Your search keyword '"van Maarle MC"' showing total 28 results

1. Rapid whole exome sequencing in pregnancies to identify the underlying genetic cause in fetuses with congenital anomalies detected by ultrasound imaging

Author

Deden, C, Neveling, K, Zafeiropopoulou, D, Gilissen, C, Pfundt, R, Rinne, T, de Leeuw, N, Faas, B, Gardeitchik, T, Sallevelt, SCEH, Paulussen, A, Stevens, SJC, Sikkel, E, Elting, MW, van Maarle, MC, Diderich, Karin, Corsten-Janssen, N, Lichtenbelt, KD, Lachmeijer, G, Vissers, LELM, Yntema, HG, Nelen, M, Feenstra, I, van Zelst-Stams, W A G, Deden, C, Neveling, K, Zafeiropopoulou, D, Gilissen, C, Pfundt, R, Rinne, T, de Leeuw, N, Faas, B, Gardeitchik, T, Sallevelt, SCEH, Paulussen, A, Stevens, SJC, Sikkel, E, Elting, MW, van Maarle, MC, Diderich, Karin, Corsten-Janssen, N, Lichtenbelt, KD, Lachmeijer, G, Vissers, LELM, Yntema, HG, Nelen, M, Feenstra, I, and van Zelst-Stams, W A G

Published

2020

2. Origin and clinical relevance of chromosomal aberrations other than the common trisomies detected by genome-wide NIPS: results of the TRIDENT study

Author

Opstal, D, van Maarle, MC, Lichtenbelt, K, Weiss, MM, Schuring-Blom, H, Bhola, SL, Hoffer, MJV, van Amsterdam, K, Macville, MV, Kooper, AJA, Faas, BHW, Govaerts, LCP, Tan-Sindhunata, GM, den Hollander, N, Feenstra, I, Galjaard, Robert-Jan, Oepkes, D, Ghesquiere, S, Brouwer, Rutger, Beulen, L, Bollen, S, Elferink, MG, Straver, R, Henneman, L, Page-Christiaens, GC, Sistermans, EA, Opstal, D, van Maarle, MC, Lichtenbelt, K, Weiss, MM, Schuring-Blom, H, Bhola, SL, Hoffer, MJV, van Amsterdam, K, Macville, MV, Kooper, AJA, Faas, BHW, Govaerts, LCP, Tan-Sindhunata, GM, den Hollander, N, Feenstra, I, Galjaard, Robert-Jan, Oepkes, D, Ghesquiere, S, Brouwer, Rutger, Beulen, L, Bollen, S, Elferink, MG, Straver, R, Henneman, L, Page-Christiaens, GC, and Sistermans, EA

Published

2018

3. Dragerschapscreening: gericht op risicogroepen of populatiebreed?:Verslag van een stakeholdermeeting POM project

Author

Holtkamp, KCA, Lakeman, P, van Maarle, MC, van der Hout, S, Dondorp, WJ, van Vliet-Lochotzki, E, Cornel, MC, and Henneman, L

Abstract

Op 29 januari 2016 is ten behoeve van het ZonMw POM project (Preconceptioneel dragerschaponderzoek Op Maat) een stakeholdermeeting gehouden om de (toekomstige) implementatie van dragerschapscreening te bespreken. Het doel van de bijeenkomst was de aanknopingspunten en uitdagingen voor een verantwoorde introductie van dragerschapscreening in Nederland in kaart te brengen. Tijdens de bijeenkomst zijn de resultaten uit eerdere onderdelen van het project gepresenteerd, is met verschillende betrokken stakeholders gezocht naar mogelijke oplossingen voor (potentiële) problemen bij de huidige implementatie van screening, met name gericht op specifieke risicogroepen, en zijn mogelijkheden van een (toekomstig) aanbod van screening op meerdere aandoeningen in de algemene bevolking verkend. Dit verslag geeft een samenvatting van de gehouden voordrachten en van de gevoerde discussie.

Published

2016

4. Dragerschapscreening: gericht op risicogroepen of populatiebreed?: Verslag van een stakeholdermeeting POM project

Author

Holtkamp, KCA, Lakeman, P, van Maarle, MC, van der Hout, S, Dondorp, WJ, van Vliet-Lochotzki, E, Cornel, MC, Henneman, L, Clinical genetics, EMGO - Quality of care, APH - Quality of Care, Amsterdam Reproduction & Development, and APH - Personalized Medicine

Abstract

Op 29 januari 2016 is ten behoeve van het ZonMw POM project (Preconceptioneel dragerschaponderzoek Op Maat) een stakeholdermeeting gehouden om de (toekomstige) implementatie van dragerschapscreening te bespreken. Het doel van de bijeenkomst was de aanknopingspunten en uitdagingen voor een verantwoorde introductie van dragerschapscreening in Nederland in kaart te brengen. Tijdens de bijeenkomst zijn de resultaten uit eerdere onderdelen van het project gepresenteerd, is met verschillende betrokken stakeholders gezocht naar mogelijke oplossingen voor (potentiële) problemen bij de huidige implementatie van screening, met name gericht op specifieke risicogroepen, en zijn mogelijkheden van een (toekomstig) aanbod van screening op meerdere aandoeningen in de algemene bevolking verkend. Dit verslag geeft een samenvatting van de gehouden voordrachten en van de gevoerde discussie.

Published

2016

5. Phenotype-to-Genotype Description of Prenatal Suspected and Postnatal Discovered Upper Limb Anomalies: A Retrospective Cohort Study.

Author

Arduç A, van Dijk SJB, Ten Cate FJ, van Doesburg MHM, Linskens IH, van Leeuwen E, van Maarle MC, and Pajkrt E

Subjects

Humans, Retrospective Studies, Female, Pregnancy, Male, Infant, Newborn, Polydactyly genetics, Polydactyly epidemiology, Polydactyly diagnosis, Polydactyly diagnostic imaging, Genotype, Cohort Studies, Syndactyly genetics, Syndactyly diagnosis, Syndactyly epidemiology, Adult, Upper Extremity Deformities, Congenital genetics, Upper Extremity Deformities, Congenital diagnosis, Upper Extremity Deformities, Congenital diagnostic imaging, Ultrasonography, Prenatal, Phenotype

