一例ZMPSTE24基因复合杂合突变导致颅骨下颌骨皮肤发育不全B型的诊断和基因检测分析

doi:10.16288/j.yczz.22-117

遗传 ›› 2022, Vol. 44 ›› Issue (12): 1167-1174.doi: 10.16288/j.yczz.22-117

一例ZMPSTE24基因复合杂合突变导致颅骨下颌骨皮肤发育不全B型的诊断和基因检测分析

吴丹丹(), 李荣(), 李晓南, 刘倩琦, 窦莉华

南京医科大学附属儿童医院儿童保健科，南京 210008

收稿日期:2022-07-25 修回日期:2022-09-06 出版日期:2022-12-20 发布日期:2022-09-15
通讯作者: 李荣 E-mail:nantongwudandan@163.com;15850780062@163.com
作者简介:吴丹丹，硕士，主治医师，研究方向：儿童发育行为。E-mail: nantongwudandan@163.com

Diagnosis and genetic analysis of a case with mandibuloacral dysplasia type B due to compound heterozygous mutations of the ZMPSTE24 gene

Dandan Wu(), Rong Li(), Xiaonan Li, Qianqi Liu, Lihua Dou

Child Healthcare Department, Children’s Hospital of Nanjing Medical University, Nanjing 210008, China

Received:2022-07-25 Revised:2022-09-06 Online:2022-12-20 Published:2022-09-15
Contact: Li Rong E-mail:nantongwudandan@163.com;15850780062@163.com

摘要/Abstract

摘要：

颅骨下颌骨皮肤发育不全(mandibuloacral dysplasia，MAD)是一种罕见的常染色体隐性遗传疾病，主要与LMNA及ZMPSTE24基因发生变异有关。本文报道了国内首例颅骨下颌骨皮肤发育不全B型患者，主要表现为特殊面容、喂养困难、体格生长明显落后、全面的发育迟缓伴牙齿和骨骼发育异常。全外显子组家系测序结果显示患者携带ZMPSTE24基因c.743C>T (p.Pro248Leu) (dbSNP: rs121908095)与1~10号外显子缺失的复合杂合突变，经Sanger测序与定量聚合酶链反应(real-time quantitative PCR, RT-qPCR)实验检测显示，两个突变分别遗传自其表型正常的母亲与父亲。通过总结分析该例病例特点及其家系遗传规律，对于临床上难以进行明确诊断的疾病，建议进行全外显子组家系测序，辅助疾病的诊断。该病例的发现提高了临床医师对MAD疾病的认识，也为该疾病后续的遗传学研究提供新的临床资料。

关键词: ZMPSTE24基因, 颅骨下颌骨皮肤发育不全B型, 全外显子组测序

Abstract:

Mandibuloacral dysplasia (MAD) is a rare autosomal recessive disorder, mainly caused by pathogenic variants of the LMNA and ZMPSTE24 genes. In this study, we reported the first case of a patient with type B cranial and mandibular dysplasia in China. The patient presented with distinctive facial features, feeding difficulties, significant physical retardation, and overall developmental delay with abnormal tooth and bone development. Trio-whole exome sequencing analysis showed that the patient carried compound heterozygous mutations of c.743C>T (p.Pro248Leu) (dbSNP: rs121908095) and the loss of exons 1-10 of the ZMPSTE24 gene. Sanger sequencing and real-time quantitative PCR (RT-qPCR) showed that these two mutations were inherited from the patient’s phenotypically normal mother and father, respectively. By summarizing and analyzing the characteristics of this case and the pedigree of the family, we suggested that trio-whole-exome sequencing could be performed to assist in the diagnosis of diseases that are difficult to be diagnosed definitively based on clinical phenotypes. The publication of this case has improved clinicians’ understanding of MAD disease and provide new clinical information for the subsequent genetic study of this disease.

Key words: ZMPSTE24, mandibuloacral dysplasia type B, whole exome sequencing

吴丹丹, 李荣, 李晓南, 刘倩琦, 窦莉华. 一例ZMPSTE24基因复合杂合突变导致颅骨下颌骨皮肤发育不全B型的诊断和基因检测分析[J]. 遗传, 2022, 44(12): 1167-1174.

Dandan Wu, Rong Li, Xiaonan Li, Qianqi Liu, Lihua Dou. Diagnosis and genetic analysis of a case with mandibuloacral dysplasia type B due to compound heterozygous mutations of the ZMPSTE24 gene[J]. Hereditas(Beijing), 2022, 44(12): 1167-1174.

