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  Česky / Czech version Trans. Hemat. dnes, 10, 2004, No. 1, p. 13–18.
 
Non-invasive foetal RHD, RHC and RHE genotyping from maternal plasma in RhD negative pregnancies 
Hromadníková I.1, Benešová B.3, Vechetová L.1, Veselá K.1, Doucha J.2, VlkR. 

12. dětská klinika, 2Gynekologicko-porodnická klinika,3Krevní banka 2. Lékařská fakulta, Karlova Univerzita a Fakultní nemocnice Motol, Praha
 


Summary:

       In this prospective study,we assessed the feasibility of foetalRHD,RHCandRHEgenotyping by analysis of DNA extracted from maternal plasma samples collected from RhD negative pregnant women using RQ-PCR and primers and probes targeted toward RHD and RHCE genes.We analysed 29 RhD negative pregnant women within 14th and 40th week of pregnancy and correlated the results with serological analysis of cord blood after the delivery. Non-invasive prenatal foetal RHD exon 7 and exon 10 genotyping analysis of maternal plasma samples was in complete concordance with the analysis of cord blood in 29 out of 29 RhD negative pregnant women delivering 13 RhD positive and 16 RhD negative newborns. Non-invasive prenatal foetal RHC exon 2 genotyping was well performed in 25 out of 25 Rhc homozygote pregnant women delivering 8 RhC positive and 17 RhC negative newborns. Similarly non-invasive prenatal foetal RHE genotyping was well done in 29 out of 29 Rhe homozygote pregnant women delivering 5 RhE positive and 24 RhE negative newborns. Foetal RHC and RHE genotyping in RhD negative pregnancies is very valuable, since in case of identification of RhD negative fetus simultaneous amplification of another paternally inherited allele (RhC or RhE positivity) proves the presence of foetal DNA in maternal circulation. We recommend to perform simultaneous foetal RHD, RHC and RHE genotyping in alloimunised RhD negative pregnancies with certain phenotypes (ccee, ccEe, Ccee).

        Key words: foetal DNA, haemolytic disease of newborn, quantitative real time PCR, maternal plasma, RHD gene, RHCE gene
       

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