Objective: To summarize the clinical and genetic characteristics of pseudoachondroplasia and multiple epiphyseal dysplasia caused by COMP gene variants in pediatric patients. Methods: This retrospective study concluded 15 pediatric patients with COMP-related pseudoachondroplasia and multiple epiphyseal dysplasia at Shanghai Children's Medical Center, Shanghai Jiao Tong University School of Medicine from July 2013 to August 2024. This paper analyzed clinical manifestations, laboratory findings and genetic testing. Results: This cohort comprised 15 pediatric patients (8 males and 7 females) with a diagnostic age of 5.3 (1.8,9.3) years. The major clinical presentations included abnormal gait (15/15), brachydactyly (11/15), genu varum (12/15), irregular metaphyseal changes (14/14) and epiphyseal dysplasia (14/14). Genetic analysis revealed 13 cases of pseudoachondroplasia and 2 multiple epiphyseal dysplasias cases associated with COMP gene variants. Fifteen variants were identified (8 pathogenic and 7 likely pathogenic), including 2 novel variants (c.1223A>G, c.1378G>C). Thirteen of these patients had variations clustered in exons 8-14 encoding the calmodulin-like domains, with c.1414_1419dupGACGAC emerging as a hotspot variant. Conclusions: COMP-related pseudoachondroplasia and multiple epiphyseal dysplasia predominantly manifest with gait abnormalities and skeletal deformities. COMP gene pathogenic variations were mainly located in calmodulin-like domains.
目的: 总结COMP基因变异导致假性软骨发育不良和多发性骨骺发育不良患儿的临床与遗传学特点。 方法: 回顾性病例分析。收集2013年7月至2024年8月在上海交通大学医学院附属上海儿童医学中心就诊的15例COMP基因变异导致假性软骨发育不良和多发性骨骺发育不良患儿的临床资料,分析其临床表现、实验室检查及基因检测结果等。 结果: 15例患儿中男8例、女7例,诊断年龄为5.3(1.8,9.3)岁,主要表现包括步态异常(15/15)、短指(11/15)、膝内翻(12/15)、不规则的干骺端(14/14)及骨骺发育异常(14/14)等。15个COMP基因变异分别导致假性软骨发育不良13例和多发性骨骺发育不良2例,其中8个为“致病性变异”,7个为“可能致病性变异”,有2个新发现变异(c.1223A>G,c.1378G>C)。13例患儿变异位点处在8~14号外显子即钙调蛋白样结构域,热点变异位点为c.1414_1419dupGACGAC。 结论: COMP基因变异导致假性软骨发育不良和多发性骨骺发育不良的主要临床特征为步态异常和骨骼畸形,致病基因变异位点主要集中在钙调蛋白结构域。.