Real-time reverse linkage using polar body analysis for preimplantation genetic diagnosis in female carriers of de novo mutations

doi:10.1093/humrep/dep293

Hum. Reprod. Advance Access published online on August 17, 2009
Human Reproduction, doi:10.1093/humrep/dep293

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© The Author 2009. Published by Oxford University Press on behalf of the European Society of Human Reproduction and Embryology. All rights reserved. For Permissions, please email: journals.permissions@oxfordjournals.org

Real-time reverse linkage using polar body analysis for preimplantation genetic diagnosis in female carriers of de novo mutations

Gheona Altarescu¹^,2^,3, Talia Eldar-Geva¹^,2, Irit Varshower², Barry Brooks², Edith Zylber Haran², Ehud J. Margalioth¹^,2, Ephrat Levy-Lahad¹^,2 and Paul Renbaum²

¹ Hebrew University School of Medicine, Jerusalem, Israel ² Medical Genetics Institute and IVF Unit, Zohar PGD Lab, Shaare Zedek Medical Center, Jerusalem, Israel

³ Correspondence address. Preimplantation Genetic Unit, Medical Genetics Institute, Shaare Zedek Medical Center, Jerusalem, Israel. Tel: +972-26666435; Fax: +972-26666935; E-mail: gheona{at}szmc.org.il

BACKGROUND: Single cell diagnosis for preimplantation genetic diagnosis(PGD) requires simultaneous analysis of multiple linked polymorphicmarkers in addition to mutation analysis in order to reducemisdiagnosis. This type of analysis requires building familyhaplotypes spanning at least two generations. We present threechildless couples in whom the female was a de novo mutationcarrier in the Duchenne Muscular Dystrophy (DMD), incontinentiapigmenti (IKBKG) or Neurofibromatosis type 2 (NF2) genes, precludinglinkage prior to the PGD cycle. We constructed haplotypes basedon linked polymorphic markers in these families and performedconcurrent diagnosis enabling embryo transfer from the firstPGD cycle.

METHODS: Informative markers flanking the DMD, IKBKG and NF2 genes wereused to construct non-linked haplotypes. Polar bodies 1 (PB1)and 2 (PB2) were biopsied and analyzed to determine allelicassociation between the mutation and markers in multiplex PCRreactions.

RESULTS: For each family, the first PGD cycle allowed the establishmentof linked haplotypes based on homozygous PB1 and PB2 analysis;however, no embryos were available for transfer. Subsequentcycles, when performed, confirmed this linkage. A mutation-freechild was born to the family affected with DMD and an ongoingpregnancy (32 weeks) was achieved with the carrier of the IKBKGdeletion.

CONCLUSIONS: PB analysis for reverse linkage in real-time coupled with thePGD cycle is a powerful tool for diagnosis and linkage betweenmarkers and de novo mutations for maternal autosomal dominantor X-linked disorders. Simultaneous amplification of multipleinformative markers in conjunction with the mutation allowsthe building of familial haplotypes and accurate PGD analysis.

Key words: preimplantation genetic diagnosis/polar bodies/single cell mutiplex PCR/de novo mutations/reverse linkage

Submitted on June 24, 2009; resubmitted on July 16, 2009; accepted on July 20, 2009.

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