Abstract

Objective: To evaluate phenotype and genotype characteristics of fetuses and children with upper limb anomalies., Method: Retrospective cohort study of a prenatal and postnatal cohort with upper limb anomalies from January 2007 to December 2021 in a Fetal Medicine Unit. Prenatally on ultrasound suspected upper limb anomalies, such as transverse and longitudinal reduction defects, polydactyly, and syndactyly, and postnatally identified children referred to the Congenital Hand Team were evaluated separately., Results: The prenatal group included 199 pregnancies: 64 transverse and 19 longitudinal reduction defects, 103 polydactylies, and 13 cases with syndactyly. The majority of cases with longitudinal reduction defects (n = 10, 52.6%), polydactyly (n = 62, 60.2%), and syndactyly (n = 10, 76.9%) were non-isolated, as opposed to transverse reduction defects, which were generally isolated (n = 41, 64.1%). The postnatal cohort included 362 children with upper limb anomalies with 49 transverse and 22 longitudinal reduction defects, 226 polydactylies, and 65 syndactylies. Chromosomal or monogenic abnormalities were identified in 76/199 (38.2%) cases of the prenatal cohort and in 31/362 (8.6%) cases of the postnatal cohort., Conclusion: Prenatal identification of minor defects of the digits is a challenge, with more postnatal than prenatal cases. The majority of cases with isolated anomalies in both groups had no underlying chromosomal or monogenic cause, nor were they associated with a syndrome, as compared to the non-isolated cases. Conducting structural anomaly scans and genetic counseling are crucial to assess the risk of genetic abnormalities., (© 2024 The Author(s). Prenatal Diagnosis published by John Wiley & Sons Ltd.)

Published

2025

6. Reply.

Author

Bet BB, Lugthart MA, Linskens IH, van Maarle MC, van Leeuwen E, and Pajkrt E

Published

2024

7. Adverse pregnancy outcome in fetuses with early increased nuchal translucency: prospective cohort study.

Author

Bet BB, Lugthart MA, Linskens IH, van Maarle MC, van Leeuwen E, and Pajkrt E

Subjects

Humans, Female, Pregnancy, Prospective Studies, Adult, Gestational Age, Congenital Abnormalities diagnostic imaging, Congenital Abnormalities embryology, Aneuploidy, Nuchal Translucency Measurement statistics & numerical data, Pregnancy Outcome epidemiology, Pregnancy Trimester, First, Crown-Rump Length

Abstract

Objectives: An increased nuchal translucency (NT) thickness of ≥ 3.5 mm is a well-established marker for congenital anomalies and adverse pregnancy outcome between 11 and 14 weeks' gestation, but little is known about its performance as a screening tool before 11 weeks. We aimed to investigate, in a prospective setting, whether fetuses with increased NT before 11 weeks are at risk for adverse pregnancy outcome., Methods: This was a prospective cohort study including pregnant women with a viable fetus with NT ≥ 2.5 mm and a crown-rump length (CRL) < 45 mm. All included women were referred to our fetal medicine unit (FMU) and scheduled for a follow-up scan where the NT was remeasured after 1 week when the CRL was > 45 mm. Two groups were evaluated: cases with a normalized NT (< 3.5 mm) and cases with persistently increased NT (≥ 3.5 mm). The cases were monitored until 4 weeks after delivery. The main outcome was a composite adverse outcome of aneuploidy, other genetic disorders, structural anomalies and pregnancy loss. We performed subgroup analyses of NT thickness at inclusion and normalized or persistently increased NT at follow-up., Results: The study included 109 cases, of which 39 (35.8%) had an adverse pregnancy outcome. Of these, 64.1% (25/39) were aneuploid, corresponding to 22.9% (25/109) of the total study population. In the subgroups of NT thickness at inclusion of 2.5-3.4 mm, 3.5-4.4 mm and ≥ 4.5 mm, an adverse outcome was reported in 22.0% (9/41), 40.0% (18/45) and 52.2% (12/23), respectively. In fetuses with a normalized NT and without ultrasound abnormalities at the follow-up scan, the incidence of adverse outcome was 8.5% (5/59), of which 5.1% (3/59) cases were aneuploid., Conclusions: Fetuses with an early increased NT thickness are at considerable risk of an adverse pregnancy outcome, even if the NT normalizes after 11 weeks. Not all congenital anomalies can be diagnosed with routine first-trimester screening, such as non-invasive prenatal testing and/or a first-trimester anomaly scan. Therefore, expectant parents should always be referred to a FMU for detailed ultrasonography. Invasive prenatal testing should be offered if an increased NT of ≥ 2.5 mm is observed before 11 weeks' gestation. © 2024 The Authors. Ultrasound in Obstetrics & Gynecology published by John Wiley & Sons Ltd on behalf of International Society of Ultrasound in Obstetrics and Gynecology., (© 2024 The Authors. Ultrasound in Obstetrics & Gynecology published by John Wiley & Sons Ltd on behalf of International Society of Ultrasound in Obstetrics and Gynecology.)

Published

2024

8. Eliminating first trimester combined testing: Consequences for early detection of significant fetal anomalies.

Author

Lugthart MA, Heinrich H, Ertugrul I, Nsiah-Asare EN, van de Kamp K, Linskens IH, van Maarle MC, van Leeuwen E, and Pajkrt E

Subjects

Humans, Female, Pregnancy, Adult, Cohort Studies, Congenital Abnormalities diagnosis, Congenital Abnormalities epidemiology, Aneuploidy, Prenatal Diagnosis methods, Prenatal Diagnosis statistics & numerical data, Early Diagnosis, Pregnancy Trimester, First, Cell-Free Nucleic Acids blood, Cell-Free Nucleic Acids analysis

Abstract

Objective: To determine whether implementation of cell-free DNA (cfDNA) testing for aneuploidy as a first-tier test and subsequent abolition of first trimester combined testing (FCT) affected the first trimester detection (<14 weeks) of certain fetal anomalies., Methods: We performed a geographical cohort study in two Fetal Medicine Units between 2011 and 2020, including 705 fetuses with prenatally detected severe brain, abdominal wall and congenital heart defects. Cases were divided into two groups: before (n = 396) and after (n = 309) cfDNA introduction. The primary outcome was the first trimester detection rate (<14 weeks) overall and for non-chromosomal anomalies solely., Results: Overall, gastroschisis, AVSD and HLHS were detected more often in the first trimester in the before group compared to the after group, respectively 54.5% versus 18.5% (p = 0.004), 45.9% versus 26.9% (p = 0.008) and 30% versus 3.4% (p = 0.005). After exclusion of chromosomal anomalies identifiable through cfDNA testing, the detection of AVSD remained higher in the before group (43.3% vs. 9.5%, p = 0.02), leading to a possible earlier gestation at termination. The termination of pregnancy (TOP) rate did not differ among the groups. In the after group, referrals for suspected anomalies following a dating scan between 11 and 14 weeks significantly increased from 17.4% to 29.1% (p < 0.001)., Conclusion: This study underscores the value of a scan dedicated to fetal anatomy in the first trimester as we observed a decline in the early detection of certain fetal anomalies (detectable in the first trimester) subsequent to the abolition of FCT., (© 2024 The Authors. Prenatal Diagnosis published by John Wiley & Sons Ltd.)

