Kanno Junko, Kure Shigeo, Narisawa Ayumi, Kamada Fumiaki, Takayanagi Masaru, Yamamoto Katsuya, Hoshino Hisao, Goto Tomohide, Takahashi Takao, Haginoya Kazuhiro, Tsuchiya Shigeru, Baumeister Fritz A M, Hasegawa Yuki, Aoki Yoko, Yamaguchi Seiji, Matsubara Yoichi
Department of Medical Genetics, Tohoku University School of Medicine, 1-1 Seiryomachi, Aobaku, Sendai 980-8574, Japan.
Mol Genet Metab. 2007 Aug;91(4):384-9. doi: 10.1016/j.ymgme.2007.02.010. Epub 2007 Apr 11.
Pyridoxine dependent seizure (PDS) is a disorder of neonates or infants with autosomal recessive inheritance characterized by seizures, which responds to pharmacological dose of pyridoxine. Recently, mutations have been identified in the ALDH7A1 gene in Caucasian families with PDS. To elucidate further the genetic background of PDS, we screened for ALDH7A1 mutations in five PDS families (patients 1-5) that included four Orientals. Diagnosis as having PDS was confirmed by pyridoxine-withdrawal test. Exon sequencing analysis of patients 1-4 revealed eight ALDH7A1 mutations in compound heterozygous forms: five missense mutations, one nonsense mutation, one point mutation at the splicing donor site in intron 1, and a 1937-bp genomic deletion. The deletion included the entire exon 17, which was flanked by two Alu elements in introns 16 and 17. None of the mutations was found in 100 control chromosomes. In patient 5, no mutation was found by the exon sequencing analysis. Furthermore, expression level or nucleotide sequences of ALDH7A1 mRNA in lymphoblasts were normal. Plasma pipecolic acid concentration was not elevated in patient 5. These observations suggest that ALDH7A1 mutation is unlikely to be responsible for patient 5. Abnormal metabolism of GABA/glutamate in brain has long been suggested as the underlying pathophysiology of PDS. CSF glutamate concentration was elevated during the off-pyridoxine period in patient 3, but not in patient 2 or 5. These results suggest allelic and non-allelic heterogeneities of PDS, and that the CSF glutamate elevation does not directly correlate with the presence of ALDH7A1 mutations.
维生素B6依赖型癫痫(PDS)是一种具有常染色体隐性遗传特征的新生儿或婴儿疾病,其特点为癫痫发作,对药理剂量的维生素B6有反应。最近,在患有PDS的白种人家庭中已鉴定出ALDH7A1基因的突变。为了进一步阐明PDS的遗传背景,我们在包括四名东方人的五个PDS家庭(患者1 - 5)中筛查了ALDH7A1突变。通过维生素B6撤药试验确诊为患有PDS。对患者1 - 4的外显子测序分析揭示了八种复合杂合形式的ALDH7A1突变:五种错义突变、一种无义突变、一种位于内含子1剪接供体位点的点突变以及一个1937 bp的基因组缺失。该缺失包括整个外显子17,其两侧分别为内含子16和17中的两个Alu元件。在100条对照染色体中未发现任何突变。在患者5中,外显子测序分析未发现突变。此外,患者5的淋巴母细胞中ALDH7A1 mRNA的表达水平或核苷酸序列正常。患者5的血浆哌可酸浓度未升高。这些观察结果表明,ALDH7A1突变不太可能是患者5发病的原因。长期以来,大脑中γ-氨基丁酸/谷氨酸的代谢异常一直被认为是PDS的潜在病理生理学机制。患者3在停用维生素B6期间脑脊液谷氨酸浓度升高,但患者2或5未出现这种情况。这些结果表明PDS存在等位基因和非等位基因异质性,并且脑脊液谷氨酸升高与ALDH7A1突变的存在没有直接相关性。
