SLC32A1 gene mutation in hereditary epilepsy with febrile convulsion addition: A case report and literature review

doi:10.3969/j.issn.1004-583X.2023.05.012

Abstract

Abstract:

Objective To investigate the influence of missense mutations in the SLC32A1 gene on hereditary epilepsy with febrile seizures plus (GEFS+). Methods Clinical data of a child with GEFS+ caused by the SLC32A1 gene mutation were retrospectively analyzed, and relevant literatures were reviewed. Results A boy with 1 and a half year old presented with recurrent febrile seizures for three times and febrile seizures twice. Two months ago, the child experienced two episodes of febrile seizures due to upper respiratory tract infection, with a temperature of 38.3 ℃. Tonic-clonic convulsions occurred and lasted 1-3 minutes, which were resolved spontaneously. He then experienced another episode of febrile seizure. One week ago, the child experienced two episodes of febrile seizures without an obvious cause, manifesting as tonic-clonic seizures. No abnormalities were found in electroencephalography and cranial magnetic resonance imaging. His father had one episode of febrile convulsion at the age of 1 year, and the remaining family members denied history of convulsions. The child was the first newborn of his mother and he did not experience hypoxia and asphyxia at delivery, with normal growth and development after birth. Full-exon sequencing showed one heterozygous variant with unknown significance in the SLC32A1 gene: c.1184C>T (p.Pro395Leu), indicating a missense variant. Conclusion SLC32A1 gene mutation is associated with GEFS+, and the phenotypic consistency of the tested subjects is relatively high. Literature review to determine its relevance to GEFS+ contributes to discover new gene profiles of GEFS+ and facilitates genetic counseling.

Key words: shereditary epilepsy with febrile convulsion addition, SLC32A1 gene, convulsions

CLC Number:

R742.1

Zhao Shuzhen, Wang Sanping, Zhao Xiaoyun. SLC32A1 gene mutation in hereditary epilepsy with febrile convulsion addition: A case report and literature review[J]. Clinical Focus, 2023, 38(5): 451-454.

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URL: https://huicui.hebmu.edu.cn/EN/10.3969/j.issn.1004-583X.2023.05.012

https://huicui.hebmu.edu.cn/EN/Y2023/V38/I5/451

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References 15

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基因	染色体位置 (hg19)	参考转录本外显子	核苷酸改变氨基酸改变	功能改变	杂合性	变异来源	人群频率	致病性定级
SLC32A1	Chr20:37356888	NM_080552.3	C.1184C>T	错义突变	杂合	父亲	未收录	意义未明
		exon2	p.Pro395Leu
相关疾病		GEFS+?

基因	染色体位置 (hg19)	参考转录本外显子	核苷酸改变氨基酸改变	功能改变	杂合性	变异来源	人群频率	致病性定级
SLC32A1	Chr20:37356888	NM_080552.3	C.1184C>T	错义突变	杂合	父亲	未收录	意义未明
		exon2	p.Pro395Leu
相关疾病		GEFS+?

家系	突变位点	临床表型
1	c.1403T>C; p.(Leu468Pro)	GEFS+
2	c.1333C>T; p.(Leu445Phe)	GEFS+
3	c.127G>T; p.(Gly43Cys)	GEFS+
4	c.989T>C; p.(Met330Thr)	热性惊厥/全面特发性癫痫
5	c.1391C>G; p.(Thr464Arg)	GEFS+
6	c.788T>C; p.(Val263Ala)	热性惊厥/局灶性癫痫发作
7	c.1382G>A; p.(Gly461Asp)	GEFS+
8	c.1393G>A; p.(Gly465Ser)	GEFS+

家系	突变位点	临床表型
1	c.1403T>C; p.(Leu468Pro)	GEFS+
2	c.1333C>T; p.(Leu445Phe)	GEFS+
3	c.127G>T; p.(Gly43Cys)	GEFS+
4	c.989T>C; p.(Met330Thr)	热性惊厥/全面特发性癫痫
5	c.1391C>G; p.(Thr464Arg)	GEFS+
6	c.788T>C; p.(Val263Ala)	热性惊厥/局灶性癫痫发作
7	c.1382G>A; p.(Gly461Asp)	GEFS+
8	c.1393G>A; p.(Gly465Ser)	GEFS+