Loss-of-function variants in DNM1 cause a specific form of developmental and epileptic encephalopathy only in biallelic state

被引：12

作者：

Yigit, Gokhan ^{[1
]}

Sheffer, Ruth ^{[2
]}

Daana, Muhannad ^{[3
]}

Li, Yun ^{[1
]}

Kaygusuz, Emrah ^{[1
,4
]}

Mor-Shakad, Hagar ^{[2
]}

Altmueller, Janine ^{[5
,6
]}

Nuernberg, Peter ^{[5
,6
]}

Douiev, Liza ^{[2
]}

Kaulfuss, Silke ^{[1
]}

Burfeind, Peter ^{[1
]}

Wollnik, Bernd ^{[1
,7
]}

Brockmann, Knut ^{[8
]}

机构：

[1] Univ Med Ctr Gottingen, Inst Human Genet, Gottingen, Germany

[2] Hadassah Univ Hosp, Dept Human Genet, Jerusalem, Israel

[3] Inst Child Dev, Clalit Hlth Serv, Tel Aviv, Israel

[4] Bilecik Seyh Edebali Univ, Mol Biol & Genet, Bilecik, Turkey

[5] Univ Cologne, Fac Med, Cologne Ctr Genom CCG, Cologne, Germany

[6] Univ Hosp Cologne, Cologne, Germany

[7] Univ Gottingen, Cluster Excellence Multiscale Bioimaging Mol Mach, Gottingen, Germany

[8] Univ Med Ctr Gottingen, Interdisciplinary Pediat Ctr Children Dev Disabil, Gottingen, Germany

来源：

JOURNAL OF MEDICAL GENETICS | 2022年 / 59卷 / 06期

关键词：

epilepsy; genetics; nervous System Diseases; Pediatrics; DYNAMIN; MUTATIONS; PHENOTYPE;

D O I：

10.1136/jmedgenet-2021-107769

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

Background Developmental and epileptic encephalopathies (DEEs) represent a group of severe neurological disorders characterised by an onset of refractory seizures during infancy or early childhood accompanied by psychomotor developmental delay or regression. DEEs are genetically heterogeneous with, to date, more than 80 different genetic subtypes including DEE31 caused by heterozygous missense variants in DNM1. Methods We performed a detailed clinical characterisation of two unrelated patients with DEE and used whole-exome sequencing to identify causative variants in these individuals. The identified variants were tested for cosegregation in the respective families. Results We excluded pathogenic variants in known, DEE-associated genes. We identified homozygous nonsense variants, c.97C>T; p.(Gln33*) in family 1 and c.850C>T; p.(Gln284*) in family 2, in the DNM1 gene, indicating that biallelic, loss-of-function pathogenic variants in DNM1 cause DEE. Conclusion Our finding that homozygous, loss-of-function variants in DNM1 cause DEE expands the spectrum of pathogenic variants in DNM1. All parents who were heterozygous carriers of the identified loss-of-function variants were healthy and did not show any clinical symptoms, indicating that the type of mutation in DNM1 determines the pattern of inheritance.

引用

页码：549 / 553

页数：5

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