小头畸形-癫痫-发育迟缓症1例报告及其遗传家系图谱分析

doi:10.13481/j.1671-587x.20190237

吉林大学学报(医学版) ›› 2019, Vol. 45 ›› Issue (02): 422-425.doi: 10.13481/j.1671-587x.20190237

• 临床医学 • 上一篇

小头畸形-癫痫-发育迟缓症1例报告及其遗传家系图谱分析

梅杰, 周文莉, 闫佳秀, 郭世杰

吉林大学第一医院新生儿科, 吉林长春 130021

收稿日期:2018-11-02 发布日期:2019-03-29
通讯作者: 郭世杰,副教授,主任医师,硕士研究生导师(Tel:0431-88782771,E-mail:guoshijie1971@126.com);闫佳秀,讲师,主治医师(Tel:0431-88782771,E-mail:yan-jia-xiu@126.com) E-mail:guoshijie1971@126.com;yan-jia-xiu@126.com
作者简介:梅杰(1993-),女,河北省衡水市人,在读医学硕士,主要从事新生儿疾病方面的研究。
基金资助:
吉林省财政厅科研基金资助课题（2017F002）

A case report of microcephaly, seizures and developmental delay and analysis on its genetic pedigree

MEI Jie, ZHOU Wenli, YAN Jiaxiu, GUO Shijie

Department of Neonatology, First Hospital, Jilin University, Changchun 130021, China

Received:2018-11-02 Published:2019-03-29

摘要/Abstract

摘要： 目的：探讨小头畸形-癫痫-发育迟缓症（MCSZ）的临床特点，分析遗传家系图谱，总结其诊断和治疗方法，提高临床医生对MCSZ的认识。方法：收集1例MCSZ患儿的临床资料，并行头部MRI平扫检查，采集患儿及其父母的血样进行全外显子组基因测序。结果：患儿临床表现为前囟和头围小、难治性癫痫、发育迟缓，4个月时因持续抽搐发作死亡。头部MRI平扫，前脑无裂畸形，白质及小脑发育不良，枕大池增大，扁平颅底。全外显子组基因测序，患儿多核苷酸激酶/磷酸酶（PNKP）基因存在杂合致病突变c.976G>A （p.Glu326Lys）和临床意义未明的杂合突变c.1482C>T （p.Gly494=），其母携带c.976G>A （p.Glu326Lys），其父携带c.1482C>T （p.Gly494=）。结论：患儿明确临床诊断为MCSZ，且为严重致死的MCSZ。患儿PNKP基因存在复合杂合突变，其中杂合突变c.1482C>T （p.Gly494=）可能为新发现的致病突变。

关键词: 小头畸形-癫痫-发育迟缓症, PNKP基因, 全外显子组基因测序, 遗传家系图谱

Abstract: Objective: To investigate the clinical characteristics of microcephaly, seizures and developmental delay (MCSZ), to analyze the genetic pedigree, to summarize its diagnosis and treatment, and to improve the understanding of the clinicians for MCSZ.Methods: The clinical data of a child with MCSZ were collected and brain MRI plain scan was performed. The blood samples of the patient and his parents were collected for whole exome gene sequencing.Results: The clinical manifestations of the patient were small anterior fontanel and head circumference, intractable epilepsy and growth retardation.He died of persistent convulsions at 4 months.Brain MRI plain scan showed holoprosencephaly, dysplasia of white matter and cerebellum, enlargement of cisterna magna and flat skull base.There were novel compound heterozygous mutations of PNKP gene in the patient, with the heterozygous pathogenic mutation of c.976G > A (p.Glu326Lys) and the unknown clinical significant heterozygous mutation of c.1482C > T (p.Gly494=).His mother had a heterozygous pathogenic mutation of c.976G > A (p.Glu326Lys) and his father carried a unknown clinical significant heterozygous mutation of c.1482C > T (p.Gly494=).Conclusion: The patient is clinically diagnosed as MCSZ and is fatal.There are novel compound heterozygous mutations of PNKP gene in the patient, among which the heterozygous mutation c.1482C > T (p.Gly494=) may be a newly discovered pathogenic mutation.

Key words: microcephaly,seizures and developmental delay, PNKP gene, whole exome sequencing, genetic pedigree

中图分类号:

R722.11

梅杰, 周文莉, 闫佳秀, 郭世杰. 小头畸形-癫痫-发育迟缓症1例报告及其遗传家系图谱分析[J]. 吉林大学学报(医学版), 2019, 45(02): 422-425.

MEI Jie, ZHOU Wenli, YAN Jiaxiu, GUO Shijie. A case report of microcephaly, seizures and developmental delay and analysis on its genetic pedigree[J]. Journal of Jilin University(Medicine Edition), 2019, 45(02): 422-425.

