Pregnancies following blastocyst stage transfer in PGD cycles at risk for {beta}-thalassaemic haemoglobinopathies

doi:10.1093/humrep/17.1.25

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Human Reproduction, Vol. 17, No. 1, 25-31, January 2002
© 2002 European Society of Human Reproduction and Embryology

Pregnancies following blastocyst stage transfer in PGD cycles at risk for ß-thalassaemic haemoglobinopathies

G.A. Palmer¹^,3, J. Traeger-Synodinos², S. Davies¹, M. Tzetis², C. Vrettou², M. Mastrominas¹ and E. Kanavakis²

¹ Embryogenesis Fertility Clinic, Kifissias Avenue, Athens 15125 and ² Medical Genetics, Athens University, St. Sophia's Children's Hospital, Athens 11527, Greece

BACKGROUND: Preimplantation genetic diagnosis (PGD) usuallyinvolves blastomere biopsy 3 days post-insemination (p.i.),followed by genetic analysis and transfer of unaffected embryoslater on day 3 or 4. We evaluate a strategy involving embryobiopsy on day 3 p.i., genetic analysis on day 4 and, followingculture in blastocyst sequential media, transfer of unaffectedembryos on day 5 p.i. METHODS: PGD cycles were initiated in15 couples at risk of transmitting ß-thalassaemiamajor. Oocyte retrieval and ICSI were performed according tostandard protocols. Embryo culture used blastocyst sequentialmedia. Embryos were biopsied on day 3 p.i. using acid Tyrode'sfor zona drilling, and the single blastomeres were genotypedby a protocol involving nested polymerase chain reaction anddenaturing gradient gel electrophoresis analysis. RESULTS: Fortyof 109 (37%) embryos biopsied on day 3 p.i. developed to blastocystsby day 5 p.i., with at least one blastocyst available for transferin 12 cycles (80%). Genotype analysis characterized 51/109 (47%)embryos unaffected for ß-thalassaemia major, of which28 were blastocysts. Transfer of 37 day 5 p.i. embryos (blastocystsand non blastocysts) initiated eight clinical pregnancies. Implantationrate per embryo transferred was 12/37 (32%). CONCLUSIONS: Embryobiopsy on day 3, followed by delayed transfer until day 5 p.i.offers a novel and effective strategy to overcome the time limitencountered when performing PGD, without compromising embryoimplantation.

Key words: ß-thalassaemia/blastocyst stage transfer/Ca²⁺Mg²⁺ free medium/preimplantation genetic diagnosis

³ To whom correspondence should be addressed at: Centre for ReproductiveMedicine, Alpha Lab, Anastasiou 8, Athens 115 24, Greece. E-mail:gpalme{at}otenet.gr

Note added in proof

By the time of publication all embryos of the three ongoingpregnancies had been confirmed as unaffected by prenatal diagnosis.The triplet pregnancy was selectively reduced to twins at therequest of the parents and all three ongoing pregnancies wentto term, resulting in the birth of five more healthy babies.

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