Perinatal follow-up of children born after preimplantation genetic diagnosis between 1995 and 2014

Malou Heijligers; Aafke Van Montfoort; Madelon Meijer-Hoogeveen; Frank Broekmans; Katelijne Bouman; Irene Homminga; Jos Dreesen; Aimee Paulussen; John Engelen; Edith Coonen; Vyne Van der Schoot; Marieke van Deursen-Luijten; Nienke Muntjewerff; Andrea Peeters; Ron van Golde; Mark van der Hoeven; Yvonne Arens; Christine de Die-Smulders

doi:10.1007/s10815-018-1286-2

Perinatal follow-up of children born after preimplantation genetic diagnosis between 1995 and 2014

Malou Heijligers^*
, Aafke Van Montfoort
, Madelon Meijer-Hoogeveen
, Frank Broekmans
, Katelijne Bouman
, Irene Homminga
, Jos Dreesen
, Aimee Paulussen
, John Engelen
, Edith Coonen
, Vyne Van der Schoot
, Marieke van Deursen-Luijten
, Nienke Muntjewerff
, Andrea Peeters
, Ron van Golde
, Mark van der Hoeven
, Yvonne Arens
, Christine de Die-Smulders

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Purpose We aim to evaluate the safety of PGD. We focus on the congenital malformation rate and additionally report on adverse perinatal outcome.

Methods We collated data from a large group of singletons and multiples born after PGD between 1995 and 2014. Data on congenital malformation rates in live born children and terminated pregnancies, misdiagnosis rate, birth parameters, perinatal mortality, and hospital admissions were prospectively collected by questionnaires.

Results Four hundred thirty-nine pregnancies in 381 women resulted in 364 live born children. Nine children (2.5%) had major malformations. This percentage is consistent with other PGD cohorts and comparable to the prevalence reported by the European Surveillance of Congenital Anomalies (EUROCAT). We reported one misdiagnosis resulting in a spontaneous abortion of a fetus with an unbalanced chromosome pattern. 20% of the children were born premature (<37 weeks) and less than 15% had a low birth weight. The incidence of hospital admissions is in line with prematurity and low birth weight rate. One child from a twin, one child from a triplet, and one singleton died at 23, 32, and 37 weeks of gestation respectively.

Conclusions We found no evidence that PGD treatment increases the risk on congenital malformations or adverse perinatal outcome.

Original language	English
Pages (from-to)	1995-2002
Number of pages	8
Journal	Journal of Assisted Reproduction and Genetics
Volume	35
Issue number	11
DOIs	https://doi.org/10.1007/s10815-018-1286-2
Publication status	Published - Nov 2018

Keywords

Preimplantation genetic diagnosis
Perinatal outcome
Congenital malformations
Children
Follow-up
ESHRE PGD CONSORTIUM
HUMAN EMBRYOS
BIRTH-WEIGHT
PREGNANCIES
MISDIAGNOSIS
METAANALYSIS
BLASTOMERE
ANEUPLOIDY
NEWBORNS
OUTCOMES

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Heijligers, M., Van Montfoort, A., Meijer-Hoogeveen, M., Broekmans, F., Bouman, K., Homminga, I., Dreesen, J., Paulussen, A., Engelen, J., Coonen, E., Van der Schoot, V., van Deursen-Luijten, M., Muntjewerff, N., Peeters, A., van Golde, R., van der Hoeven, M., Arens, Y., & de Die-Smulders, C. (2018). Perinatal follow-up of children born after preimplantation genetic diagnosis between 1995 and 2014. Journal of Assisted Reproduction and Genetics, 35(11), 1995-2002. https://doi.org/10.1007/s10815-018-1286-2

@article{3007fa6b4dd047aca0c16817d42dff86,

title = "Perinatal follow-up of children born after preimplantation genetic diagnosis between 1995 and 2014",

abstract = "Purpose We aim to evaluate the safety of PGD. We focus on the congenital malformation rate and additionally report on adverse perinatal outcome.Methods We collated data from a large group of singletons and multiples born after PGD between 1995 and 2014. Data on congenital malformation rates in live born children and terminated pregnancies, misdiagnosis rate, birth parameters, perinatal mortality, and hospital admissions were prospectively collected by questionnaires.Results Four hundred thirty-nine pregnancies in 381 women resulted in 364 live born children. Nine children (2.5\%) had major malformations. This percentage is consistent with other PGD cohorts and comparable to the prevalence reported by the European Surveillance of Congenital Anomalies (EUROCAT). We reported one misdiagnosis resulting in a spontaneous abortion of a fetus with an unbalanced chromosome pattern. 20\% of the children were born premature (<37 weeks) and less than 15\% had a low birth weight. The incidence of hospital admissions is in line with prematurity and low birth weight rate. One child from a twin, one child from a triplet, and one singleton died at 23, 32, and 37 weeks of gestation respectively.Conclusions We found no evidence that PGD treatment increases the risk on congenital malformations or adverse perinatal outcome.",

keywords = "Preimplantation genetic diagnosis, Perinatal outcome, Congenital malformations, Children, Follow-up, ESHRE PGD CONSORTIUM, HUMAN EMBRYOS, BIRTH-WEIGHT, PREGNANCIES, MISDIAGNOSIS, METAANALYSIS, BLASTOMERE, ANEUPLOIDY, NEWBORNS, OUTCOMES",

