Range of genetic mutations associated with severe non-syndromic sporadic intellectual disability: An exome sequencing study

Anita Rauch; Dagmar Wieczorek; Elisabeth Graf; Thomas Wieland; Sabine Endele; Thomas Schwarzmayr; Beate Albrecht; Deborah Bartholdi; Jasmin Beygo; Nataliya Di Donato; Andreas Dufke; Kirsten Cremer; Maja Hempel; Denise Horn; Juliane Hoyer; Pascal Joset; Albrecht Röpke; Ute Moog; Angelika Riess; Christian T. Thiel; Andreas Tzschach; Antje Wiesener; Eva Wohlleber; Christiane Zweier; Arif B. Ekici; Alexander M. Zink; Andreas Rump; Christa Meisinger; Harald Grallert; Heinrich Sticht; Annette Schenck; Hartmut Engels; Gudrun Rappold; Evelin Schröck; Peter Wieacker; Olaf Riess; Thomas Meitinger; André Reis; Tim M. Strom

doi:10.1016/S0140-6736(12)61480-9

Range of genetic mutations associated with severe non-syndromic sporadic intellectual disability: An exome sequencing study

Anita Rauch
, Dagmar Wieczorek
, Elisabeth Graf
, Thomas Wieland
, Sabine Endele
, Thomas Schwarzmayr
, Beate Albrecht
, Deborah Bartholdi
, Jasmin Beygo
, Nataliya Di Donato
, Andreas Dufke
, Kirsten Cremer
, Maja Hempel
, Denise Horn
, Juliane Hoyer
, Pascal Joset
, Albrecht Röpke
, Ute Moog
, Angelika Riess
, Christian T. Thiel

Andreas Tzschach, Antje Wiesener, Eva Wohlleber, Christiane Zweier, Arif B. Ekici, Alexander M. Zink, Andreas Rump, Christa Meisinger, Harald Grallert, Heinrich Sticht, Annette Schenck, Hartmut Engels, Gudrun Rappold, Evelin Schröck, Peter Wieacker, Olaf Riess, Thomas Meitinger, André Reis, Tim M. Strom

Medicine and Health

University of Zurich
Friedrich Alexander Universität Erlangen-Nürnberg
University Hospital of Essen
Helmholtz Zentrum München German Research Center for Environmental Health
Technische Universität Dresden
University of Tübingen
Technische Universität München
Charité – Universitätsmedizin Berlin
University of Münster
Heidelberg University
University of Bonn
Radboud University Nijmegen Medical Centre Nijmegen

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

873 Zitate (Scopus)

Abstract

Background The genetic cause of intellectual disability in most patients is unclear because of the absence of morphological clues, information about the position of such genes, and suitable screening methods. Our aim was to identify de-novo variants in individuals with sporadic non-syndromic intellectual disability. Methods In this study, we enrolled children with intellectual disability and their parents from ten centres in Germany and Switzerland. We compared exome sequences between patients and their parents to identify de-novo variants. 20 children and their parents from the KORA Augsburg Diabetes Family Study were investigated as controls. Findings We enrolled 51 participants from the German Mental Retardation Network. 45 (88%) participants in the case group and 14 (70%) in the control group had de-novo variants. We identifi ed 87 de-novo variants in the case group, with an exomic mutation rate of 1•71 per individual per generation. In the control group we identifi ed 24 de-novo variants, which is 1•2 events per individual per generation. More participants in the case group had loss-of-function variants than in the control group (20/51 vs 2/20; p=0•022), suggesting their contribution to disease development. 16 patients carried de-novo variants in known intellectual disability genes with three recurrently mutated genes (STXBP1, SYNGAP1, and SCN2A). We deemed at least six loss-of-function mutations in six novel genes to be disease causing. We also identifi ed several missense alterations with potential pathogenicity. Interpretation After exclusion of copy-number variants, de-novo point mutations and small indels are associated with severe, sporadic non-syndromic intellectual disability, accounting for 45-55% of patients with high locus heterogeneity. Autosomal recessive inheritance seems to contribute little in the outbred population investigated. The large number of de-novo variants in known intellectual disability genes is only partially attributable to known non-specifi c phenotypes. Several patients did not meet the expected syndromic manifestation, suggesting a strong bias in present clinical syndrome descriptions. Funding German Ministry of Education and Research, European Commission 7th Framework Program, and Swiss National Science Foundation.

