Recepción del artículo: 19 de Agosto, 2004

Aprobación: 24 de Agosto, 2004

Primera edición: 7 de Abril, 2005

Palabras clave

Clasificación en siicsalud
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página www.siicsalud.com/des/des042/05323006.htm

Especialidades
Principal: Genética Humana
Relacionadas: Bioética,  Diagnóstico por Laboratorio,  Medicina Interna,  Pediatría

Enviar correspondencia a:
Hromadnikova, Ilona,

Patrocinio y reconocimiento
Agradecimientos: Este proyecto fue respaldado por la 2da. Facultad de Medicina, Universidad Charles, Praga, Nº VZ11130003.

NON-INVASIVE PRENATAL DIAGNOSIS BASED ON THE AMPLIFICATION OF PATERNALLY-INHERETED ALLELES IN MATERNAL PLASMA

Abstract
We assessed the feasibility of fetal sex, RhD and RhCE genotyping by analysis of DNA extracted from maternal plasma samples by using real-time PCR. We determined fetal sex in 39 pregnancies at risk of X-linked disorders from 10^th to 22^nd weeks of gestation and correlated with the results of chorionic villus sampling and amniocentesis or checked after the delivery. SRY real-time PCR analysis of maternal plasma was in complete concordance with fetal sex in all 39 tested pregnant women bearing 18 males and 21 females. We analysed 45 Rh D negative pregnant women within 11^th and 40^th week of pregnancy and correlated the results with serological analysis of cord blood after the delivery. Non-invasive prenatal fetal RhD exon 7, RhD exon 10, RhCE exon 2 (C allele) and RhCE exon 5 (E allele) genotyping analysis of maternal plasma samples was well performed in 45/45 Rh D negative pregnant women delivering 24 Rh D, 17 Rh C and 7 Rh E positive newborns. We suggest that amplification of free fetal DNA in maternal plasma is a promising approach for a valid and rapid fetal sex, RhD and RhCE status determination. We recommend to perform non-invasive fetal RhD and RhCE genotyping in alloimunised Rh D negative pregnancies to evaluate the risk of haemolytic disease of the newborn and fetal sex determination in pregnancies at risk of X-linked disorders with a follow-up of invasive diagnostic procedures restricted to male fetuses only.

Key words
Fetal DNA, maternal plasma, real-time PCR, haemolytic disease of the newborn, X-linked disorders

Bibliografía del artículo

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