Expanding Access to Noninvasive Prenatal Diagnosis for Monogenic Conditions to Consanguineous Families

单倍型 遗传学 产前诊断 基因型 遗传咨询 单核苷酸多态性 血缘关系 基因检测 生物 怀孕 医学 胎儿 基因
作者
Britt Hanson,Joe J. Shaw,Nikita Povarnitsyn,Benjamin Bowns,Elizabeth Young,Amy Gerrish,Stephanie Allen,Elizabeth Scotchman,Lyn S. Chitty,Natalie Chandler
出处
期刊:Clinical Chemistry [American Association for Clinical Chemistry]
被引量:1
标识
DOI:10.1093/clinchem/hvae023
摘要

Cell-free fetal DNA exists within the maternal bloodstream during pregnancy and provides a means for noninvasive prenatal diagnosis (NIPD). Our accredited clinical service offers definitive NIPD for several autosomal recessive (AR) and X-linked conditions using relative haplotype dosage analysis (RHDO). RHDO involves next-generation sequencing (NGS) of thousands of common single nucleotide polymorphism (SNPs) surrounding the gene of interest in the parents and an affected or unaffected offspring to conduct haplotype phasing of the high- and low-risk alleles. NGS is carried out in parallel on the maternal cell-free DNA, and fetal inheritance is predicted using sensitive dosage calculations performed at sites where the parental genotypes differ. RHDO is not currently offered to consanguineous couples owing to the shared haplotype between parents. Here we test the expansion of RHDO for AR monogenic conditions to include consanguineous couples.The existing sequential probability ratio test analysis pipeline was modified to apply to SNPs where both parents are heterozygous for the same genotype. Quality control thresholds were developed using 33 nonconsanguineous cases. The performance of the adapted RHDO pipeline was tested on 8 consanguineous cases.The correct fetal genotype was predicted by our revised RHDO approach in all conclusive cases with known genotypes (n = 5). Haplotype block classification accuracies of 94.5% and 93.9% were obtained for the nonconsanguineous and consanguineous case cohorts, respectively.Our modified RHDO pipeline correctly predicts the genotype in fetuses from consanguineous families, allowing the potential to expand access to NIPD services for these families.
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