Originalsprache	Englisch
Seiten (von - bis)	1674-1682
Seitenumfang	9
Fachzeitschrift	The Lancet
Jahrgang	380
Ausgabenummer	9854
DOIs	https://doi.org/10.1016/S0140-6736(12)61480-9
Publikationsstatus	Veröffentlicht - Nov. 2012

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Dieser Output leistet einen Beitrag zu folgendem(n) Ziel(en) für nachhaltige Entwicklung

SDG 3 – Gute Gesundheit und Wohlergehen

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10.1016/S0140-6736(12)61480-9

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Rauch, A., Wieczorek, D., Graf, E., Wieland, T., Endele, S., Schwarzmayr, T., Albrecht, B., Bartholdi, D., Beygo, J., Di Donato, N., Dufke, A., Cremer, K., Hempel, M., Horn, D., Hoyer, J., Joset, P., Röpke, A., Moog, U., Riess, A., ... Strom, T. M. (2012). Range of genetic mutations associated with severe non-syndromic sporadic intellectual disability: An exome sequencing study. The Lancet, 380(9854), 1674-1682. https://doi.org/10.1016/S0140-6736(12)61480-9

@article{3fa77cedc09c4e64bb929567f085d20a,

title = "Range of genetic mutations associated with severe non-syndromic sporadic intellectual disability: An exome sequencing study",

abstract = "Background The genetic cause of intellectual disability in most patients is unclear because of the absence of morphological clues, information about the position of such genes, and suitable screening methods. Our aim was to identify de-novo variants in individuals with sporadic non-syndromic intellectual disability. Methods In this study, we enrolled children with intellectual disability and their parents from ten centres in Germany and Switzerland. We compared exome sequences between patients and their parents to identify de-novo variants. 20 children and their parents from the KORA Augsburg Diabetes Family Study were investigated as controls. Findings We enrolled 51 participants from the German Mental Retardation Network. 45 (88\%) participants in the case group and 14 (70\%) in the control group had de-novo variants. We identifi ed 87 de-novo variants in the case group, with an exomic mutation rate of 1•71 per individual per generation. In the control group we identifi ed 24 de-novo variants, which is 1•2 events per individual per generation. More participants in the case group had loss-of-function variants than in the control group (20/51 vs 2/20; p=0•022), suggesting their contribution to disease development. 16 patients carried de-novo variants in known intellectual disability genes with three recurrently mutated genes (STXBP1, SYNGAP1, and SCN2A). We deemed at least six loss-of-function mutations in six novel genes to be disease causing. We also identifi ed several missense alterations with potential pathogenicity. Interpretation After exclusion of copy-number variants, de-novo point mutations and small indels are associated with severe, sporadic non-syndromic intellectual disability, accounting for 45-55\% of patients with high locus heterogeneity. Autosomal recessive inheritance seems to contribute little in the outbred population investigated. The large number of de-novo variants in known intellectual disability genes is only partially attributable to known non-specifi c phenotypes. Several patients did not meet the expected syndromic manifestation, suggesting a strong bias in present clinical syndrome descriptions. Funding German Ministry of Education and Research, European Commission 7th Framework Program, and Swiss National Science Foundation.",

