儿童进行性脊肌萎缩症的分子诊断(附10例报告)  

作　　者：曾健[1] 柯龙凤[1] 涂向东[1] 黄梁浒[1] 李惠忠[2] 郑德柱[1] 杨渤生[3] 兰风华[1] 

机构地区：[1]南京军区福州总医院遗传病分子诊断中心,福州350025 [2]南京军区福州总医院超声科,福州350025 [3]南京军区福州总医院神经内科,福州350025

出　　处：《解放军医学杂志》2007年第7期729-731,共3页Medical Journal of Chinese People's Liberation Army

基　　金：南京军区医药卫生科研基金资助项目(编号06MA136)

摘　　要：目的对10例儿童进行性脊肌萎缩症(SMA)患者进行分子诊断。方法提取10例SMA患者和其19例家系成员(患者的父母)以及20例健康正常人对照的基因组DNA。常规PCR扩增SMN基因第7外显子(E7),PCR产物经DraI酶切后,行琼脂糖凝胶电泳。同时行特异性PCR扩增SMN1和SMN2的E7。结果常规PCR中,所有10例SMA患者的SMN1PCR产物(189bp)全部被DraI切割,所有39例对照组成员(包括19例家系成员和20例健康正常人对照)的SMN1PCR产物仅有部分可被DraI切割。在位点特异性PCR中,所有10例SMA患者只有SMN2的E7扩增,所有39例对照组成员既有SMN1、也有SMN2的E7扩增产物。结论所有10例SMA患者可见SMN1纯合性缺失。所有39例对照组成员未见SMN1纯合性缺失。本研究采用PCR-RFLP和位点特异性PCR相结合,相互佐证,形成一套特有的分子诊断方法,确保了诊断的准确性。Objective To make molecular diagnosis for puerile spinal muscular atrophy （SMA）. Methods Genomic DNA was extracted directly from the blood of both the case group （10 children with SMA） and the control group （including 19 parents of SMA patients and 20 healthy individuals）. Two methods, polymerase chain reaction-restriction fragment length polymorphism （PCR-RFLP） and allele-specific PCR, were used to analyze exon 7 of SMN gene from genomic DNA, and consequent electrophoresis of PCR products on agarose gel was performed. Results Genotyping results obtained by both methods were in complete agreement for all of the samples analyzed. In conventional PCR-RFLP, part of the PCR products （189bp） from genomic DNA of all 39 members in the control group remained intact after digestion with DraⅠ, while the PCR products from genomic DNA of all 10 SMA children in the case group was completely digested by DraⅠ. In allele-specific PCR, exon 7 of both SMN1 and SMN2 could be seen when genomic DNA of all 39 members in the control group was used, while only SMN2＇s exon 7 could be seen when genomic DNA of all 10 SMA children in the case group was used. Conclusion Homozygous deletion of SMN1 was present in all 10 SMA children in the case group, while homozygous deletion of SMN1 was not detected in all 39 members in the control group. The combination of PCR-RFLP and allele-specific PCR, both their results can be references for each other, offers efficient and accurate methodology for molecular diagnosis of SMA.

关 键 词：肌萎缩 脊髓性 运动神经元 基因 分子诊断技术 

分 类 号：R746.4[医药卫生—神经病学与精神病学]