A Proposal for Reproductive Counselling in Carriers of Robertsonian Translocations: 10 Years of Experience with Preimplantation Genetic Diagnosis

Overview

Journal Hum Reprod

Publisher Oxford University Press

Specialty Reproductive Medicine

Date 2009 Jun 5

PMID 19493873

Citations 16

Authors

Kathelijn Keymolen

Catherine Staessen

Willem Verpoest

An Michiels

Maryse Bonduelle

Patrick Haentjens

Josiane Vanderelst

Inge Liebaers

Affiliations

Soon will be listed here.

Abstract

Background: Carriers of Robertsonian translocations are at increased risk for infertility, repeated miscarriage and aneuploid offspring. In the present study, 10 years of experience with preimplantation genetic diagnosis (PGD) for Robertsonian translocations is reviewed and these data are used to improve the reproductive counselling in the carriers.

Methods: A retrospective analysis was performed of all requests and cycles for PGD for Robertsonian translocations at our centre between January 1997 and December 2006. Data on the characteristics of the couples and on the PGD cycles were retrieved from the medical records. These data were recorded for the whole group and according to the sex of the carrier.

Results: A total of 111 couples made a request for PGD in our centre, of which 76 had at least one PGD cycle. In the PGD cycles embryo transfer could take place in 66.1% of the cycles with oocyte pick-up and positive hCG was found in 42.7% of the cycles with embryo transfer. The live born delivery rate was 20.2% per cycle with oocyte retrieval and 30.5% per cycle with embryo transfer.

Conclusions: With a live birth delivery rate of 32.9% per couple, PGD is considered a good option for these couples, especially when there is a coexisting fertility problem. PGD reduces the risk of miscarriage and allows couples to have a healthy child within a relatively short time span compared with spontaneous pregnancies. However, for young, fertile couples, the chances of having a healthy child after a number of spontaneous pregnancies, should not be ignored.

Citing Articles

Cytogenetic analysis of 3488 patients with recurrent pregnancy loss: An experience of two decades from a tertiary care center in South India.

Singhal P, Maharjan K, Srivastava V, Shenoy V, Kamath V, Aleyamma T Med J Armed Forces India. 2025; 80(6):675-686.

PMID: 39990533 PMC: 11842917. DOI: 10.1016/j.mjafi.2023.09.010.

Recurrent miscarriage and male factor infertility: diagnostic and therapeutic implications. A narrative review.

Gkeka K, Symeonidis E, Tsampoukas G, Moussa M, Issa H, Kontogianni E Cent European J Urol. 2024; 76(4):336-346.

PMID: 38230311 PMC: 10789276. DOI: 10.5173/ceju.2023.74.

Retrospective Analysis of Meiotic Segregation Pattern and Reproductive Outcomes in Blastocysts from Robertsonian Preimplantation Genetic Testing Cycles.

Jia M, Shi J, Xue X Reprod Sci. 2023; 30(10):2983-2989.

PMID: 37099230 DOI: 10.1007/s43032-023-01244-6.

Age and Serum AMH and FSH Levels as Predictors of the Number of Oocytes Retrieved from Chromosomal Translocation Carriers after Controlled Ovarian Hyperstimulation: Applicability and Limitations.

Shilenkova Y, Pendina A, Mekina I, Efimova O, Komarova E, Lesik E Genes (Basel). 2020; 12(1).

PMID: 33375549 PMC: 7824090. DOI: 10.3390/genes12010018.

Noninvasive prenatal testing for chromosome aneuploidies and subchromosomal microdeletions/microduplications in a cohort of 8141 single pregnancies.

Hu H, Wang L, Wu J, Zhou P, Fu J, Sun J Hum Genomics. 2019; 13(1):14.

PMID: 30871627 PMC: 6419401. DOI: 10.1186/s40246-019-0198-2.