参考文献

[1] SHEN J, GILMORE E C, MARSHALL C A, et al. Mutations in PNKP cause microcephaly, seizures and defects in DNA repair[J].Nat Genet, 2010, 42(3):245-249.
[2] NAKASHIMA M, TAKANO K, OSAKA H, et al.Causative novel PNKP mutations and concomitant PCDH15 mutations in a patient with microcephaly with early-onset seizures and developmental delay syndrome and hearing loss[J].J Hum Genet, 2014, 59(8):471-474.
[3] NAIR P, HAMZEH A R, MOHAMED M, et al.Microcephalic primordial dwarfism in an Emirati patient with PNKP mutation[J].Am J Med Genet A, 2016, 170(8):2127-2132.
[4] ENTEZAM M, RAZIPOUR M, TALEBI S, et al.Multi affected pedigree with congenital microcephaly:WES revealed PNKP gene mutation[J].Brain Dev, 2018, DOI:10.1016/j.braindev.2018.08.005.
[5] REYNOLDS J J,WALKER A K, GILMORE E C, et al.Impact of PNKP mutations associated with microcephaly, seizures and developmental delay on enzyme activity and DNA strand break repair[J].Nucleic Acids Res, 2012, 40(14):6608-6619.
[6] HASHMI J A, AL-HARBI K M, RAMZAN K, et al.A novel splice-site mutation in the ASPM gene underlies autosomal recessive primary microcephaly[J].Ann Saudi Med, 2016, 36(6):391-396.
[7] YE Y Z, CHO M T, RETTERER K, et al.De novo POGZ mutations are associated with neurodevelopmental disorders and microcephaly[J].Cold Spring Harb Mol Case Stud, 2015, 1(1):a000455.
[8] FAHEEM M, NASEER M I, RASOOL M, et al.Molecular genetics of human primary microcephaly:an overview[J].BMC Med Genomics, 2015, 8(Suppl 1):S4.
[9] DOOBIN D J, KEMAL S, DANTAS T J, et al.Severe NDE1-mediated microcephaly results from neural progenitor cell cycle arrests at multiple specific stages[J].Nat Commun, 2016, 7:12551.
[10] RUMP P, JAZAYERI O, van DIJK-BOS K K, et al.Whole-exome sequencing is a powerful approach for establishing the etiological diagnosis in patients with intellectual disability and microcephaly[J].BMC Med Genomics, 2016, 9:7.
[11] BASIT S, AL-HARBI K M, ALHIJJI S A, et al.CIT, a gene involved in neurogenic cytokinesis, is mutated in human primary microcephaly[J].Hum Genet, 2016, 135(10):1199-1207.
[12] HANZLIK E, GIGANTE J.Microcephaly[J].Children, 2017, 4(6):E47.
[13] KAYMAKCALAN H, YARMAN Y, GOC N, et al.Novel compound heterozygous mutations in GPT2 linked to microcephaly, and intellectual developmental disability with or without spastic paraplegia[J].Am J Med Genet A, 2018, 176(2):421-425.
[14] WEINFELD M, MANI R S, ABDOU I, et al.Tidying up loose ends:the role of polynucleotide kinase/phosphatase in DNA strand break repair[J].Trends Biochem Sci, 2011, 36(5):262-271.
[15] IYAMA T, WILSON D M 3rd.DNA repair mechanisms in dividing and non-dividing cells[J].DNA Repair (Amst), 2013, 12(8):620-636.
[16] SHIMADA M, DUMITRACHE L C, RUSSELL H R, et al.Polynucleotide kinase-phosphatase enables neurogenesis via multiple DNA repair pathways to maintain genome stability[J].EMBO J, 2015, 34(19):2465-2480.
[17] BRESLIN C, MANI R S, FANTA M, et al.The Rev1 interacting region (RIR) motif in the scaffold protein XRCC1 mediates a low-affinity interaction with polynucleotide kinase/phosphatase (PNKP) during DNA single-strand break repair[J].J Biol Chem, 2017, 292(39):16024-16031.
[18] REYNOLDS J J, STEWART G S.A nervous predisposition to unrepaired DNA double strand breaks[J].DNA Repair (Amst), 2013, 12(8):588-599.
[19] POULTON C, OEGEMA R, HEIJSMAN D, et al.Progressive cerebellar atrophy and polyneuropathy:expanding the spectrum of PNKP mutations[J].Neurogenetics, 2013, 14(1):43-51.
[20] BRAS J, ALONSO I, BARBOT C, et al.Mutations in PNKP cause recessive ataxia with oculomotor apraxia type 4[J].Am J Hum Genet, 2015, 96(3):474-479.

小头畸形-癫痫-发育迟缓症1例报告及其遗传家系图谱分析

A case report of microcephaly, seizures and developmental delay and analysis on its genetic pedigree

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