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从母体血液中通过流式细胞术分选的胎儿细胞中的胎儿RhD基因分型。

Fetal RhD genotyping in fetal cells flow sorted from maternal blood.

作者信息

Geifman-Holtzman O, Bernstein I M, Berry S M, Holtzman E J, Vadnais T J, DeMaria M A, Bianchi D W

机构信息

Division of Maternal-Fetal Medicine, Medical Center Hospital of Vermont, Burlington, USA.

出版信息

Am J Obstet Gynecol. 1996 Mar;174(3):818-22. doi: 10.1016/s0002-9378(96)70306-x.

Abstract

OBJECTIVE

The aim of this study was to determine the accuracy of noninvasive fetal RhD genotyping by fetal cell isolation from maternal blood.

STUDY DESIGN

Candidate fetal cells from 18 pregnant women (one twin gestation) were flow-sorted. Polymerase chain reaction amplification of a 261 bp fragment of the RhD gene was performed on sorted fetal cells. The presence of amplified product was considered predictive of the Rhd-positive genotype in the fetus.

RESULTS

Sixteen of the 19 fetal RhD genotypes were correctly predicted in fetal cells isolated from maternal blood (10 were Rh positive, 6 were Rh negative). In 3 cases no amplification products were detected in RhD-positive fetuses. The association between presence of the fragment and RhD-positive genotype was significant (p=0.003, Fisher's exact test).

CONCLUSIONS

Noninvasive prenatal diagnosis of the fetal RhD genotype is feasible. Absence of amplification products in the reaction requires confirmation that fetal material is present. Improvements in fetal cell purity and yield should increase diagnostic accuracy, although the current protocol has a positive predictive value of 100% and a negative predictive value of 67%.

摘要

目的

本研究旨在通过从母血中分离胎儿细胞来确定无创胎儿RhD基因分型的准确性。

研究设计

对18名孕妇(其中1例为双胎妊娠)的候选胎儿细胞进行流式分选。对分选后的胎儿细胞进行RhD基因261bp片段的聚合酶链反应扩增。扩增产物的存在被认为可预测胎儿的Rhd阳性基因型。

结果

从母血中分离出的胎儿细胞中,19例胎儿RhD基因型中有16例被正确预测(10例为Rh阳性,6例为Rh阴性)。在3例RhD阳性胎儿中未检测到扩增产物。片段的存在与RhD阳性基因型之间的关联具有显著性(p=0.003,Fisher精确检验)。

结论

胎儿RhD基因型的无创产前诊断是可行的。反应中无扩增产物需要确认存在胎儿物质。尽管当前方案的阳性预测值为100%,阴性预测值为67%,但提高胎儿细胞的纯度和产量应能提高诊断准确性。

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