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Literature DB >> 30626931

Inverse PCR to perform long-distance haplotyping: main applications to improve preimplantation genetic diagnosis in hemophilia.

Miguel Martín Abelleyro¹, Vanina Daniela Marchione¹, Micaela Palmitelli¹, Claudia Pamela Radic¹, Daniela Neme², Irene Beatriz Larripa¹, Enrique Medina-Acosta³, Carlos Daniel De Brasi^1,4, Liliana Carmen Rossetti⁵.

Abstract

Among other applications of long-distance haplotype phasing in clinical genetics, determination of linked DNA markers as surrogate for problematic structural variants (e.g., repeat-mediated rearrangements) is essential to perform diagnosis from low-quality DNA samples. We describe a next-of-kin-independent (physical) phasing approach based on inverse-PCR (iPCR) paired-end amplification (PI). This method enables typing the multialleles of the short tandem repeat (STR) F8Int21[CA]n at the F8-intron 21, as a surrogate DNA marker for the F8-intron 22 inversion (Inv22), the hemophilia A-causative hotspot, within the transmitted haplotype in informative carriers. We provide proof-of-concept by blindly validating the PI approach in 15 carrier mother/affected-son duos. Every F8Int21[CA]n STR allele determined in phase with the Inv22 allele in the female carriers from the informative duos was confirmed in the hemizygous proband (P = 0.00003). A second surrogate STR locus at the F8-IVS22 was obtained by the PI approach improving severe-HA preimplantation genetic diagnosis by augmenting heterozygosity in Inv22 carriers bypassing the requirement for family linkage analysis. The ability of the PI-assay to combine other marker pairs was demonstrated by haplotyping a SNV (F8:c.6118T > C) with a >28kb-distant F8-IVS22 STR. The PI approach has proven flexibility to target different marker pairs and has potential for multiplex characterization of iPCR products by massively parallel sequencing.

Entities: Disease Mutation

Mesh：

Substances：
Genetic Markers

Year: 2019 PMID： 30626931 PMCID： PMC6460640 DOI： 10.1038/s41431-018-0334-9

Source DB: PubMed Journal: Eur J Hum Genet ISSN： 1018-4813 Impact factor: 4.246

35 in total

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Journal: Clin Chem Date: 2005-04-28 Impact factor: 8.327

6. Developing a new generation of tests for genotyping hemophilia-causative rearrangements involving int22h and int1h hotspots in the factor VIII gene.

Authors: L C Rossetti; C P Radic; I B Larripa; C D De Brasi
Journal: J Thromb Haemost Date: 2008-02-12 Impact factor: 5.824

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