author = "Malou Heijligers and \{Van Montfoort\}, Aafke and Madelon Meijer-Hoogeveen and Frank Broekmans and Katelijne Bouman and Irene Homminga and Jos Dreesen and Aimee Paulussen and John Engelen and Edith Coonen and \{Van der Schoot\}, Vyne and \{van Deursen-Luijten\}, Marieke and Nienke Muntjewerff and Andrea Peeters and \{van Golde\}, Ron and \{van der Hoeven\}, Mark and Yvonne Arens and \{de Die-Smulders\}, Christine",

year = "2018",

month = nov,

doi = "10.1007/s10815-018-1286-2",

language = "English",

volume = "35",

pages = "1995--2002",

journal = "Journal of Assisted Reproduction and Genetics",

issn = "1058-0468",

publisher = "Springer",

number = "11",

}

Heijligers, M, Van Montfoort, A, Meijer-Hoogeveen, M, Broekmans, F, Bouman, K, Homminga, I, Dreesen, J , Paulussen, A, Engelen, J, Coonen, E, Van der Schoot, V, van Deursen-Luijten, M, Muntjewerff, N , Peeters, A , van Golde, R, van der Hoeven, M, Arens, Y & de Die-Smulders, C 2018, 'Perinatal follow-up of children born after preimplantation genetic diagnosis between 1995 and 2014', Journal of Assisted Reproduction and Genetics, vol. 35, no. 11, pp. 1995-2002. https://doi.org/10.1007/s10815-018-1286-2

TY - JOUR

T1 - Perinatal follow-up of children born after preimplantation genetic diagnosis between 1995 and 2014

AU - Heijligers, Malou

AU - Van Montfoort, Aafke

AU - Meijer-Hoogeveen, Madelon

AU - Broekmans, Frank

AU - Bouman, Katelijne

AU - Homminga, Irene

AU - Dreesen, Jos

AU - Paulussen, Aimee

AU - Engelen, John

AU - Coonen, Edith

AU - Van der Schoot, Vyne

AU - van Deursen-Luijten, Marieke

AU - Muntjewerff, Nienke

AU - Peeters, Andrea

AU - van Golde, Ron

AU - van der Hoeven, Mark

AU - Arens, Yvonne

AU - de Die-Smulders, Christine

PY - 2018/11

Y1 - 2018/11

N2 - Purpose We aim to evaluate the safety of PGD. We focus on the congenital malformation rate and additionally report on adverse perinatal outcome.Methods We collated data from a large group of singletons and multiples born after PGD between 1995 and 2014. Data on congenital malformation rates in live born children and terminated pregnancies, misdiagnosis rate, birth parameters, perinatal mortality, and hospital admissions were prospectively collected by questionnaires.Results Four hundred thirty-nine pregnancies in 381 women resulted in 364 live born children. Nine children (2.5%) had major malformations. This percentage is consistent with other PGD cohorts and comparable to the prevalence reported by the European Surveillance of Congenital Anomalies (EUROCAT). We reported one misdiagnosis resulting in a spontaneous abortion of a fetus with an unbalanced chromosome pattern. 20% of the children were born premature (<37 weeks) and less than 15% had a low birth weight. The incidence of hospital admissions is in line with prematurity and low birth weight rate. One child from a twin, one child from a triplet, and one singleton died at 23, 32, and 37 weeks of gestation respectively.Conclusions We found no evidence that PGD treatment increases the risk on congenital malformations or adverse perinatal outcome.

AB - Purpose We aim to evaluate the safety of PGD. We focus on the congenital malformation rate and additionally report on adverse perinatal outcome.Methods We collated data from a large group of singletons and multiples born after PGD between 1995 and 2014. Data on congenital malformation rates in live born children and terminated pregnancies, misdiagnosis rate, birth parameters, perinatal mortality, and hospital admissions were prospectively collected by questionnaires.Results Four hundred thirty-nine pregnancies in 381 women resulted in 364 live born children. Nine children (2.5%) had major malformations. This percentage is consistent with other PGD cohorts and comparable to the prevalence reported by the European Surveillance of Congenital Anomalies (EUROCAT). We reported one misdiagnosis resulting in a spontaneous abortion of a fetus with an unbalanced chromosome pattern. 20% of the children were born premature (<37 weeks) and less than 15% had a low birth weight. The incidence of hospital admissions is in line with prematurity and low birth weight rate. One child from a twin, one child from a triplet, and one singleton died at 23, 32, and 37 weeks of gestation respectively.Conclusions We found no evidence that PGD treatment increases the risk on congenital malformations or adverse perinatal outcome.

KW - Preimplantation genetic diagnosis

KW - Perinatal outcome

KW - Congenital malformations

KW - Children

KW - Follow-up

KW - ESHRE PGD CONSORTIUM

KW - HUMAN EMBRYOS

KW - BIRTH-WEIGHT

KW - PREGNANCIES

KW - MISDIAGNOSIS

KW - METAANALYSIS

KW - BLASTOMERE

KW - ANEUPLOIDY

KW - NEWBORNS

KW - OUTCOMES

U2 - 10.1007/s10815-018-1286-2

DO - 10.1007/s10815-018-1286-2

M3 - Article

C2 - 30187425

SN - 1058-0468

VL - 35

SP - 1995

EP - 2002

JO - Journal of Assisted Reproduction and Genetics

JF - Journal of Assisted Reproduction and Genetics

IS - 11

ER -

Perinatal follow-up of children born after preimplantation genetic diagnosis between 1995 and 2014

Abstract

Keywords

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