Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.

Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.

The β-thalassemias are genetic disorder caused by more than 200 mutations in the β-globin gene, resulting in a total (β0) or partial (β+) deficit of the globin chain synthesis. The most frequent Mediterranean mutations for β-thalassemia are: β039, β+IVSI-110, β+IVSI-6 and β0IVSI-1. Several molecular...

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Main Authors: Giulia Breveglieri, Anna Travan, Elisabetta D'Aversa, Lucia Carmela Cosenza, Patrizia Pellegatti, Giovanni Guerra, Roberto Gambari, Monica Borgatti
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2017-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC5325530?pdf=render
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spelling doaj-7f982c0b6152487e9033ade00fe891512020-11-25T01:48:05ZengPublic Library of Science (PLoS)PLoS ONE1932-62032017-01-01122e017275610.1371/journal.pone.0172756Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.Giulia BreveglieriAnna TravanElisabetta D'AversaLucia Carmela CosenzaPatrizia PellegattiGiovanni GuerraRoberto GambariMonica BorgattiThe β-thalassemias are genetic disorder caused by more than 200 mutations in the β-globin gene, resulting in a total (β0) or partial (β+) deficit of the globin chain synthesis. The most frequent Mediterranean mutations for β-thalassemia are: β039, β+IVSI-110, β+IVSI-6 and β0IVSI-1. Several molecular techniques for the detection of point mutations have been developed based on the amplification of the DNA target by polymerase chain reaction (PCR), but they could be labor-intensive and technically demanding. On the contrary, TaqMan® genotyping assays are a simple, sensitive and versatile method suitable for the single nucleotide polymorphism (SNP) genotyping affecting the human β-globin gene. Four TaqMan® genotyping assays for the most common β-thalassemia mutations present in the Mediterranean area were designed and validated for the genotype characterization of genomic DNA extracted from 94 subjects comprising 25 healthy donors, 33 healthy carriers and 36 β-thalassemia patients. In addition, 15 specimens at late gestation (21-39 gestational weeks) and 11 at early gestation (5-18 gestational weeks) were collected from pregnant women, and circulating cell-free fetal DNAs were extracted and analyzed with these four genotyping assays. We developed four simple, inexpensive and versatile genotyping assays for the postnatal and prenatal identification of the thalassemia mutations β039, β+IVSI-110, β+IVSI-6, β0IVSI-1. These genotyping assays are able to detect paternally inherited point mutations in the fetus and could be efficiently employed for non-invasive prenatal diagnosis of β-globin gene mutations, starting from the 9th gestational week.http://europepmc.org/articles/PMC5325530?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Giulia Breveglieri
Anna Travan
Elisabetta D'Aversa
Lucia Carmela Cosenza
Patrizia Pellegatti
Giovanni Guerra
Roberto Gambari
Monica Borgatti
spellingShingle Giulia Breveglieri
Anna Travan
Elisabetta D'Aversa
Lucia Carmela Cosenza
Patrizia Pellegatti
Giovanni Guerra
Roberto Gambari
Monica Borgatti
Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.
PLoS ONE
author_facet Giulia Breveglieri
Anna Travan
Elisabetta D'Aversa
Lucia Carmela Cosenza
Patrizia Pellegatti
Giovanni Guerra
Roberto Gambari
Monica Borgatti
author_sort Giulia Breveglieri
title Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.
title_short Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.
title_full Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.
title_fullStr Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.
title_full_unstemmed Postnatal and non-invasive prenatal detection of β-thalassemia mutations based on Taqman genotyping assays.
title_sort postnatal and non-invasive prenatal detection of β-thalassemia mutations based on taqman genotyping assays.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2017-01-01
description The β-thalassemias are genetic disorder caused by more than 200 mutations in the β-globin gene, resulting in a total (β0) or partial (β+) deficit of the globin chain synthesis. The most frequent Mediterranean mutations for β-thalassemia are: β039, β+IVSI-110, β+IVSI-6 and β0IVSI-1. Several molecular techniques for the detection of point mutations have been developed based on the amplification of the DNA target by polymerase chain reaction (PCR), but they could be labor-intensive and technically demanding. On the contrary, TaqMan® genotyping assays are a simple, sensitive and versatile method suitable for the single nucleotide polymorphism (SNP) genotyping affecting the human β-globin gene. Four TaqMan® genotyping assays for the most common β-thalassemia mutations present in the Mediterranean area were designed and validated for the genotype characterization of genomic DNA extracted from 94 subjects comprising 25 healthy donors, 33 healthy carriers and 36 β-thalassemia patients. In addition, 15 specimens at late gestation (21-39 gestational weeks) and 11 at early gestation (5-18 gestational weeks) were collected from pregnant women, and circulating cell-free fetal DNAs were extracted and analyzed with these four genotyping assays. We developed four simple, inexpensive and versatile genotyping assays for the postnatal and prenatal identification of the thalassemia mutations β039, β+IVSI-110, β+IVSI-6, β0IVSI-1. These genotyping assays are able to detect paternally inherited point mutations in the fetus and could be efficiently employed for non-invasive prenatal diagnosis of β-globin gene mutations, starting from the 9th gestational week.
url http://europepmc.org/articles/PMC5325530?pdf=render
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