Lee W L, Biervert C, Hallmann K, Tay A, Dean J C, Steinlein O K
Department of Pediatrics, National University of Singapore, Singapore.
Neuropediatrics. 2000 Feb;31(1):9-12. doi: 10.1055/s-2000-15290.
Benign familial neonatal convulsions (BFNC) are one of the rare idiopathic epilepsies with autosomal dominant mode of inheritance. Two voltage-gated potassium channels, KCNQ2 on chromosome 20q13.3 and KCNQ3 on 8q24, have been recently identified as the genes responsible for BFNC. Here we describe a large family with BFNC in which we found a previously undescribed mutation in the KCNQ2 gene. A 1187(+2)T/G nucleotide exchange affects the conserved donor splice site motif in intron 9. This mutation can be predicted to give rise to aberrant splicing of the primary transcript. There was a wide range of clinical manifestations in this family. An unusual clinical feature is the occurrence of partial seizures in later life with corresponding focal neurological deficits.
良性家族性新生儿惊厥(BFNC)是一种罕见的常染色体显性遗传模式的特发性癫痫。最近已确定位于20q13.3染色体上的两个电压门控钾通道KCNQ2和位于8q24上的KCNQ3是导致BFNC的基因。在此,我们描述了一个患有BFNC的大家族,在该家族中我们发现了KCNQ2基因中一个以前未描述的突变。1187(+2)T/G核苷酸交换影响内含子9中保守的供体剪接位点基序。可以预测该突变会导致初级转录本的异常剪接。这个家族有广泛的临床表现。一个不寻常的临床特征是在晚年出现部分性癫痫发作并伴有相应的局灶性神经功能缺损。
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