4.7 Article

The Performance of Whole Genome Amplification Methods and Next-Generation Sequencing for Pre-Implantation Genetic Diagnosis of Chromosomal Abnormalities

Journal

JOURNAL OF GENETICS AND GENOMICS
Volume 42, Issue 4, Pages 151-159

Publisher

SCIENCE PRESS
DOI: 10.1016/j.jgg.2015.03.001

Keywords

Single cells; Whole genome amplification; Next-generation sequencing; Copy number variation; Pre-implantation genetic diagnosis

Funding

  1. Key Program of the Twelfth Five-year plan of People's liberation Army [BWS11J058]
  2. National High Technology Research and Development Program [SS2015AA020402]

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Reliable and accurate pre-implantation genetic diagnosis (PGD) of patient's embryos by next-generation sequencing (NGS) is dependent on efficient whole genome amplification (WGA) of a representative biopsy sample. However, the performance of the current state of the art WGA methods has not been evaluated for sequencing. Using low template DNA (15 pg) and single cells, we showed that the two PCR-based WGA systems SurePlex and MALBAC are superior to the REPLI-g WGA multiple displacement amplification (MDA) system in terms of consistent and reproducible genome coverage and sequence bias across the 24 chromosomes, allowing better normalization of test to reference sequencing data. When copy number variation sequencing (CNV-Seq) was applied to single cell WGA products derived by either SurePlex or MALBAC amplification, we showed that known disease CNVs in the range of 3-15 Mb could be reliably and accurately detected at the correct genomic positions. These findings indicate that our CNV-Seq pipeline incorporating either SurePlex or MALBAC as the key initial WGA step is a powerful methodology for clinical PGD to identify euploid embryos in a patient's cohort for uterine transplantation.

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