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A novel high-throughput molecular counting method with single base-pair resolution enables accurate single-gene NIPT.


ABSTRACT: Next-generation DNA sequencing is currently limited by an inability to accurately count the number of input DNA molecules. Molecular counting is particularly needed when accurate quantification is required for diagnostic purposes, such as in single gene non-invasive prenatal testing (sgNIPT) and liquid biopsy. We developed Quantitative Counting Template (QCT) molecular counting to reconstruct the number of input DNA molecules using sequencing data. We then used QCT molecular counting to develop sgNIPTs of sickle cell disease, cystic fibrosis, spinal muscular atrophy, alpha-thalassemia, and beta-thalassemia. The analytical sensitivity and specificity of sgNIPT was >98% and >99%, respectively. Validation of sgNIPTs was further performed with maternal blood samples collected during pregnancy, and sgNIPTs were 100% concordant with newborn follow-up.

SUBMITTER: Tsao DS 

PROVIDER: S-EPMC6779891 | biostudies-literature | 2019 Oct

REPOSITORIES: biostudies-literature

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A novel high-throughput molecular counting method with single base-pair resolution enables accurate single-gene NIPT.

Tsao David S DS   Silas Sukrit S   Landry Brian P BP   Itzep Nelda P NP   Nguyen Amy B AB   Greenberg Samuel S   Kanne Celeste K CK   Sheehan Vivien A VA   Sharma Rani R   Shukla Rahul R   Arora Prem N PN   Atay Oguzhan O  

Scientific reports 20191007 1


Next-generation DNA sequencing is currently limited by an inability to accurately count the number of input DNA molecules. Molecular counting is particularly needed when accurate quantification is required for diagnostic purposes, such as in single gene non-invasive prenatal testing (sgNIPT) and liquid biopsy. We developed Quantitative Counting Template (QCT) molecular counting to reconstruct the number of input DNA molecules using sequencing data. We then used QCT molecular counting to develop  ...[more]

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