Published

2024

9. Expanding the molecular and clinical spectrum of autosomal recessive congenital ichthyosis caused by pathogenic variants in NIPAL4 and PNPLA1 and evaluation of novel therapeutic interventions.

Author

Rossel SVJ, Clabbers JMK, Steijlen PM, van den Akker PC, Spuls PI, Middelkamp Hup MA, van Maarle MC, Vreeburg M, Bolling MC, van Geel M, and Gostyński A

Subjects

Humans, Acyltransferases, Genes, Recessive, Mutation, Phospholipases, Ichthyosis, Lamellar genetics

Published

2023

10. Efficacy and Toxicity of Calcitonin Treatment in Children with Cherubism: A Single-Center Cohort Study.

Author

Schreuder WH, Meijer EB, Cleven AHG, Edelenbos E, Klop C, Schreurs R, de Jong RT, van Maarle MC, Horsthuis RBG, de Lange J, and van den Berg H

Subjects

Child, Humans, Male, Female, Cohort Studies, Retrospective Studies, Minerals, Calcitonin adverse effects, Cherubism drug therapy

Abstract

Cherubism is a rare autosomal dominant disease characterized by expansile osteolytic jawbone lesions. The effect and safety of off-label calcitonin treatment during the progressive phase of the disease are not well described. In this retrospective study, we present data on the radiological response and adverse effects of subcutaneously administered calcitonin in a cohort of nine cherubism children (three female, six male). Two of the nine patients underwent two separate treatment courses with a significant off-treatment interval in between; therefore, a total of 11 treatment courses with a mean duration of 17.9 months (range <1 to 35, SD 10.8) were studied. To measure the response, the cumulative volume of cherubism lesions was calculated from available three-dimensional imaging. The primary outcome was the change in the volume of lesions during calcitonin treatment and only assessed for the eight treatment courses with a minimal duration of 6 months. A statistically significant reduction in the mean cumulative volume of lesions was seen regardless of treatment duration. Average volume reduction was highest in the first half year of treatment, with a gradual, ongoing reduction thereafter. For the secondary outcome, the change in the cumulative volume of lesions after treatment cessation was assessed for the seven treatment courses with follow-up imaging available. After six of these seven treatment courses, the cumulative volume increased again but remained undoubtedly smaller than the initial volume at the start of therapy. Adverse effects were assessed for all 11 treatment courses and occurred in 73% of them. Most adverse effects were mild and low grade, with the most severe being one grade 3 symptomatic hypocalcemia requiring hospitalization and early treatment termination. Calcitonin treatment seems effective and tolerable in treating actively progressing cherubism in children. However, further research is required to better understand the pharmacological treatment of cherubism, including also other drugs, dosing, and protocols. © 2023 The Authors. Journal of Bone and Mineral Research published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research (ASBMR)., (© 2023 The Authors. Journal of Bone and Mineral Research published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research (ASBMR).)

Published

2023

11. Counseling couples at risk of having a child with homozygous familial hypercholesterolemia - Clinical experience and recommendations.

Author

Tromp TR, Reijman MD, Wiegman A, Hovingh GK, Defesche JC, van Maarle MC, and Mathijssen IB

Subjects

Humans, Child, Phenotype, Prospective Studies, Counseling, Homozygote, Homozygous Familial Hypercholesterolemia, Hyperlipoproteinemia Type II drug therapy

Abstract

Homozygous familial hypercholesterolemia (HoFH) is a rare, potentially life-limiting, inherited disorder of lipoprotein metabolism characterized by extremely high low-density lipoprotein cholesterol levels. When both parents have heterozygous FH, there is a 25% chance they will conceive a child with HoFH. Here we describe our clinical experience with two such prospective parent couples who were counseled regarding reproductive options and prenatal testing for HoFH. These cases showcase how, in consultation with a molecular geneticist and pediatric cardiologist, parents may be informed of the prognosis and treatment outlook of HoFH based on the FH-variants carried, to ultimately make personal decisions on reproductive options. One couple opted for prenatal testing and termination of pregnancy in case HoFH was found, while the other accepted the risk without testing. We review the available literature on preconception counseling for HoFH and provide practical guidance to clinicians counseling at-risk couples. Optimal counseling of prospective parents may help prevent future physical and psychological problems for both parent and child., Competing Interests: Declaration of Competing Interest AW has received consulting fees from Novartis, is chair of the Steering Committee for the ORION-13 and ORION-16 trial, received payment or honoraria from Amgen, Regeneron and Novartis, and participated on a Data Safety Monitoring Board or Advisory Board of Amgen. GKH reports research grants from the Netherlands Organization for Scientific Research (vidi 016.156.445), CardioVascular Research Initiative, European Union and the Klinkerpad fonds; institutional research support from Aegerion, Amgen, AstraZeneca, Eli Lilly, Genzyme, Ionis, Kowa, Pfizer, Regeneron, Roche, Sanofi, and The Medicines Company; speaker's bureau and consulting fees from Amgen, Aegerion, Sanofi, and Regeneron until April 2019 (fees paid to the academic institution); and part-time employment at Novo Nordisk A/S, Denmark since April 2019. TRT, MDR, JCD, MCvM and IMA declare no conflicts of interest., (Copyright © 2022. Published by Elsevier Inc.)

Published

2023

12. Noninvasive Prenatal Test Results Indicative of Maternal Malignancies: A Nationwide Genetic and Clinical Follow-Up Study.

Author

Heesterbeek CJ, Aukema SM, Galjaard RH, Boon EMJ, Srebniak MI, Bouman K, Faas BHW, Govaerts LCP, Hoffer MJV, den Hollander NS, Lichtenbelt KD, van Maarle MC, van Prooyen Schuurman L, van Rij MC, Schuring-Blom GH, Stevens SJC, Tan-Sindhunata G, Zamani Esteki M, de Die-Smulders CEM, Tjan-Heijnen VCG, Henneman L, Sistermans EA, and Macville MVE

Subjects

Aneuploidy, Chromosome Aberrations, Female, Follow-Up Studies, Humans, Pregnancy, Retrospective Studies, Neoplasms, Prenatal Diagnosis methods

