Prenatal diagnostic testing of the Noonan syndrome genes in fetuses with abnormal ultrasound findings

Ellen A. Croonen; Willy M. Nillesen; Kyra E. Stuurman; Gretel Oudesluijs; Ingrid M. B. M. van de Laar; Liesbeth Martens; Charlotte Ockeloen; Inge B. Mathijssen; Marga Schepens; Martina Ruiterkamp-Versteeg; Hans Scheffer; Brigitte H. W. Faas; Ineke van der Burgt; Helger G. Yntema

doi:https://doi.org/10.1038/ejhg.2012.285

Prenatal diagnostic testing of the Noonan syndrome genes in fetuses with abnormal ultrasound findings

Ellen A. Croonen, Willy M. Nillesen, Kyra E. Stuurman, Gretel Oudesluijs, Ingrid M. B. M. van de Laar, Liesbeth Martens, Charlotte Ockeloen, Inge B. Mathijssen, Marga Schepens, Martina Ruiterkamp-Versteeg, Hans Scheffer, Brigitte H. W. Faas, Ineke van der Burgt, Helger G. Yntema

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Abstract

In recent studies on prenatal testing for Noonan syndrome (NS) in fetuses with an increased nuchal translucency (NT) and a normal karyotype, mutations have been reported in 9-16% of cases. In this study, DNA of 75 fetuses with a normal karyotype and abnormal ultrasound findings was tested in a diagnostic setting for mutations in (a subset of) the four most commonly mutated NS genes. A de novo mutation in either PTPN11, KRAS or RAF1 was detected in 13 fetuses (17.3%). Ultrasound findings were increased NT, distended jugular lymphatic sacs (JLS), hydrothorax, renal anomalies, polyhydramnios, cystic hygroma, cardiac anomalies, hydrops fetalis and ascites. A second group, consisting of anonymized DNA of 60 other fetuses with sonographic abnormalities, was tested for mutations in 10 NS genes. In this group, five possible pathogenic mutations have been identified (in PTPN11 (n=2), RAF1, BRAF and MAP2K1 (each n=1)). We recommend prenatal testing of PTPN11, KRAS and RAF1 in pregnancies with an increased NT and at least one of the following additional features: polyhydramnios, hydrops fetalis, renal anomalies, distended JLS, hydrothorax, cardiac anomalies, cystic hygroma and ascites. If possible, mutation analysis of BRAF and MAP2K1 should be considered

Original language	English
Pages (from-to)	936-942
Journal	European journal of human genetics
Volume	21
Issue number	9
DOIs	https://doi.org/10.1038/ejhg.2012.285
Publication status	Published - 2013

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Croonen, E. A., Nillesen, W. M., Stuurman, K. E., Oudesluijs, G., van de Laar, I. M. B. M., Martens, L., Ockeloen, C., Mathijssen, I. B., Schepens, M., Ruiterkamp-Versteeg, M., Scheffer, H., Faas, B. H. W., van der Burgt, I., & Yntema, H. G. (2013). Prenatal diagnostic testing of the Noonan syndrome genes in fetuses with abnormal ultrasound findings. European journal of human genetics, 21(9), 936-942. https://doi.org/10.1038/ejhg.2012.285

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title = "Prenatal diagnostic testing of the Noonan syndrome genes in fetuses with abnormal ultrasound findings",

abstract = "In recent studies on prenatal testing for Noonan syndrome (NS) in fetuses with an increased nuchal translucency (NT) and a normal karyotype, mutations have been reported in 9-16% of cases. In this study, DNA of 75 fetuses with a normal karyotype and abnormal ultrasound findings was tested in a diagnostic setting for mutations in (a subset of) the four most commonly mutated NS genes. A de novo mutation in either PTPN11, KRAS or RAF1 was detected in 13 fetuses (17.3%). Ultrasound findings were increased NT, distended jugular lymphatic sacs (JLS), hydrothorax, renal anomalies, polyhydramnios, cystic hygroma, cardiac anomalies, hydrops fetalis and ascites. A second group, consisting of anonymized DNA of 60 other fetuses with sonographic abnormalities, was tested for mutations in 10 NS genes. In this group, five possible pathogenic mutations have been identified (in PTPN11 (n=2), RAF1, BRAF and MAP2K1 (each n=1)). We recommend prenatal testing of PTPN11, KRAS and RAF1 in pregnancies with an increased NT and at least one of the following additional features: polyhydramnios, hydrops fetalis, renal anomalies, distended JLS, hydrothorax, cardiac anomalies, cystic hygroma and ascites. If possible, mutation analysis of BRAF and MAP2K1 should be considered",