author = "Anita Rauch and Dagmar Wieczorek and Elisabeth Graf and Thomas Wieland and Sabine Endele and Thomas Schwarzmayr and Beate Albrecht and Deborah Bartholdi and Jasmin Beygo and \{Di Donato\}, Nataliya and Andreas Dufke and Kirsten Cremer and Maja Hempel and Denise Horn and Juliane Hoyer and Pascal Joset and Albrecht R{\"o}pke and Ute Moog and Angelika Riess and Thiel, \{Christian T.\} and Andreas Tzschach and Antje Wiesener and Eva Wohlleber and Christiane Zweier and Ekici, \{Arif B.\} and Zink, \{Alexander M.\} and Andreas Rump and Christa Meisinger and Harald Grallert and Heinrich Sticht and Annette Schenck and Hartmut Engels and Gudrun Rappold and Evelin Schr{\"o}ck and Peter Wieacker and Olaf Riess and Thomas Meitinger and Andr{\'e} Reis and Strom, \{Tim M.\}",

note = "Funding Information: We thank all patients and their families for participating in this study. This work was supported by the German Ministry of Education and Research ( 01GS08160, 01GR0802, and 01GM0867 ), the European Commission 7th Framework Program ( 261123, GEUVADIS ), and the Swiss National Science Foundation ( 320030\_135669 ). ",

year = "2012",

month = nov,

doi = "10.1016/S0140-6736(12)61480-9",

language = "English",

volume = "380",

pages = "1674--1682",

journal = "The Lancet",

issn = "0140-6736",

publisher = "Elsevier B.V.",

number = "9854",

}

Rauch, A, Wieczorek, D, Graf, E, Wieland, T, Endele, S, Schwarzmayr, T, Albrecht, B, Bartholdi, D, Beygo, J, Di Donato, N, Dufke, A, Cremer, K, Hempel, M, Horn, D, Hoyer, J, Joset, P, Röpke, A, Moog, U, Riess, A, Thiel, CT, Tzschach, A, Wiesener, A, Wohlleber, E, Zweier, C, Ekici, AB, Zink, AM, Rump, A, Meisinger, C, Grallert, H, Sticht, H, Schenck, A, Engels, H, Rappold, G, Schröck, E, Wieacker, P, Riess, O, Meitinger, T, Reis, A & Strom, TM 2012, 'Range of genetic mutations associated with severe non-syndromic sporadic intellectual disability: An exome sequencing study', The Lancet, Jg. 380, Nr. 9854, S. 1674-1682. https://doi.org/10.1016/S0140-6736(12)61480-9

TY - JOUR

T1 - Range of genetic mutations associated with severe non-syndromic sporadic intellectual disability

T2 - An exome sequencing study

AU - Rauch, Anita

AU - Wieczorek, Dagmar

AU - Graf, Elisabeth

AU - Wieland, Thomas

AU - Endele, Sabine

AU - Schwarzmayr, Thomas

AU - Albrecht, Beate

AU - Bartholdi, Deborah

AU - Beygo, Jasmin

AU - Di Donato, Nataliya

AU - Dufke, Andreas

AU - Cremer, Kirsten

AU - Hempel, Maja

AU - Horn, Denise

AU - Hoyer, Juliane

AU - Joset, Pascal

AU - Röpke, Albrecht

AU - Moog, Ute

AU - Riess, Angelika

AU - Thiel, Christian T.

AU - Tzschach, Andreas

AU - Wiesener, Antje

AU - Wohlleber, Eva

AU - Zweier, Christiane

AU - Ekici, Arif B.

AU - Zink, Alexander M.

AU - Rump, Andreas

AU - Meisinger, Christa

AU - Grallert, Harald

AU - Sticht, Heinrich

AU - Schenck, Annette

AU - Engels, Hartmut

AU - Rappold, Gudrun

AU - Schröck, Evelin

AU - Wieacker, Peter

AU - Riess, Olaf

AU - Meitinger, Thomas

AU - Reis, André

AU - Strom, Tim M.

N1 - Funding Information: We thank all patients and their families for participating in this study. This work was supported by the German Ministry of Education and Research ( 01GS08160, 01GR0802, and 01GM0867 ), the European Commission 7th Framework Program ( 261123, GEUVADIS ), and the Swiss National Science Foundation ( 320030_135669 ).

