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Detection of fetal subchromosomal abnormalities by sequencing circulating cell-free DNA from maternal plasma.
Chen Zhao
1 ,
John Tynan
1 ,
Mathias Ehrich
2 ,
Gregory Hannum
1 ,
Ron McCullough
1 ,
Juan-Sebastian Saldivar
1 ,
Paul Oeth
1 ,
Dirk van den Boom
3 ,
Cosmin Deciu
4
Apr 2015
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Abstract
The development of sequencing-based noninvasive prenatal testing (NIPT) has been largely focused on whole-chromosome aneuploidies (chromosomes 13, 18, 21, X, and Y). Collectively, they account for only 30% of all live births with a chromosome abnormality. Various structural chromosome changes, such as microdeletion/microduplication (MD) syndromes are more common but more challenging to detect. Recently, several publications have shown results on noninvasive detection of MDs by deep sequencing. These approaches demonstrated the proof of concept but are not economically feasible for large-scale clinical applications.