Abstract

Purpose: Noninvasive prenatal testing (NIPT) for fetal aneuploidy screening using cell-free DNA derived from maternal plasma can incidentally raise suspicion for cancer. Diagnostic routing after malignancy suspicious-NIPT faces many challenges. Here, we detail malignancy suspicious-NIPT cases, and describe the clinical characteristics, chromosomal aberrations, and diagnostic routing of the patients with a confirmed malignancy. Clinical lessons can be learned from our experience., Methods: Patients with NIPT results indicative of a malignancy referred for tumor screening between April 2017 and April 2020 were retrospectively included from a Dutch nationwide NIPT implementation study, TRIDENT-2. NIPT profiles from patients with confirmed malignancies were reviewed, and the pattern of chromosomal aberrations related to tumor type was analyzed. We evaluated the diagnostic contribution of clinical and genetic examinations., Results: Malignancy suspicious-NIPT results were reported in 0.03% after genome-wide NIPT, and malignancies confirmed in 16 patients (16/48, 33.3%). Multiple chromosomal aberrations were seen in 23 of 48 patients with genome-wide NIPT, and a malignancy was confirmed in 16 patients (16/23, 69.6%). After targeted NIPT, 0.005% malignancy suspicious-NIPT results were reported, in 2/3 patients a malignancy was confirmed. Different tumor types and stages were diagnosed, predominantly hematologic malignancies (12/18). NIPT data showed recurrent gains and losses in primary mediastinal B-cell lymphomas and classic Hodgkin lymphomas. Magnetic resonance imaging and computed tomography were most informative in diagnosing the malignancy., Conclusion: In 231,896 pregnant women, a low percentage (0.02%) of NIPT results were assessed as indicative of a maternal malignancy. However, when multiple chromosomal aberrations were found, the risk of a confirmed malignancy was considerably high. Referral for extensive oncologic examination is recommended, and may be guided by tumor-specific hallmarks in the NIPT profile.

Published

2022

13. Clinical impact of additional findings detected by genome-wide non-invasive prenatal testing: Follow-up results of the TRIDENT-2 study.

Author

van Prooyen Schuurman L, Sistermans EA, Van Opstal D, Henneman L, Bekker MN, Bax CJ, Pieters MJ, Bouman K, de Munnik S, den Hollander NS, Diderich KEM, Faas BHW, Feenstra I, Go ATJI, Hoffer MJV, Joosten M, Komdeur FL, Lichtenbelt KD, Lombardi MP, Polak MG, Jehee FS, Schuring-Blom H, Stevens SJC, Srebniak MI, Suijkerbuijk RF, Tan-Sindhunata GM, van der Meij KRM, van Maarle MC, Vernimmen V, van Zelderen-Bhola SL, van Ravesteyn NT, Knapen MFCM, Macville MVE, and Galjaard RH

Published

2022

14. Increased nuchal translucency before 11 weeks of gestation: Reason for referral?

Author

Lugthart MA, Bet BB, Elsman F, van de Kamp K, de Bakker BS, Linskens IH, van Maarle MC, van Leeuwen E, and Pajkrt E

Subjects

Adult, Cohort Studies, Female, Humans, Nuchal Translucency Measurement statistics & numerical data, Pregnancy, Pregnancy Outcome epidemiology, Prospective Studies, Referral and Consultation statistics & numerical data, Retrospective Studies, Ultrasonography, Prenatal methods, Gestational Age, Nuchal Translucency Measurement classification, Referral and Consultation standards

Abstract

Objectives: In this era of non-invasive-prenatal testing (NIPT), when dating scans are usually performed around 10 weeks of gestation, an increased NT before the official established timeframe (CRL between 45 and 84 mm) may be encountered. Information on management of these pregnancies is limited. Therefore, we evaluated the relationship between an early increased NT and adverse pregnancy outcome. Secondary, we evaluated the rate of chromosomal anomalies that might have been missed in first trimester should solely NIPT be performed as first-tier test, and the rate of adverse pregnancy outcome if NT normalizes before 14 weeks., Methods: We performed a retrospective cohort study that included all pregnancies between January 1, 2007 and June 1, 2020 in Amsterdam UMC locations AMC and VUmc. We included fetuses with a crown-rump length (CRL) < 45 mm (∼11 weeks) and a nuchal translucency (NT) measurement ≥2.5 mm. Fetuses referred with an early increased NT and a major fetal anomaly at the dating scan were excluded, as were cases of parents with a family history of monogenetic disease(s) or recognized carriers of a balanced translocation., Results: We included 120 fetuses of which 66.7% (80/120) had an adverse pregnancy outcome. Congenital anomalies were present in 56.7% (68/120), 45.8% (55/120) had a chromosomal anomaly. The prevalence of congenital anomalies was 30.3% in fetuses with NT 2.5-3.4 mm compared to 66.7% with NT ≥ 3.5 mm (p < 0.001). 16.7% (20/120) had a chromosomal anomaly that might have been missed by conventional NIPT in first trimester. We found an adverse pregnancy outcome of 24% in the group with a normalized NT compared to 78.1% in the group with a persistently increased NT (p < 0.001)., Conclusion: An early increased NT should make the sonographer alert. In this selected cohort, an early increased NT was associated with a high probability of having an adverse pregnancy outcome. Regardless of CRL, we deem that an early increased NT ≥ 3.5 mm warrants referral to a Fetal Medicine Unit for an extensive work-up. NT normalization seems favorable, but a prospective study should define the appropriate work-up for NT in the lower range (2.5-3.4 mm)., (© 2021 The Authors. Prenatal Diagnosis published by John Wiley & Sons Ltd.)

Published

2021

15. Distal muscle weakness and optic atrophy without central nervous system involvement in a patient with a homozygous missense mutation in the C19ORF12-gene.

Author

de Vries RJ, Jaeger B, Hellebrekers DMEI, Reneman L, Verhamme C, Smeets HJM, van Maarle MC, de Visser M, and Bleeker FE

Subjects

Adult, Humans, Male, Mutation, Missense, Mitochondrial Proteins genetics, Muscle Weakness genetics, Neuroaxonal Dystrophies genetics, Neuroaxonal Dystrophies pathology, Optic Atrophies, Hereditary genetics, Peripheral Nervous System Diseases genetics

Abstract

Variants of the C19ORF12-gene have been described in patients with spastic paraplegia type 43 and in patients with mitochondrial membrane protein-associated neurodegeneration (MPAN), a subtype of neurodegeneration associated with brain iron accumulation (NBIA). In both subtypes optic atrophy and neuropathy have been frequently described. This case report describes a patient with bilateral optic atrophy and severe distal muscle weakness based on motor neuropathy without involvement of the central nervous system. Exome sequencing revealed a homozygous pathogenic missense variant (c.187G>C;p.Ala63Pro) of the C19ORF12-gene while iron deposits were absent on repeat MR-imaging of the brain, thus showing that peripheral neuropathy and optic neuropathy can be the sole manifestations of the C19ORF12-related disease spectrum whereby iron accumulation in the brain may be absent., (Copyright © 2021 The Authors. Published by Elsevier B.V. All rights reserved.)

Published

2021

16. Rapid whole exome sequencing in pregnancies to identify the underlying genetic cause in fetuses with congenital anomalies detected by ultrasound imaging.