author = "Croonen, {Ellen A.} and Nillesen, {Willy M.} and Stuurman, {Kyra E.} and Gretel Oudesluijs and {van de Laar}, {Ingrid M. B. M.} and Liesbeth Martens and Charlotte Ockeloen and Mathijssen, {Inge B.} and Marga Schepens and Martina Ruiterkamp-Versteeg and Hans Scheffer and Faas, {Brigitte H. W.} and {van der Burgt}, Ineke and Yntema, {Helger G.}",

year = "2013",

doi = "https://doi.org/10.1038/ejhg.2012.285",

language = "English",

volume = "21",

pages = "936--942",

journal = "European journal of human genetics",

issn = "1018-4813",

publisher = "Nature Publishing Group",

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Croonen, EA, Nillesen, WM, Stuurman, KE, Oudesluijs, G, van de Laar, IMBM, Martens, L, Ockeloen, C, Mathijssen, IB, Schepens, M, Ruiterkamp-Versteeg, M, Scheffer, H, Faas, BHW, van der Burgt, I & Yntema, HG 2013, 'Prenatal diagnostic testing of the Noonan syndrome genes in fetuses with abnormal ultrasound findings', European journal of human genetics, vol. 21, no. 9, pp. 936-942. https://doi.org/10.1038/ejhg.2012.285

TY - JOUR

T1 - Prenatal diagnostic testing of the Noonan syndrome genes in fetuses with abnormal ultrasound findings

AU - Croonen, Ellen A.

AU - Nillesen, Willy M.

AU - Stuurman, Kyra E.

AU - Oudesluijs, Gretel

AU - van de Laar, Ingrid M. B. M.

AU - Martens, Liesbeth

AU - Ockeloen, Charlotte

AU - Mathijssen, Inge B.

AU - Schepens, Marga

AU - Ruiterkamp-Versteeg, Martina

AU - Scheffer, Hans

AU - Faas, Brigitte H. W.

AU - van der Burgt, Ineke

AU - Yntema, Helger G.

PY - 2013

Y1 - 2013

N2 - In recent studies on prenatal testing for Noonan syndrome (NS) in fetuses with an increased nuchal translucency (NT) and a normal karyotype, mutations have been reported in 9-16% of cases. In this study, DNA of 75 fetuses with a normal karyotype and abnormal ultrasound findings was tested in a diagnostic setting for mutations in (a subset of) the four most commonly mutated NS genes. A de novo mutation in either PTPN11, KRAS or RAF1 was detected in 13 fetuses (17.3%). Ultrasound findings were increased NT, distended jugular lymphatic sacs (JLS), hydrothorax, renal anomalies, polyhydramnios, cystic hygroma, cardiac anomalies, hydrops fetalis and ascites. A second group, consisting of anonymized DNA of 60 other fetuses with sonographic abnormalities, was tested for mutations in 10 NS genes. In this group, five possible pathogenic mutations have been identified (in PTPN11 (n=2), RAF1, BRAF and MAP2K1 (each n=1)). We recommend prenatal testing of PTPN11, KRAS and RAF1 in pregnancies with an increased NT and at least one of the following additional features: polyhydramnios, hydrops fetalis, renal anomalies, distended JLS, hydrothorax, cardiac anomalies, cystic hygroma and ascites. If possible, mutation analysis of BRAF and MAP2K1 should be considered

AB - In recent studies on prenatal testing for Noonan syndrome (NS) in fetuses with an increased nuchal translucency (NT) and a normal karyotype, mutations have been reported in 9-16% of cases. In this study, DNA of 75 fetuses with a normal karyotype and abnormal ultrasound findings was tested in a diagnostic setting for mutations in (a subset of) the four most commonly mutated NS genes. A de novo mutation in either PTPN11, KRAS or RAF1 was detected in 13 fetuses (17.3%). Ultrasound findings were increased NT, distended jugular lymphatic sacs (JLS), hydrothorax, renal anomalies, polyhydramnios, cystic hygroma, cardiac anomalies, hydrops fetalis and ascites. A second group, consisting of anonymized DNA of 60 other fetuses with sonographic abnormalities, was tested for mutations in 10 NS genes. In this group, five possible pathogenic mutations have been identified (in PTPN11 (n=2), RAF1, BRAF and MAP2K1 (each n=1)). We recommend prenatal testing of PTPN11, KRAS and RAF1 in pregnancies with an increased NT and at least one of the following additional features: polyhydramnios, hydrops fetalis, renal anomalies, distended JLS, hydrothorax, cardiac anomalies, cystic hygroma and ascites. If possible, mutation analysis of BRAF and MAP2K1 should be considered

U2 - https://doi.org/10.1038/ejhg.2012.285

DO - https://doi.org/10.1038/ejhg.2012.285

M3 - Article

C2 - 23321623

SN - 1018-4813

VL - 21

SP - 936

EP - 942

JO - European journal of human genetics

JF - European journal of human genetics

IS - 9

ER -