Non-invasive prenatal diagnosis of beta-thalassemia and sickle-cell disease using pyrophosphorolysis-activated polymerization and melting curve analysis

ABSTRACT Objective The aim of this study was to develop a pyrophosphorolysis‐activated polymerization (PAP) assay for non‐invasive prenatal diagnosis (NIPD) of β‐thalassemia major and sickle‐cell disease (SCD). PAP is able to detect mutations in free fetal DNA in a highly contaminating environment o...

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Published in:Prenatal diagnosis 2012-06, Vol.32 (6), p.578-587
Main Authors: Phylipsen, Marion, Yamsri, Supawadee, Treffers, Emmely E., Jansen, Diahann T. S. L., Kanhai, Warsha A., Boon, Elles M. J., Giordano, Piero C., Fucharoen, Supan, Bakker, Egbert, Harteveld, Cornelis L.
Format: Article
Language:English
Subjects:
Alleles
Anemia, Sickle Cell - diagnosis
beta-Globins - genetics
beta-Thalassemia - diagnosis
DNA - blood
Fathers
Female
Genetic Carrier Screening
Genetic Linkage
Genotyping Techniques
Humans
Leukocytes - chemistry
Male
Mutation
Polymerase Chain Reaction
Polymerization
Polymorphism, Single Nucleotide - genetics
Pregnancy
Prenatal Diagnosis - methods
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Summary:ABSTRACT Objective The aim of this study was to develop a pyrophosphorolysis‐activated polymerization (PAP) assay for non‐invasive prenatal diagnosis (NIPD) of β‐thalassemia major and sickle‐cell disease (SCD). PAP is able to detect mutations in free fetal DNA in a highly contaminating environment of maternal plasma DNA. Methods Pyrophosphorolysis‐activated polymerization primers were designed for 12 informative SNPs, genotyped by melting curve analysis (MCA) in both parents. The PAP assay was tested in a series of 13 plasma DNA samples collected from pregnant women. A retrospective NIPD was performed in a couple at risk for SCD. Results All PAP reactions were optimized and able to detect 97% wildtype gDNA. In all 13 cases, the paternal allele was detected by PAP in maternal plasma at 10 to 18 weeks of gestation. For the couple at risk, PAP showed presence of the normal paternal SNP allele in maternal plasma, which was confirmed by results of the chorionic villus sampling analysis. Conclusions In contrast to other methods used for NIPD, the combined PAP and MCA analysis detecting the normal paternal allele is also applicable for couples at risk carrying the same mutation, provided that a previously born child is available for testing to determine the linkage to the paternal SNPs. © 2012 John Wiley & Sons, Ltd.
ISSN:0197-3851
1097-0223
DOI:10.1002/pd.3864