临床儿科杂志
臨床兒科雜誌
림상인과잡지
2014年
4期
384-387
,共4页
李琳迪%蓝丹%杨湖%许田田%李琼艳%高宗燕
李琳迪%藍丹%楊湖%許田田%李瓊豔%高宗燕
리림적%람단%양호%허전전%리경염%고종연
软骨发育不全%软骨发育低下%成纤维细胞生长因子受体3基因%基因诊断
軟骨髮育不全%軟骨髮育低下%成纖維細胞生長因子受體3基因%基因診斷
연골발육불전%연골발육저하%성섬유세포생장인자수체3기인%기인진단
achondroplasia%hypochondroplasia%fibroblast growth factor receptor 3 Gene%Genetic diagnosis
目的:了解临床诊断为软骨发育异常类疾病患儿及其家系成员的成纤维细胞生长因子受体3(FGFR3)基因突变情况。方法应用聚合酶链式反应(PCR)和DNA测序技术分析7例患儿及其家系成员的FGFR3基因突变热点分布区域第10外显子以及第13外显子的序列。结果4例患儿存在FGFR3基因第10外显子c.1138G>A(p.Gly380Arg)杂合突变,确诊为软骨发育不全(ACH),其父母未见突变。1例症状较轻微的患儿及其有同样表型的母亲存在FGFR3基因第13外显子c.1620C>A(p.Asn540Lys)杂合突变,确诊为软骨发育低下(HCH)。2例患儿未发现以上两个位点的突变。结论检测FGFR3基因第10、第13外显子可诊断大部分ACH或HCH病例,但少数患儿尚有必要检测FGFR3基因其他区域及其他相关基因以明确诊断。
目的:瞭解臨床診斷為軟骨髮育異常類疾病患兒及其傢繫成員的成纖維細胞生長因子受體3(FGFR3)基因突變情況。方法應用聚閤酶鏈式反應(PCR)和DNA測序技術分析7例患兒及其傢繫成員的FGFR3基因突變熱點分佈區域第10外顯子以及第13外顯子的序列。結果4例患兒存在FGFR3基因第10外顯子c.1138G>A(p.Gly380Arg)雜閤突變,確診為軟骨髮育不全(ACH),其父母未見突變。1例癥狀較輕微的患兒及其有同樣錶型的母親存在FGFR3基因第13外顯子c.1620C>A(p.Asn540Lys)雜閤突變,確診為軟骨髮育低下(HCH)。2例患兒未髮現以上兩箇位點的突變。結論檢測FGFR3基因第10、第13外顯子可診斷大部分ACH或HCH病例,但少數患兒尚有必要檢測FGFR3基因其他區域及其他相關基因以明確診斷。
목적:료해림상진단위연골발육이상류질병환인급기가계성원적성섬유세포생장인자수체3(FGFR3)기인돌변정황。방법응용취합매련식반응(PCR)화DNA측서기술분석7례환인급기가계성원적FGFR3기인돌변열점분포구역제10외현자이급제13외현자적서렬。결과4례환인존재FGFR3기인제10외현자c.1138G>A(p.Gly380Arg)잡합돌변,학진위연골발육불전(ACH),기부모미견돌변。1례증상교경미적환인급기유동양표형적모친존재FGFR3기인제13외현자c.1620C>A(p.Asn540Lys)잡합돌변,학진위연골발육저하(HCH)。2례환인미발현이상량개위점적돌변。결론검측FGFR3기인제10、제13외현자가진단대부분ACH혹HCH병례,단소수환인상유필요검측FGFR3기인기타구역급기타상관기인이명학진단。
Objective To screen the sequence of fibroblast growth factor receptor 3 (FGFR3) genes in children with dys-chondroplasia and their family members for searching the mutations. Methods The sequence of exon 10 and exon 13 in muta-tion hot spot region of FGFR3 gene in seven families was analyzed using polymerase chain reaction (PCR) and DNA sequenc-ing technology. Results The c.1138G>A missense mutation in exon 10 was found in 4 probands who were diagnosed as achon-droplasia (ACH), while this mutation was absent in their parents. The c.1620C>A missense mutation in exon 13 was found in one girl and her mother who both were diagnosed as hypochondroplasia (HCH) with mild symptoms. Neither mutation men-tioned above was found in the other two probands. Conclusions Through detecting the mutation in exon 10, exon 13 of FGFR3 gene, most patients of ACH or HCH can be finally diagnosed. However, it is necessary to perform the mutation screening on the other zones of FGFR3 gene and on other related genes for a few cases.