Author

Deden C, Neveling K, Zafeiropopoulou D, Gilissen C, Pfundt R, Rinne T, de Leeuw N, Faas B, Gardeitchik T, Sallevelt SCEH, Paulussen A, Stevens SJC, Sikkel E, Elting MW, van Maarle MC, Diderich KEM, Corsten-Janssen N, Lichtenbelt KD, Lachmeijer G, Vissers LELM, Yntema HG, Nelen M, Feenstra I, and van Zelst-Stams WAG

Subjects

Abnormalities, Multiple diagnosis, Abnormalities, Multiple genetics, Adult, Decision Making, Female, Fetus diagnostic imaging, Genetic Testing methods, Humans, Male, Pregnancy, Prenatal Diagnosis methods, Reproducibility of Results, Young Adult, Congenital Abnormalities diagnosis, Congenital Abnormalities genetics, Ultrasonography, Prenatal, Exome Sequencing

Abstract

Objective: The purpose of this study was to explore the diagnostic yield and clinical utility of trio-based rapid whole exome sequencing (rWES) in pregnancies of fetuses with a wide range of congenital anomalies detected by ultrasound imaging., Methods: In this observational study, we analyzed the first 54 cases referred to our laboratory for prenatal rWES to support clinical decision making, after the sonographic detection of fetal congenital anomalies. The most common identified congenital anomalies were skeletal dysplasia (n = 20), multiple major fetal congenital anomalies (n = 17) and intracerebral structural anomalies (n = 7)., Results: A conclusive diagnosis was identified in 18 of the 54 cases (33%). Pathogenic variants were detected most often in fetuses with skeletal dysplasia (n = 11) followed by fetuses with multiple major fetal congenital anomalies (n = 4) and intracerebral structural anomalies (n = 3). A survey, completed by the physicians for 37 of 54 cases, indicated that the rWES results impacted clinical decision making in 68% of cases., Conclusions: These results suggest that rWES improves prenatal diagnosis of fetuses with congenital anomalies, and has an important impact on prenatal and peripartum parental and clinical decision making., (© 2020 The Authors. Prenatal Diagnosis published by John Wiley & Sons Ltd.)

Published

2020

17. TRIDENT-2: National Implementation of Genome-wide Non-invasive Prenatal Testing as a First-Tier Screening Test in the Netherlands.

Author

van der Meij KRM, Sistermans EA, Macville MVE, Stevens SJC, Bax CJ, Bekker MN, Bilardo CM, Boon EMJ, Boter M, Diderich KEM, de Die-Smulders CEM, Duin LK, Faas BHW, Feenstra I, Haak MC, Hoffer MJV, den Hollander NS, Hollink IHIM, Jehee FS, Knapen MFCM, Kooper AJA, van Langen IM, Lichtenbelt KD, Linskens IH, van Maarle MC, Oepkes D, Pieters MJ, Schuring-Blom GH, Sikkel E, Sikkema-Raddatz B, Smeets DFCM, Srebniak MI, Suijkerbuijk RF, Tan-Sindhunata GM, van der Ven AJEM, van Zelderen-Bhola SL, Henneman L, Galjaard RH, Van Opstal D, and Weiss MM

Subjects

Adolescent, Adult, Chromosome Aberrations, Down Syndrome epidemiology, Down Syndrome genetics, Female, Follow-Up Studies, Humans, Middle Aged, Netherlands epidemiology, Pregnancy, Pregnancy Trimester, First, Prognosis, Trisomy 13 Syndrome epidemiology, Trisomy 13 Syndrome genetics, Trisomy 18 Syndrome epidemiology, Trisomy 18 Syndrome genetics, Young Adult, Down Syndrome diagnosis, Genetic Testing methods, Genome, Human, Health Plan Implementation, Prenatal Diagnosis methods, Trisomy 13 Syndrome diagnosis, Trisomy 18 Syndrome diagnosis

Abstract

The Netherlands launched a nationwide implementation study on non-invasive prenatal testing (NIPT) as a first-tier test offered to all pregnant women. This started on April 1, 2017 as the TRIDENT-2 study, licensed by the Dutch Ministry of Health. In the first year, NIPT was performed in 73,239 pregnancies (42% of all pregnancies), 7,239 (4%) chose first-trimester combined testing, and 54% did not participate. The number of trisomies 21 (239, 0.33%), 18 (49, 0.07%), and 13 (55, 0.08%) found in this study is comparable to earlier studies, but the Positive Predictive Values (PPV)-96% for trisomy 21, 98% for trisomy 18, and 53% for trisomy 13-were higher than expected. Findings other than trisomy 21, 18, or 13 were reported on request of the pregnant women; 78% of women chose to have these reported. The number of additional findings was 207 (0.36%); these included other trisomies (101, 0.18%, PPV 6%, many of the remaining 94% of cases are likely confined placental mosaics and possibly clinically significant), structural chromosomal aberrations (95, 0.16%, PPV 32%,) and complex abnormal profiles indicative of maternal malignancies (11, 0.02%, PPV 64%). The implementation of genome-wide NIPT is under debate because the benefits of detecting other fetal chromosomal aberrations must be balanced against the risks of discordant positives, parental anxiety, and a potential increase in (invasive) diagnostic procedures. Our first-year data, including clinical data and laboratory follow-up data, will fuel this debate. Furthermore, we describe how NIPT can successfully be embedded into a national screening program with a single chain for prenatal care including counseling, testing, and follow-up., (Copyright © 2019 American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2019

18. Mosaic maternal 10qter deletions are associated with FRA10B expansions and may cause false-positive noninvasive prenatal screening results.

Author

Huijsdens-van Amsterdam K, Straver R, van Maarle MC, Knegt AC, Van Opstal D, Sleutels F, Smeets D, and Sistermans EA

Subjects

Adult, Chromosome Deletion, Chromosomes, Human, Pair 10 genetics, Female, Fetus, Genome, Human genetics, Humans, In Situ Hybridization, Fluorescence, Pregnancy, Sequence Deletion genetics, Trisomy diagnosis, Chromosome Fragile Sites genetics, Genetic Testing standards, Prenatal Diagnosis methods, Trisomy genetics

Abstract

Purpose: Using genome-wide noninvasive prenatal screening (NIPS), we detected a 20-megabase specific deletion starting at 10q25 in eight pregnancies. The deletion could not be confirmed by invasive testing. Since all 10(q25→qter) deletions started close to the FRA10B fragile site in 10q25, we investigated whether the pregnant women were indeed carriers of FRA10B., Methods: We performed NIPS analysis for all autosomes using single-read sequencing. Analysis was done with the WISECONDOR algorithm. Culture of blood lymphocytes with bromodeoxyuridine was used to detect FRA10B expansions. Fluorescence in situ hybridization and array analysis were used to find maternal and/or fetal deletions., Results: We confirmed the presence of a FRA10B expansion in all four tested mothers. Fluorescence in situ hybridization and array analysis confirmed the presence of a maternal mosaic deletion of 10(q25→qter)., Conclusion: The recurring 10(q25→qter) deletion detected with NIPS is a false-positive result caused by a maternal low-level mosaic deletion associated with FRA10B expansions. This has important consequences for clinical follow-up, as invasive procedures are unnecessary. Expanded maternal FRA10B repeats should be added to the growing group of variants in the maternal genome that may cause false-positive NIPS results.