PY - 2012/11

Y1 - 2012/11

N2 - Background The genetic cause of intellectual disability in most patients is unclear because of the absence of morphological clues, information about the position of such genes, and suitable screening methods. Our aim was to identify de-novo variants in individuals with sporadic non-syndromic intellectual disability. Methods In this study, we enrolled children with intellectual disability and their parents from ten centres in Germany and Switzerland. We compared exome sequences between patients and their parents to identify de-novo variants. 20 children and their parents from the KORA Augsburg Diabetes Family Study were investigated as controls. Findings We enrolled 51 participants from the German Mental Retardation Network. 45 (88%) participants in the case group and 14 (70%) in the control group had de-novo variants. We identifi ed 87 de-novo variants in the case group, with an exomic mutation rate of 1•71 per individual per generation. In the control group we identifi ed 24 de-novo variants, which is 1•2 events per individual per generation. More participants in the case group had loss-of-function variants than in the control group (20/51 vs 2/20; p=0•022), suggesting their contribution to disease development. 16 patients carried de-novo variants in known intellectual disability genes with three recurrently mutated genes (STXBP1, SYNGAP1, and SCN2A). We deemed at least six loss-of-function mutations in six novel genes to be disease causing. We also identifi ed several missense alterations with potential pathogenicity. Interpretation After exclusion of copy-number variants, de-novo point mutations and small indels are associated with severe, sporadic non-syndromic intellectual disability, accounting for 45-55% of patients with high locus heterogeneity. Autosomal recessive inheritance seems to contribute little in the outbred population investigated. The large number of de-novo variants in known intellectual disability genes is only partially attributable to known non-specifi c phenotypes. Several patients did not meet the expected syndromic manifestation, suggesting a strong bias in present clinical syndrome descriptions. Funding German Ministry of Education and Research, European Commission 7th Framework Program, and Swiss National Science Foundation.

AB - Background The genetic cause of intellectual disability in most patients is unclear because of the absence of morphological clues, information about the position of such genes, and suitable screening methods. Our aim was to identify de-novo variants in individuals with sporadic non-syndromic intellectual disability. Methods In this study, we enrolled children with intellectual disability and their parents from ten centres in Germany and Switzerland. We compared exome sequences between patients and their parents to identify de-novo variants. 20 children and their parents from the KORA Augsburg Diabetes Family Study were investigated as controls. Findings We enrolled 51 participants from the German Mental Retardation Network. 45 (88%) participants in the case group and 14 (70%) in the control group had de-novo variants. We identifi ed 87 de-novo variants in the case group, with an exomic mutation rate of 1•71 per individual per generation. In the control group we identifi ed 24 de-novo variants, which is 1•2 events per individual per generation. More participants in the case group had loss-of-function variants than in the control group (20/51 vs 2/20; p=0•022), suggesting their contribution to disease development. 16 patients carried de-novo variants in known intellectual disability genes with three recurrently mutated genes (STXBP1, SYNGAP1, and SCN2A). We deemed at least six loss-of-function mutations in six novel genes to be disease causing. We also identifi ed several missense alterations with potential pathogenicity. Interpretation After exclusion of copy-number variants, de-novo point mutations and small indels are associated with severe, sporadic non-syndromic intellectual disability, accounting for 45-55% of patients with high locus heterogeneity. Autosomal recessive inheritance seems to contribute little in the outbred population investigated. The large number of de-novo variants in known intellectual disability genes is only partially attributable to known non-specifi c phenotypes. Several patients did not meet the expected syndromic manifestation, suggesting a strong bias in present clinical syndrome descriptions. Funding German Ministry of Education and Research, European Commission 7th Framework Program, and Swiss National Science Foundation.

UR - https://www.scopus.com/pages/publications/84868543309

U2 - 10.1016/S0140-6736(12)61480-9

DO - 10.1016/S0140-6736(12)61480-9

M3 - Article

C2 - 23020937

AN - SCOPUS:84868543309

SN - 0140-6736

VL - 380

SP - 1674

EP - 1682

JO - The Lancet

JF - The Lancet

IS - 9854

ER -

Range of genetic mutations associated with severe non-syndromic sporadic intellectual disability: An exome sequencing study

Abstract

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