先天性少毛症一例致病基因突变研究

doi:10.3760/cma.j.issn.0412-4030.2017.11.010

Abstract

Abstract: Zhou Na, Shi Chuankui, Zhang Kaihui, Liu Yi, Gai Zhongtao Pediatric Research Institute, Qilu Children′s Hospital of Shandong University, Shandong 250022, China （Zhou N, Zhang KH, Liu Y, Gai ZT）; Department of Dermatology, Qilu Children′s Hospital of Shandong University, Shandong 250022, China （Shi CK） Corresponding authors: Gai Zhongtao, Email: gaizhongtao@sina.com; Shi Chuankui, Email: shichuankui@163.com 【Abstract】 Objective To identify the genetic cause of a case of congenital hypotrichosis by a next-generation sequencing technology. Methods A 9-year and 3-month-old girl presented with few villous hairs at birth, which grew slowly. Skin examination showed sparse, thin, soft, woolly and light-yellow hairs, small amount of hairs on the top of the head and a less amount of hairs around the head, hairline recession and broadened forehead. No abnormality was found by ophthalmic examination. No similar aberrant phenotype was observed in the patient′s parents or her younger sister. Her parents were non-consanguineous marriage. Peripheral venous blood samples were obtained from the patient, her mother and younger sister. Genomic DNA was extracted and then analyzed by a next-generation sequencing technology. The suspected pathogenic mutations were validated by Sanger sequencing and subjected to bioinformatics analysis. Results Two mutations were identified in the CDH3 gene in the patient, including a c.1057G > T （p.D353Y） heterozygous mutation in exon 5 and a c.1767delC （p.I589Ifs） heterozygous mutation in exon 10. They were both novel mutations, and their pathogenicity was predicted by softwares. Sanger sequencing indicated that the c.1057G > T （p.D353Y） heterozygous mutation was inherited from the patient′s mother, and gene transfer analysis revealed that the c.1767delC （p.I589Ifs） heterozygous mutation was inherited from the patient′s father. Conclusion The c.1057G > T （p.D353Y） and c.1767delC （p.I589Ifs） heterozygous mutations may cause hypotrichosis and juvenile macular dystrophy in the patient, so careful observation and comprehensive ophthalmic examination should be performed on time for early diagnosis and treatment of eye symptoms.

Zhou Na, Shi Chuankui, Zhang Kaihui, Liu Yi, Gai Zhongtao. Mutation analysis of causative genes in a case of congenital hypotrichosis[J]. Chinese Journal of Dermatology, 2017, 50(11): 820-824.doi:10.3760/cma.j.issn.0412-4030.2017.11.010

References ［17］

［1］	宋闯, 范卫新. 先天性秃发/少毛症的遗传学研究进展［J］. 临床皮肤科杂志, 2014, 43（12）: 753⁃758. DOI: 1000⁃4963（2014）12⁃0753⁃06.
［2］	张晓燕, 王培光, 杨森, 等. 遗传性秃发或少毛症研究进展［J］. 中国麻风皮肤病杂志, 2008, 24（9）: 721⁃723. DOI: 10.3969/j.issn.1009⁃1157.2008.09.020.
［3］	Kamran⁃ul⁃Hassan Naqvi S, Azeem Z, Ali G, et al. A novel splice⁃acceptor site mutation in CDH3 gene in a consanguineous family exhibiting hypotrichosis with juvenile macular dystrophy［J］. Arch Dermatol Res, 2010, 302（9）: 701⁃703. DOI: 10.1007/s00403⁃010⁃1035⁃6.
［4］	Indelman M, Bergman R, Lurie R, et al. A missense mutation in CDH3, encoding P⁃cadherin, causes hypotrichosis with juvenile macular dystrophy［J］. J Invest Dermatol, 2002, 119（5）: 1210⁃1213. DOI: 10.1046/j.1523⁃1747.2002.19528.x.
［5］	Indelman M, Eason J, Hummel M, et al. Novel CDH3 mutations in hypotrichosis with juvenile macular dystrophy［J］. Clin Exp Dermatol, 2007, 32（2）: 191⁃196. DOI: 10.1111/j.1365⁃2230. 2006.02335.x.
［6］	Sprecher E, Bergman R, Richard G, et al. Hypotrichosis with juvenile macular dystrophy is caused by a mutation in CDH3, encoding P⁃cadherin［J］. Nat Genet, 2001, 29（2）: 134⁃136. DOI: 10.1038/ng716.
［7］	Shimomura Y, Wajid M, Shapiro L, et al. P⁃cadherin is a p63 target gene with a crucial role in the developing human limb bud and hair follicle［J］. Development, 2008, 135（4）: 743⁃753. DOI: 10.1242/dev.006718.
［8］	Carroll DK, Carroll JS, Leong CO, et al. p63 regulates an adhesion programme and cell survival in epithelial cells［J］. Nat Cell Biol, 2006, 8（6）: 551⁃561. DOI: 10.1038/ncb1420.
［9］	Boggon TJ, Murray J, Chappuis⁃Flament S, et al. C⁃cadherin ectodomain structure and implications for cell adhesion mechanisms［J］. Science, 2002, 296（5571）: 1308⁃1313. DOI: 10.1126/science.1071559.
［10］	Steinberg MS, McNutt PM. Cadherins and their connections: adhesion junctions have broader functions［J］. Curr Opin Cell Biol, 1999, 11（5）: 554⁃560. DOI: 10.1016/S0955⁃0674（99）00027⁃7.
［11］	Yohe S, Thyagarajan B. Review of clinical next⁃generation sequencing［J/OL］. Arch Pathol Lab Med, 2017 Aug 7. https://www.ncbi.nlm.nih.gov/pubmed/28782984. ［published online ahead of print Aug 7, 2017］. DOI: 10.5858/arpa.2016⁃0501⁃RA.
［12］	Cram DS, Zhou D. Next generation sequencing: coping with rare genetic diseases in China［J］. Intractable Rare Dis Res, 2016, 5（3）: 140⁃144. DOI: 10.5582/irdr.2016.01020.
［13］	Stenson PD, Mort M, Ball EV, et al. The Human Gene Mutation Database: towards a comprehensive repository of inherited mutation data for medical research, genetic diagnosis and next⁃generation sequencing studies［J］. Hum Genet, 2017, 136（6）: 665⁃677. DOI: 10.1007/s00439⁃017⁃1779⁃6.
［14］	Maquat LE. Defects in RNA splicing and the consequence of shortened translational reading frames［J］. Am J Hum Genet, 1996, 59（2）: 279⁃286.
［15］	Troyanovsky SM. Mechanism of cell⁃cell adhesion complex assembly［J］. Curr Opin Cell Biol, 1999, 11（5）: 561⁃566. DOI: 10.1016/S0955⁃0674（99）00021⁃6.w.
［16］	Indelman M, Hamel CP, Bergman R, et al. Phenotypic diversity and mutation spectrum in hypotrichosis with juvenile macular dystrophy［J］. J Invest Dermatol, 2003, 121（5）: 1217⁃1220. DOI: 10.1046/j.1523⁃1747.2003.12550_1.x.
［17］	Kjaer KW, Hansen L, Schwabe GC, et al. Distinct CDH3 muta⁃tions cause ectodermal dysplasia, ectrodactyly, macular dystrophy （EEM syndrome）［J］. J Med Genet, 2005, 42（4）: 292⁃298. DOI: 10.1136/jmg.2004.027821.

Mutation analysis of causative genes in a case of congenital hypotrichosis

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