Objective: To summarize the clinical phenotype and genetic characteristics of deficiency in ELF4 gene X-linked (DEX). Methods: A case series study was conducted to retrospectively analyze the clinical data and genetic testing results of 2 cases of DEX treated at Peking Union Medical College Hospital, Chinese Academy of Medical Sciences and the First Hospital of Jilin University from January 2023 to April 2024. And literature up to April 2024 was searched from the PubMed database, as well as CNKI and Wanfang databases, using keywords such as "ELF4 deficiency" "deficiency in ELF4, X-linked""ELF4 gene". The main clinical manifestations and genotypes of DEX were summarized. Results: Both patients were male, with onset ages of 3 months and 3 years, respectively. Both patients presented with recurrent oral ulcers and abdominal pain. And the laboratory examination showed a significant increase in inflammatory markers. Intestinal examinations showed multiple intestinal ulcers, and both patients developed intestinal fistulas. Whole exome sequencing found ELF4 c.799C>T, p Arg267Trp and ELF4 c. 248-7G>A, both maternal variants. Based on clinical and genetic results, DEX were diagnosed. In terms of treatment, both patients underwent surgical treatment during the acute phase of the disease and received anti-tumor necrosis factor α therapy, but recurrent gastrointestinal symptoms were still observed in Patient 1, while the clinical effect in Patient 2 was still acceptable. However, the inflammatory markers in both patients were not normal even after treatment. Literature review found 18 patients including 2 patients in this study, reported in 5 English articles and no Chinese reports. Thirteen patients had disease onset age before 5. The main clinical manifestations were fever (12/17), oral ulcers (14/18), abdominal pain (8/18), diarrhea (6/18), perianal ulcers (5/17), ileum ulcers (6/16), colon ulcers (7/16), skin involvement (7/17) and recurrent infections (7/18); laboratory examinations found increased erythrocyte sedimentation rate (13/15) as well as C-reactive protein (9/9), and anemia (13/15); in terms of immunological function, there is a decrease in natural killer cells (9/15) as well as a decrease in class switching memory B cells (8/9). The main types of gene variantions were missense variantions (6/18), nonsense variantions (4/18) or frameshift variantions (3/18). Conclusions: DEX should be considered when an early-onset male patient manifested with recurrent fever, oral ulcers or mucosal ulcers, with elevated inflammatory markers, with or without recurrent infection. It is recommended to perform lymphocyte subsets analysis, gastrointestinal endoscopy and genetic testing to support the diagnosis.
目的: 总结X连锁ELF4基因缺陷的临床表型和遗传学特点。 方法: 病例系列研究,回顾性分析2023年1月至2024年4月中国医学科学院北京协和医院和吉林大学第一医院诊治的2例X连锁ELF4基因缺陷的临床资料和遗传学检测结果。并分别以“ELF4 deficiency”“deficiency in ELF4,X-linked”“ELF4基因”为关键词检索PubMed数据库、中国知网、万方数据库自建库至2024年4月的中英文文献。对X连锁ELF4基因缺陷的主要临床表现和基因型特点进行描述和总结。 结果: 2例患儿均为男性,起病年龄分别为3月龄和3岁,均表现为反复口腔溃疡、腹痛,辅助检查提示炎症指标明显升高,肠道检查提示多发肠道溃疡,并发肠瘘。全外显子测序分别提示ELF4 c.799C>T,p.Arg267Trp和ELF4 c. 248-7G>A,均为母源变异,结合临床及基因结果,诊断为X连锁ELF4基因缺陷。2例患儿均在疾病急性期接受手术治疗,均接受抗肿瘤坏死因子α单抗治疗,但例1胃肠道症状反复,例2临床效果尚可,但2例患儿的炎症指标均未能降至正常。文献复习符合检索条件英文文献5篇,中文文献0篇,包括本组2例共18例患儿,13例在5岁以内起病,主要临床表现为发热(12/17)、口腔溃疡(14/18)、腹痛(8/18)、腹泻(6/18)、肛周溃疡(5/17)、小肠溃疡(6/16)、结肠溃疡(7/16)、皮肤受累(7/17)和反复感染(7/18)。辅助检查提示红细胞沉降率增快(13/15)、C反应蛋白增高(9/9)和贫血(13/15)。免疫功能存在自然杀伤细胞降低(9/15)以及类别转换的记忆B细胞的下降(8/9)。基因的变异类型中包括错义变异(6/18)、无义变异(4/18)、移码变异(3/18)。 结论: 当低龄男性患儿存在反复发热伴有口腔或黏膜溃疡或反复感染等症状,需考虑X连锁ELF4基因缺陷,建议完善淋巴细胞亚群、消化道内镜以及基因检测以明确诊断。.