Published

2018

19. Origin and clinical relevance of chromosomal aberrations other than the common trisomies detected by genome-wide NIPS: results of the TRIDENT study.

Author

Van Opstal D, van Maarle MC, Lichtenbelt K, Weiss MM, Schuring-Blom H, Bhola SL, Hoffer MJV, Huijsdens-van Amsterdam K, Macville MV, Kooper AJA, Faas BHW, Govaerts L, Tan-Sindhunata GM, den Hollander N, Feenstra I, Galjaard RH, Oepkes D, Ghesquiere S, Brouwer RWW, Beulen L, Bollen S, Elferink MG, Straver R, Henneman L, Page-Christiaens GC, and Sistermans EA

Subjects

DNA Copy Number Variations, Female, Genomics methods, Humans, Placenta metabolism, Pregnancy, Pregnancy Outcome, Whole Genome Sequencing, Chromosome Aberrations, Chromosome Disorders diagnosis, Chromosome Disorders genetics, Genetic Testing methods, Prenatal Diagnosis methods, Trisomy

Abstract

PurposeNoninvasive prenatal screening (NIPS) using cell-free DNA in maternal blood is highly sensitive for detecting fetal trisomies 21, 18, and 13. Using a genome-wide approach, other chromosome anomalies can also be detected. We report on the origin, frequency, and clinical significance of these other chromosome aberrations found in pregnancies at risk for trisomy 21, 18, or 13.MethodsWhole-genome shallow massively parallel sequencing was used and all autosomes were analyzed.ResultsIn 78 of 2,527 cases (3.1%) NIPS was indicative of trisomy 21, 18, or 13, and in 41 (1.6%) of other chromosome aberrations. The latter were of fetal (n = 10), placental (n = 22), maternal (n = 1) or unknown (n = 7). One case lacked cytogenetic follow-up. Nine of the 10 fetal cases were associated with an abnormal phenotype. Thirteen of the 22 (59%) placental aberrations were associated with fetal congenital anomalies and/or poor fetal growth (

Published

2018

20. An inactivating mutation in the histone deacetylase SIRT6 causes human perinatal lethality.

Author

Ferrer CM, Alders M, Postma AV, Park S, Klein MA, Cetinbas M, Pajkrt E, Glas A, van Koningsbruggen S, Christoffels VM, Mannens MMAM, Knegt L, Etchegaray JP, Sadreyev RI, Denu JM, Mostoslavsky G, van Maarle MC, and Mostoslavsky R

Subjects

Animals, Cell Differentiation genetics, Embryoid Bodies, Embryonic Stem Cells, Fetal Death, Gene Expression genetics, Humans, Mice, Myocytes, Cardiac cytology, Myocytes, Cardiac metabolism, Pluripotent Stem Cells cytology, Pluripotent Stem Cells metabolism, Mutation genetics, Sirtuins genetics

Abstract

It has been well established that histone and DNA modifications are critical to maintaining the equilibrium between pluripotency and differentiation during early embryogenesis. Mutations in key regulators of DNA methylation have shown that the balance between gene regulation and function is critical during neural development in early years of life. However, there have been no identified cases linking epigenetic regulators to aberrant human development and fetal demise. Here, we demonstrate that a homozygous inactivating mutation in the histone deacetylase SIRT6 results in severe congenital anomalies and perinatal lethality in four affected fetuses. In vitro, the amino acid change at Asp63 to a histidine results in virtually complete loss of H3K9 deacetylase and demyristoylase functions. Functionally, SIRT6 D63H mouse embryonic stem cells (mESCs) fail to repress pluripotent gene expression, direct targets of SIRT6, and exhibit an even more severe phenotype than Sirt6-deficient ESCs when differentiated into embryoid bodies (EBs). When terminally differentiated toward cardiomyocyte lineage, D63H mutant mESCs maintain expression of pluripotent genes and fail to form functional cardiomyocyte foci. Last, human induced pluripotent stem cells (iPSCs) derived from D63H homozygous fetuses fail to differentiate into EBs, functional cardiomyocytes, and neural progenitor cells due to a failure to repress pluripotent genes. Altogether, our study described a germline mutation in SIRT6 as a cause for fetal demise, defining SIRT6 as a key factor in human development and identifying the first mutation in a chromatin factor behind a human syndrome of perinatal lethality., (© 2018 Ferrer et al.; Published by Cold Spring Harbor Laboratory Press.)

Published

2018

21. Preconception carrier screening for multiple disorders: evaluation of a screening offer in a Dutch founder population.

Author

Mathijssen IB, Holtkamp KCA, Ottenheim CPE, van Eeten-Nijman JMC, Lakeman P, Meijers-Heijboer H, van Maarle MC, and Henneman L

Subjects

Adult, Awareness, Female, Founder Effect, Humans, Male, Genetic Counseling psychology, Genetic Testing, Health Knowledge, Attitudes, Practice, Heterozygote, Population genetics, Preconception Care

Abstract

Technological developments have enabled carrier screening for multiple disorders. This study evaluated experiences with a preconception carrier screening offer for four recessive disorders in a Dutch founder population. Questionnaires were completed by 182 attendees pretesting and posttesting and by 137 non-attendees. Semistructured interviews were conducted with seven of the eight carrier couples. Attendees were mainly informed about the existence of screening by friends/colleagues (49%) and family members (44%). Familiarity with the genetic disorders was high. Knowledge after counseling increased (p < 0.001); however, still 9%, compared to 29% before counseling, wrongly mentioned an increased risk of having an affected child if both parents are carriers of different disorders. Most attendees (97%) recalled their test results correctly, but two couples reported being carrier of another disorder than reported. Overall, 63% felt worried while waiting for results but anxiety levels returned to normal afterwards. In all, 2/39 (5%) carriers felt less healthy. Screened individuals were very satisfied; they did not regret testing (97%) and would recommend testing to others (97%). The majority (94%) stated that couples should always have a pretest consultation, preferably by a genetic counselor rather than their general practitioner (83%). All carrier couples made reproductive decisions based on their results. Main reason for non-attendance was unawareness of the screening offer. With expanded carrier screening, adequately informing couples pretest and posttesting is of foremost importance. Close influencers (family/friends) can be used to raise awareness of a screening offer. Our findings provide lessons for the implementation of expanded carrier screening panels in other communities and other settings.