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参考文献 10

[1]	Simha V, Garg A. Body fat distribution and metabolic derangements in patients with familial partial lipodystrophy associated with mandibuloacral dysplasia. J Clin Endocrinol Metab, 2002, 87(2): 776-785. doi: 10.1210/jcem.87.2.8258
[2]	Shen JJ, Brown CA, Lupski JR, Potocki L. Mandibuloacral dysplasia is caused by homozygosity for the R527H mutation in lamin A/C. J Med Genet, 2003, 40(11): 854-857. pmid: 14627682
[3]	Novelli G, Muchir A, Sangiuolo F, Helbing-Leclerc A, D'Apice MR, Massart C, Sbraccia P, Federice M, Lauro R, Tudisco C, Pollatta R, Scarano G, Dallapiccola B, Merlini L, Bonne G. Mandibuloacral dysplasia is caused by a mutation in LMNA-encoding lamin A/C. Am J Hum Genet, 2002, 71(2): 426-431. pmid: 12075506
[4]	Agarwal AK, Kazachkova I, Ten S, Garg A. Severe mandibuloacral dysplasia-associated lipodystrophy and progeria in a young girl with a novel homozygous Arg527Cys LMNA mutation. J Clin Endocrinol Metab, 2008, 93(12):4617-4623. doi: 10.1210/jc.2008-0123
[5]	Agarwal AK, Fryns JP, Auchus RJ, Garg A. Zinc metalloproteinase, ZMPSTE24, is mutated in mandibuloacral dysplasia. Hum Mol Genet, 2003, 12(16): 1995-2001. pmid: 12913070
[6]	Lattanzi G, Benedetti S, Bertini E, Boriani G, Mazzanti L, Novelli G, Pasquali R, Pini A, Politano L. Laminopathies: many diseases, one gene. Report of the first Italian meeting course on laminopathies. Acta Myol, 2011, 30(2): 138-143.
[7]	Miyoshi Y, Akagi M, Agarwal AK, Namba N, Kato- Nishimura K, Mohri I, Yamagata M, Nakajima S, Mushiake S, Shima M, Auchus RJ, Taniike M, Garg A, Ozono K. Severe mandibuloacral dysplasia caused by novel compound heterozygous ZMPSTE24 mutations in two Japanese siblings. Clin Genet, 2008, 73(6): 535-544.
[8]	Haye D, Dridi H, Levy J, Lambert V, Lambert M, Agha M, Adjimi F, Kohlhase J, Lipsker D, Verlose A. Failure of ossification of the occipital bone in mandibuloacral dysplasia type B. Am J Med Genet A, 2016, 170(10): 2750-2755. doi: 10.1002/ajmg.a.37825 pmid: 27410998
[9]	Brown RJ, Araujo-Vilar D, Cheung PT, Dunger D, Garg A, Jack M, Mungai L, Oral EA, Patni N, Rother KI, von Schnurbein J, Sorkina E, Stanley T, Vigouroux C, Wabitsch M, Williams R, Yorifuji T. The diagnosis and management of lipodystrophy syndromes: a multi-society practice guideline. J Clin Endocrinol Metab, 2016, 101(12): 4500-4511. doi: 10.1210/jc.2016-2466 pmid: 27710244
[10]	Li XZ, Huang XJ. Congenital and acquired lipodystrophies. Chin J Appl Clin Pediatr, 2015, 30(20): 1533-1537.
	李秀珍, 黄新疆. 先天性及获得性脂肪营养不良. 中华实用儿科临床杂志, 2015, 30(20): 1533-1537.

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典型症状	既往报道病例	本例患儿
先天面部畸形
外观：鸟样面容、面部脂肪丢失、颅缝闭合延迟	+	+
眼睛：眼球突出	+	+
鼻子：窄鼻梁	+	-
口腔：嘴窄、高腭、小颌畸形、牙列拥挤，牙齿发育不全、牙齿过早脱落	+	+
耳部:耳廓畸形	NA	+
毛发：毛发脆弱、头发稀疏	+	+
皮肤
斑驳状色素沉着，皮肤萎缩	+	+
骨骼
枕骨形态小	NA	+
枕骨缝间骨	+	+
短锁骨	+	-
进展性锁骨肢端骨质溶解	+	-
指骨远端骨质溶解	+	-
手指指骨短	+	+
手远关节指骨溶骨质性骨质缺损	+	-
双侧股骨、胫骨、坐骨多发骨皮质吸收改变	NA	+
脂肪分布
广泛性脂肪营养不良(颈部、躯干、四肢)	+	+
生化检验
高血糖	+	-
高脂血症	+	-
高尿酸	NA	+
高胰岛素与C肽	+	-

一例ZMPSTE24基因复合杂合突变导致颅骨下颌骨皮肤发育不全B型的诊断和基因检测分析

Diagnosis and genetic analysis of a case with mandibuloacral dysplasia type B due to compound heterozygous mutations of the ZMPSTE24 gene

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