[史密斯-马吉尼斯综合征]
[Smith-Magenis syndrome].
作者信息
Lacombe D, Moncla A, Malzac P, Mattei M G, Battin J
机构信息
Service de pédiatrie et de génétique médicale, hôpital Pellegrin-Enfants, Bordeaux, France.
出版信息
Arch Pediatr. 1997 May;4(5):438-42. doi: 10.1016/s0929-693x(97)86671-7.
BACKGROUND
The main features of the Smith-Magenis syndrome include broad flat midface, brachycephaly, broad nasal bridge, brachydactyly, hoarse deep voice, speech and developmental delay, and behavioral anomalies. This syndrome is due to interstitial deletion of chromosome 17p11.2.
CASE REPORT
A 7-year-old girl was admitted for mental retardation. Clinical examination showed brachycephaly, broad flat midface, broad nasal bridge, malar hypoplasia, brachydactyly, decreased or absent deep tendon reflexes, and hoarse deep voice. She had a mild deafness, behavioral problems, and sleep disturbances. Chromosome analysis on lymphocytes identified a microdeletion of one chromosome subband 17p11.2. Molecular studies indicated loss of maternal allele.
CONCLUSION
The Smith-Magenis syndrome is probably underdiagnosed because of its usually mild clinical features. High-resolution chromosome analysis is needed for diagnosis.
背景
史密斯-马吉尼斯综合征的主要特征包括面部中部宽阔扁平、短头畸形、鼻梁宽阔、短指畸形、声音嘶哑低沉、言语和发育迟缓以及行为异常。该综合征是由于17p11.2染色体间质缺失所致。
病例报告
一名7岁女孩因智力发育迟缓入院。临床检查显示短头畸形、面部中部宽阔扁平、鼻梁宽阔、颧骨发育不全、短指畸形、腱反射减弱或消失以及声音嘶哑低沉。她有轻度耳聋、行为问题和睡眠障碍。淋巴细胞染色体分析发现一条17p11.2染色体亚带微缺失。分子研究表明母本等位基因缺失。
结论
史密斯-马吉尼斯综合征可能因临床特征通常较轻而诊断不足。诊断需要进行高分辨率染色体分析。
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