一个约旦家庭中罕见的阿拉扎米综合征近亲病例:临床表现、遗传分析和治疗方法--病例报告

Irshaid Fawzi, Alawneh Salim, Al Souhail Qasim, Alshdefat Aisha, Irshaid Bashar, Irshaid Ahmed
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摘要

目的:阿拉扎米综合征(AS)是一种不常见的常染色体隐性遗传疾病,其特点是存在多种先天性畸形。本研究探讨了一例患有 AS 的 4 岁女孩,研究内容包括症状、遗传因素和治疗效果。病例报告:一名 4 岁女孩的父母是近亲结婚的约旦人,她的畸形特征包括出生体重低、小头畸形、甲状腺功能亢进、身材矮小、蓝色巩膜、三角形脸、深陷的眼睛、狭窄的睑裂、前额突出。检查显示,身高(92 厘米)和体重(7.7 千克)分别低于第 5 百分位数和第 3 百分位数。血液化验和肾脏超声检查均正常。全外显子组测序(WES)发现,患者染色体4q25上的LARP7基因第5外显子上有一个8碱基对的同源缺失,确诊为AS,这是一种常染色体隐性遗传疾病。这种变异会诱发移帧突变,导致过早的终止密码子,这表明其发病机制可能是功能缺失。通过生长监测和治疗,三个月内身高、体重和沟通能力均有明显改善。结论我们描述了一个罕见的常染色体隐性遗传强直性脊柱炎病例,该病例由近亲结婚引起,通过 WES 发现 LARP7 基因存在框移位突变。我们的强直性脊柱炎治疗方案能有效缓解症状,促进发育。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A Rare Consanguineous Case of Alazami Syndrome in a Jordanian Family: Clinical Presentation, Genetic Analysis, and Therapeutic Approaches - A Case Report
Objective: Alazami syndrome (AS) is an infrequent genetic disorder inherited in an autosomal recessive pattern, characterized by the presence of multiple congenital abnormalities. This study explores a case of a 4-year-old girl with AS, examining symptoms, genetic factors, and treatment efficacy. Case report: A 4-year-old girl, born to consanguineous Jordanian parents, displayed dysmorphic features including low birth weight, microcephaly, hyperthyroidism, short stature, blue sclera, triangular-shaped face, deep-set eyes, narrow palpebral fissures, and a prominent forehead. Examination revealed height (92 cm) and weight (7.7 kg) below the 5th and 3rd percentiles respectively. Blood tests and renal ultrasound were normal. Whole exome sequencing (WES) identified a homozygous eight-base pair deletion within exon 5 of the LARP7 gene on chromosome 4q25, confirming the diagnosis of AS, an autosomal recessive disorder. This variant induces frameshift mutations leading to premature stop codons, suggesting a probable mechanism of illness via loss of function. Treatment involving growth monitoring and therapy led to significant improvements in height, weight, and communication skills within three months. Conclusion: We describe a rare autosomal recessive AS case due to consanguinity, with a frameshift mutation in the LARP7 gene found via WES. Our AS treatment program effectively alleviates symptoms and enhances developmental progress.
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