Published

2018

22. Women's Experience with Non-Invasive Prenatal Testing and Emotional Well-being and Satisfaction after Test-Results.

Author

van Schendel RV, Page-Christiaens GCML, Beulen L, Bilardo CM, de Boer MA, Coumans ABC, Faas BHW, van Langen IM, Lichtenbelt KD, van Maarle MC, Macville MVE, Oepkes D, Pajkrt E, and Henneman L

Subjects

Adult, Anxiety psychology, Down Syndrome diagnosis, Female, Health Literacy, Humans, Pregnancy, Pregnancy Trimester, First psychology, Prenatal Diagnosis methods, Surveys and Questionnaires, Patient Acceptance of Health Care psychology, Personal Satisfaction, Prenatal Diagnosis psychology

Abstract

Increasingly, high-risk pregnant women opt for non-invasive prenatal testing (NIPT) instead of invasive diagnostic testing. Since NIPT is less accurate than invasive testing, a normal NIPT result might leave women less reassured. A questionnaire study was performed among pregnant women with elevated risk for fetal aneuploidy based on first-trimester combined test (risk ≥1:200) or medical history, who were offered NIPT in the nationwide Dutch TRIDENT study. Pre- and post-test questionnaires (n = 682) included measures on: experiences with NIPT procedure, feelings of reassurance, anxiety (State-Trait Anxiety Inventory, STAI), child-related anxiety (PRAQ-R), and satisfaction. The majority (96.1%) were glad to have been offered NIPT. Most (68.5%) perceived the waiting time for NIPT results (mean: 15 days, range 5-32) as (much) too long. Most women with a normal NIPT result felt reassured (80.9%) or somewhat reassured (15.7%). Levels of anxiety and child-related anxiety were significantly lower after receiving a normal NIPT result as compared to the moment of intake (p < 0.001). Women with inadequate health literacy or a medical history (e.g. previous child with trisomy) experienced significantly higher post-test-result anxiety (Mean (M) STAI = 31.6 and 30.0, respectively) compared to those with adequate health literacy (M = 28.6) and no medical history (M = 28.6), indicating these women might benefit from extra information and/or guidance when communicating NIPT test-results. Introducing NIPT as an alternative to invasive testing, led to an offer that satisfied and largely reassured high-risk pregnant women.

Published

2017

23. With expanded carrier screening, founder populations run the risk of being overlooked.

Author

Mathijssen IB, van Maarle MC, Kleiss IIM, Redeker EJW, Ten Kate LP, Henneman L, and Meijers-Heijboer H

Abstract

Genetically isolated populations exist worldwide. Specific genetic disorders, including rare autosomal recessive disorders may have high prevalences in these populations. We searched for Dutch genetically isolated populations and their autosomal recessive founder mutations. We investigated whether these founder mutations are covered in the (preconception) expanded carrier screening tests of five carrier screening providers. Our results show that the great majority of founder mutations are not covered in these screening panels, and these panels may thus not be appropriate for use in founder populations. It is therefore important to be aware of founder mutations in a population when offering carrier tests.

Published

2017

24. Factors for successful implementation of population-based expanded carrier screening: learning from existing initiatives.

Author

Holtkamp KCA, Mathijssen IB, Lakeman P, van Maarle MC, Dondorp WJ, Henneman L, and Cornel MC

Subjects

Adolescent, Adult, Female, Humans, Jews genetics, Male, Netherlands, Young Adult, Genetic Testing methods, Heterozygote, Mass Screening methods

Abstract

Background: Carrier screening for autosomal recessive disorders aims to facilitate reproductive decision-making by identifying couples with a 1-in-4 risk in every pregnancy of having an affected child. Except for a few countries or regions, carrier screening is not widely offered and is mostly ancestry-based. Technological advances enable carrier screening for multiple diseases simultaneously allowing universal screening regardless of ancestry (population-based expanded carrier screening). It is important to study how this can be successfully implemented. This study therefore aims to identify critical factors involved in successful implementation, from a user perspective, by learning from already implemented initiatives., Methods: Factors associated with successful implementation were identified by: (i) a literature review and (ii) two case studies; studying experiences with carrier screening in two high-risk communities (a Dutch founder population and the Ashkenazi Jewish population), including a survey among community members., Results: Factors identified were familiarity with (specific) genetic diseases and its availability, high perceived benefits of screening (e.g. screening avoids much suffering), acceptance of reproductive options, perceived risk of being a carrier and low perceived social barriers (e.g. stigmatization). In contrast to the Jewish community, the initial demand for screening in the Dutch founder population did not entirely come from the community itself. However, the large social cohesion of the community facilitated the implementation process., Conclusion: To ensure successful implementation of population-based expanded carrier screening, efforts should be made to increase knowledge about genetic diseases, create awareness and address personal benefits of screening in a non-directive way., (© The Author 2016. Published by Oxford University Press on behalf of the European Public Health Association.)

Published

2017

25. Trial by Dutch laboratories for evaluation of non-invasive prenatal testing. Part II-women's perspectives.

Author

van Schendel RV, Page-Christiaens GC, Beulen L, Bilardo CM, de Boer MA, Coumans AB, Faas BH, van Langen IM, Lichtenbelt KD, van Maarle MC, Macville MV, Oepkes D, Pajkrt E, and Henneman L

Subjects

Adult, Chromosomes, Human, Pair 13, Chromosomes, Human, Pair 18, Down Syndrome diagnosis, Educational Status, False Positive Reactions, Female, Follow-Up Studies, Humans, Middle Aged, Netherlands, Pregnancy, Pregnancy Trimester, First, Surveys and Questionnaires, Time Factors, Trisomy diagnosis, Trisomy 13 Syndrome, Trisomy 18 Syndrome, Young Adult, Anxiety psychology, Attitude to Health, Chromosome Disorders diagnosis, Conflict, Psychological, DNA blood, Decision Making, Health Literacy, Sequence Analysis, DNA methods

