijing Children's Hospital, Capital Medical University, Beijing, China.
Laboratory of Immunology, Beijing Pediatric Research Institute, Beijing Children's Hospital, Capital Medical University, Beijing, 100045, China.
Immunogenetics. 2017 Jan;69(1):29-38. doi: 10.1007/s00251-016-0949-3. Epub 2016 Aug 26.
Severe combined immunodeficiency (SCID) is the most serious disorder among primary immunodeficiency diseases threatening children's life. Atypical SCID variant, presenting with mild reduced T cells subsets, is often associated with infection susceptibility but poor clinical diagnosis. The atypical X-SCID patient in the present study showed a mild clinical presentation with a TNKB immunophenotype. The patient has reduced T- cell subpopulations with a subdued thymic output measured by sjTRECs. Further analysis showed that T cells maintained a normal proliferation and a broad Vβ repertoire. NK cells, however, exhibited a skewed development toward immature CD3CD16CD56 cells. Genetic analysis revealed a novel deletion at nucleotide 52 in exon 1 of IL2RG gene. Sequence alignment predicted a truncated IL2RG protein missing signal peptide derived from a possible alternative reading frame. The novel mutation in IL2RG gene identified in our study may help the early diagnosis of atypical X-SCID.
重症联合免疫缺陷(SCID)是原发性免疫缺陷疾病中最严重的一种,威胁着儿童的生命。非典型SCID变异型表现为T细胞亚群轻度减少,常伴有感染易感性,但临床诊断困难。本研究中的非典型X-SCID患者表现为轻度临床表现和TNKB免疫表型。该患者T细胞亚群减少,通过sjTRECs测量胸腺输出减弱。进一步分析表明,T细胞保持正常增殖和广泛的Vβ谱系。然而,NK细胞表现出向未成熟CD3CD16CD56细胞的偏向性发育。基因分析揭示了IL2RG基因第1外显子核苷酸52处的一个新缺失。序列比对预测了一个截短的IL2RG蛋白,该蛋白缺失了可能来自另一个可读框的信号肽。我们研究中鉴定出的IL2RG基因新突变可能有助于非典型X-SCID的早期诊断。
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