中华皮肤科杂志
中華皮膚科雜誌
중화피부과잡지
Chinese Journal of Dermatology
2012年
10期
704-707
,共4页
周城%温广东%金彦%于聪%臧东杰%孙青苗%张建中
週城%溫廣東%金彥%于聰%臧東傑%孫青苗%張建中
주성%온엄동%금언%우총%장동걸%손청묘%장건중
表皮松解性角化过度型鱼鳞病%角蛋白10%角蛋白1%DNA突变分析
錶皮鬆解性角化過度型魚鱗病%角蛋白10%角蛋白1%DNA突變分析
표피송해성각화과도형어린병%각단백10%각단백1%DNA돌변분석
Epidermolytic hyperkeratosis%Keratin-10%Keratin-1%DNA mutational analysis
目的 探讨两个表皮松解性角化过度型鱼鳞病(EHK)家系的基因突变情况.方法 收集两个EHK家系的临床资料,提取外周血DNA,通过PCR扩增角蛋白基因KRT1和KRT10编码区的全部外显子及其侧翼序列并测序,以表型正常家系成员及50例健康人作为对照.结果 发现两个家系中患者均存在KRT10基因突变,分别为KRT10的剪接位点突变c.1030-2A>G和错义突变c.467G>A,在家系中健康人及健康对照者未发现上述突变.结论 剪接位点突变c.1030-2A>G和错义突变c.467G>A,可能分别是导致这两个家系临床表型的原因.
目的 探討兩箇錶皮鬆解性角化過度型魚鱗病(EHK)傢繫的基因突變情況.方法 收集兩箇EHK傢繫的臨床資料,提取外週血DNA,通過PCR擴增角蛋白基因KRT1和KRT10編碼區的全部外顯子及其側翼序列併測序,以錶型正常傢繫成員及50例健康人作為對照.結果 髮現兩箇傢繫中患者均存在KRT10基因突變,分彆為KRT10的剪接位點突變c.1030-2A>G和錯義突變c.467G>A,在傢繫中健康人及健康對照者未髮現上述突變.結論 剪接位點突變c.1030-2A>G和錯義突變c.467G>A,可能分彆是導緻這兩箇傢繫臨床錶型的原因.
목적 탐토량개표피송해성각화과도형어린병(EHK)가계적기인돌변정황.방법 수집량개EHK가계적림상자료,제취외주혈DNA,통과PCR확증각단백기인KRT1화KRT10편마구적전부외현자급기측익서렬병측서,이표형정상가계성원급50례건강인작위대조.결과 발현량개가계중환자균존재KRT10기인돌변,분별위KRT10적전접위점돌변c.1030-2A>G화착의돌변c.467G>A,재가계중건강인급건강대조자미발현상술돌변.결론 전접위점돌변c.1030-2A>G화착의돌변c.467G>A,가능분별시도치저량개가계림상표형적원인.
Objective To identify gene mutations in two families with epidermolytic hyperkeratosis (EHK).Methods Clinical data were collected from two families with EHK.Peripheral blood was isolated from the probands and unaffected family members in the families as well as from 50 healthy controls.PCR was performed to amplify the encoding exons and flanking intron regions of KRT1 and KRT10 genes followed by direct DNA sequencing.Results Two mutations in the KRT10 gene,including a heterozygous acceptor splice site mutation in intron 4 (c.1030-2 A>G) and a heterozygous missense mutation c.467 G>A,were identified in the probands of both families,but absent in the unaffected family members or healthy controls.Conclusion The splice site mutation c.1030-2 A>G and missense mutation c.467 G>A might be responsible for the phenotype of EHK in the two families.
