Young J H, Wang J C, Gau J P, Hu H T
Department of Internal Medicine, Taichung Veterans General Hospital, Taiwan.
Am J Hematol. 1996 Aug;52(4):243-7. doi: 10.1002/(SICI)1096-8652(199608)52:4<243::AID-AJH1>3.0.CO;2-S.
Prenatal diagnosis was carried out on a woman who had previously given birth to a son with a spontaneous mutation of C-->T transition at nt 31133 of the factor IX (F.IX) gene. The diagnosis was performed on chorionic villi sampling by the method of amplification-created restriction site (ACRS). It revealed a female fetus with a normal F.IX gene, as confirmed by DNA sequencing after delivery. Meanwhile, a survey using the ACRS method to evaluate the inheritance of 63 individuals from 8 hemophilia B families was done. A different single-point mutation in each family was proved by DNA sequencing. One individual had a mutation with a naturally-created restriction site. In each of the remaining patients, we were able to show an enzyme-cutting site in their DNA amplification product for ACRS with the designed mutagenesis primers. All patients and carriers could be diagnosed accurately by comparing ACRS results with clinical and laboratory findings. There were new novel mutations among the patients.
对一名曾生育过一名患有因子IX(F.IX)基因第31133位核苷酸C→T自发突变儿子的女性进行了产前诊断。通过扩增产生限制位点(ACRS)方法对绒毛取样进行诊断。结果显示为一名具有正常F.IX基因的女胎,产后DNA测序证实了这一点。同时,采用ACRS方法对8个乙型血友病家庭的63名个体进行了遗传评估调查。DNA测序证实每个家庭存在不同的单点突变。一名个体具有天然产生的限制位点突变。在其余每位患者中,我们能够通过设计的诱变引物在其DNA扩增产物中显示出ACRS的酶切位点。通过将ACRS结果与临床和实验室检查结果进行比较,所有患者和携带者均能得到准确诊断。患者中存在新的突变。
