Your search keyword '"Brechard, Marie"' showing total 2 results

1. A Broad Test Based on Fluorescent-Multiplex PCR for Noninvasive Prenatal Diagnosis of Cystic Fibrosis.

Author

Guissart C, Tran Mau Them F, Debant V, Viart V, Dubucs C, Pritchard V, Rouzier C, Boureau-Wirth A, Haquet E, Puechberty J, Bieth E, Khau Van Kien P, Brechard MP, Raynal C, Girardet A, Claustres M, Koenig M, and Vincent MC

Subjects

Cystic Fibrosis Transmembrane Conductance Regulator chemistry, Haplotypes, Humans, Multiplex Polymerase Chain Reaction methods, Cell-Free Nucleic Acids chemistry, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Prenatal Diagnosis methods

Abstract

Background: Analysis of cell-free fetal DNA in maternal plasma is very promising for early diagnosis of monogenic diseases. However, it has been limited by the need to set up patient- or disease-specific custom-made approaches. Here we propose a universal test based on fluorescent multiplex PCR and size fragment analysis for an indirect diagnosis of cystic fibrosis (CF)., Methods: The test, based on haplotyping, includes nine intra- and extragenic short tandem repeats of the CFTR locus, the coamplification of p.Phe508del (the most frequent mutation in CF patients worldwide), and a specific SRY sequence. The assay is able to determine the inherited paternal allele., Results: Our simple approach was successfully applied to 30 couples and provided clear results from the maternal plasma. The mean rate of informative markers was sufficient to propose it for use in indirect diagnosis., Conclusions: This noninvasive prenatal diagnosis test, focused on indirect diagnosis of CF, offers many advantages over current methods: it is simple, rapid, and cost-effective. It allows for the testing of a large number of couples with high risk of CF, whatever the familial mutation of the CFTR gene. It provides an alternative method to reduce the number of invasive tests., (© 2018 S. Karger AG, Basel.)

Published

2019

2. Strategy for Use of Genome-Wide Non-Invasive Prenatal Testing for Rare Autosomal Aneuploidies and Unbalanced Structural Chromosomal Anomalies.

Author

Kleinfinger, Pascale, Lohmann, Laurence, Luscan, Armelle, Trost, Detlef, Bidat, Laurent, Debarge, Véronique, Castaigne, Vanina, Senat, Marie-Victoire, Brechard, Marie-Pierre, Guilbaud, Lucie, Le Guyader, Gwenaël, Satre, Véronique, Laurichesse Delmas, Hélène, Lallaoui, Hakima, Manca-Pellissier, Marie-Christine, Boughalem, Aicha, Valduga, Mylene, Hodeib, Farah, Benachi, Alexandra, and Costa, Jean Marc

Subjects

PRENATAL diagnosis, TRISOMY, FETAL development, PREGNANT women

Abstract

Atypical fetal chromosomal anomalies are more frequent than previously recognized and can affect fetal development. We propose a screening strategy for a genome-wide non-invasive prenatal test (NIPT) to detect these atypical chromosomal anomalies (ACAs). Two sample cohorts were tested. Assay performances were determined using Cohort A, which consisted of 192 biobanked plasma samples—42 with ACAs, and 150 without. The rate of additional invasive diagnostic procedures was determined using Cohort B, which consisted of 3097 pregnant women referred for routine NIPT. Of the 192 samples in Cohort A, there were four initial test failures and six discordant calls; overall sensitivity was 88.1% (37/42; CI 75.00–94.81) and specificity was 99.3% (145/146; CI 96.22–99.88). In Cohort B, there were 90 first-pass failures (2.9%). The rate of positive results indicating an anomaly was 1.2% (36/3007) and 0.57% (17/3007) when limited to significant unbalanced chromosomal anomalies and trisomies 8, 9, 12, 14, 15, 16, and 22. These results show that genome-wide NIPT can screen for ACAs with an acceptable sensitivity and a small increase in invasive testing, particularly for women with increased risk following maternal serum screening and by limiting screening to structural anomalies and the most clinically meaningful trisomies. [ABSTRACT FROM AUTHOR]

Published

2020