Abstract

Objective: To evaluate preferences and decision-making among high-risk pregnant women offered a choice between Non-Invasive Prenatal Testing (NIPT), invasive testing or no further testing., Methods: Nationwide implementation study (TRIDENT) offering NIPT as contingent screening test for women at increased risk for fetal aneuploidy based on first-trimester combined testing (>1:200) or medical history. A questionnaire was completed after counseling assessing knowledge, attitudes and participation following the Multidimensional Measure of Informed Choice., Results: A total of 1091/1253 (87%) women completed the questionnaire. Of these, 1053 (96.5%) underwent NIPT, 37 (3.4%) invasive testing and 1 (0.1%) declined testing. 91.7% preferred NIPT because of test safety. Overall, 77.9% made an informed choice, 89.8% had sufficient knowledge and 90.5% had positive attitudes towards NIPT. Women with intermediate (odds ratio (OR) = 3.51[1.70-7.22], p < 0.001) or high educational level (OR = 4.36[2.22-8.54], p < 0.001) and women with adequate health literacy (OR = 2.60[1.36-4.95], p = 0.004) were more likely to make an informed choice. Informed choice was associated with less decisional conflict and less anxiety (p < 0.001). Intention to terminate the pregnancy for Down syndrome was higher among women undergoing invasive testing (86.5%) compared to those undergoing NIPT (58.4%) (p < 0.001)., Conclusions: The majority of women had sufficient knowledge and made an informed choice. Continuous attention for counseling is required, especially for low-educated and less health-literate women. © 2016 The Authors. Prenatal Diagnosis published by John Wiley & Sons, Ltd., (© 2016 The Authors. Prenatal Diagnosis published by John Wiley & Sons, Ltd.)

Published

2016

26. Do people from the Jewish community prefer ancestry-based or pan-ethnic expanded carrier screening?

Author

Holtkamp KC, van Maarle MC, Schouten MJ, Dondorp WJ, Lakeman P, and Henneman L

Subjects

Adolescent, Adult, Aged, Female, Founder Effect, Genetic Carrier Screening, Genetic Diseases, Inborn epidemiology, Genetic Predisposition to Disease, Humans, Male, Middle Aged, Netherlands, Pregnancy, Prenatal Diagnosis, Surveys and Questionnaires, Genetic Diseases, Inborn genetics, Genetic Testing, Heterozygote, Jews genetics

Abstract

Ancestry-based carrier screening in the Ashkenazi Jewish population entails screening for specific autosomal recessive founder mutations, which are rarer among the general population. As it is now technically feasible to screen for many more diseases, the question arises whether this population prefers a limited ancestry-based offer or a pan-ethnic expanded carrier screening panel that goes beyond the diseases that are frequent in their own population, and is offered regardless of ancestry. An online questionnaire was completed by 145 individuals from the Dutch Jewish community (≥ 18 years) between April and July 2014. In total, 64.8% were aware of the existence of ancestry-based carrier screening, and respondents were generally positive about screening. About half (53.8%) preferred pan-ethnic expanded carrier screening, whereas 42.8% preferred ancestry-based screening. Reasons for preferring pan-ethnic screening included 'everyone has a right to be tested', 'fear of stigmatization when offering ancestry-based panels', and 'difficulties with identifying risk owing to mixed backgrounds'. 'Preventing high healthcare costs' was the most important reason against pan-ethnic carrier screening among those in favor of an ancestry-based panel. In conclusion, these findings show that people from the Dutch Jewish community have a positive attitude regarding carrier screening in their community for a wide range of diseases. As costs of expanded carrier screening panels are most likely to drop in the near future, it is expected that these panels will receive more support in the future.

Published

2016

27. Prenatal Evidence of Persistent Notochord and Absent Sacrum Caused by a Mutation in the T (Brachyury) Gene.

Author

Fontanella F, van Maarle MC, Robles de Medina P, Oostra RJ, van Rijn RR, Pajkrt E, and Bilardo CM

Abstract

Caudal regression syndrome (CRS) is a rare congenital disorder characterized by developmental abnormalities of caudal spinal segments. To date, the etiology of CRS is unclear; sporadic cases are strongly associated with maternal diabetes, while familiar recurrence is infrequent. We describe in detail the prenatal clinical and sonographic findings of a recently described hereditary caudal regression syndrome, in four fetuses reported to be homozygous for a mutation in the T (brachyury) gene. The syndrome occurred in three consanguineous, but unrelated families, originating from the same geographical area. All affected fetuses had persistence of the notochord in association with abnormal vertebral ossification, sacral agenesis, and bilateral clubfoot. These findings suggest that, in case of prenatal diagnosis of sacral agenesis, an advanced ultrasound examination should assess the vertebral ossification and the rare persistence of the notochord, in order to rule the involvement of the T gene., Competing Interests: The authors declare that there is no conflict of interests regarding the publication of this paper.

Published

2016

28. Targeted carrier screening for four recessive disorders: high detection rate within a founder population.

Author

Mathijssen IB, Henneman L, van Eeten-Nijman JM, Lakeman P, Ottenheim CP, Redeker EJ, Ottenhof W, Meijers-Heijboer H, and van Maarle MC

Subjects

Adolescent, Adult, Arthrogryposis diagnosis, Arthrogryposis genetics, Chondrodysplasia Punctata, Rhizomelic diagnosis, Chondrodysplasia Punctata, Rhizomelic genetics, Female, Founder Effect, Genetic Counseling, Humans, Male, Middle Aged, Netherlands, Olivopontocerebellar Atrophies diagnosis, Olivopontocerebellar Atrophies genetics, Osteogenesis Imperfecta diagnosis, Osteogenesis Imperfecta genetics, Pedigree, Peroxisomal Targeting Signal 2 Receptor deficiency, Pregnancy, Young Adult, Genes, Recessive, Genetic Carrier Screening methods, Genetic Testing methods

Abstract

In a genetically isolated community in the Netherlands four severe recessive genetic disorders occur at relatively high frequency (pontocerebellar hypoplasia type 2 (PCH2), fetal akinesia deformation sequence (FADS), rhizomelic chondrodysplasia punctata type 1 (RCDP1), and osteogenesis imperfecta (OI) type IIB/III. Over the past decades multiple patients with these disorders have been identified. This warranted the start of a preconception outpatient clinic, in 2012, aimed at couples planning a pregnancy. The aim of our study was to evaluate the offer of targeted genetic carrier screening as a method to identify high-risk couples for having affected offspring in this high-risk subpopulation. In one year, 203 individuals (92 couples and 19 individuals) were counseled. In total, 65 of 196 (33.2%) tested individuals were carriers of at least one disease, five (7.7%) of them being carriers of two diseases. Carrier frequencies of PCH2, FADS, RCDP1, and OI were 14.3%, 11.2%, 6.1%, and 4.1% respectively. In individuals with a positive family history for one of the diseases, the carrier frequency was 57.8%; for those with a negative family history this was 25.8%. Four PCH2 carrier-couples were identified. Thus, targeted (preconception) carrier screening in this genetically isolated population in which a high prevalence of specific disorders occurs detects a high number of carriers, and is likely to be more effective compared to cascade genetic testing. Our findings and set-up can be seen as a model for carrier screening in other high-risk subpopulations and contributes to the discussion about the way carrier screening can be offered and organized in the general population., (Copyright © 2015 Elsevier Masson SAS. All rights reserved.)

Published

2015