Disruption of the methyltransferase-like 23 gene METTL23 causes mild autosomal recessive intellectual disability

Marie Bernkopf; Gerald Webersinke; Chanakan Tongsook; Chintan N. Koyani; Muhammed Arshad; Muhammed Ayaz; Doris Müller; Christian Enzinger; Muhammed Aslam; Farooq Naeem; Kurt Schmidt; Karl Gruber; Michael R. Speicher; Ernst Malle; Peter Macheroux; Muhammed Ayub; John B. Vincent; Christian Windpassinger; Hans-Christoph Duba

doi:10.1093/hmg/ddu115

Disruption of the methyltransferase-like 23 gene METTL23 causes mild autosomal recessive intellectual disability

Marie Bernkopf, Gerald Webersinke, Chanakan Tongsook, Chintan N. Koyani, Muhammed Arshad, Muhammed Ayaz, Doris Müller, Christian Enzinger, Muhammed Aslam, Farooq Naeem, Kurt Schmidt, Karl Gruber, Michael R. Speicher, Ernst Malle, Peter Macheroux, Muhammed Ayub, John B. Vincent, Christian Windpassinger^*, Hans-Christoph Duba

^*Korrespondierende/r Autor/-in für diese Arbeit

Institut für Biochemie (6480)

Publikation: Beitrag in einer Fachzeitschrift › Artikel › Begutachtung

Abstract

We describe the characterization of a gene for mild nonsyndromic autosomal recessive intellectual disability (ID) in two unrelated families, one from Austria, the other from Pakistan. Genome-wide single nucleotide polymorphism microarray analysis enabled us to define a region of homozygosity by descent on chromosome 17q25. Whole-exome sequencing and analysis of this region in an affected individual from the Austrian family identified a 5 bp frameshifting deletion in the METTL23 gene. By means of Sanger sequencing of METTL23, a nonsense mutation was detected in a consanguineous ID family from Pakistan for which homozygosity-by-descent mapping had identified a region on 17q25. Both changes lead to truncation of the putative METTL23 protein, which disrupts the predicted catalytic domain and alters the cellular localization. 3D-modelling of the protein indicates that METTL23 is strongly predicted to function as an S-adenosyl-methionine (SAM)-dependent methyltransferase. Expression analysis of METTL23 indicated a strong association with heat shock proteins, which suggests that these may act as a putative substrate for methylation by METTL23. A number of methyltransferases have been described recently in association with ID. Disruption of METTL23 presented here supports the importance of methylation processes for intact neuronal function and brain development.

Originalsprache	englisch
Seiten (von - bis)	4015-4023
Fachzeitschrift	Human Molecular Genetics
Jahrgang	23
Ausgabenummer	15
DOIs	https://doi.org/10.1093/hmg/ddu115
Publikationsstatus	Veröffentlicht - 2014

Fields of Expertise

Human- & Biotechnology

Treatment code (Nähere Zuordnung)

Basic - Fundamental (Grundlagenforschung)

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10.1093/hmg/ddu115Lizenz: CC BY-NC 3.0

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Bernkopf, M., Webersinke, G., Tongsook, C., Koyani, C. N., Arshad, M., Ayaz, M., Müller, D., Enzinger, C., Aslam, M., Naeem, F., Schmidt, K., Gruber, K., Speicher, M. R., Malle, E., Macheroux, P., Ayub, M., Vincent, J. B., Windpassinger, C., & Duba, H.-C. (2014). Disruption of the methyltransferase-like 23 gene METTL23 causes mild autosomal recessive intellectual disability. Human Molecular Genetics, 23(15), 4015-4023. https://doi.org/10.1093/hmg/ddu115

Bernkopf, M, Webersinke, G, Tongsook, C, Koyani, CN, Arshad, M, Ayaz, M, Müller, D, Enzinger, C, Aslam, M, Naeem, F, Schmidt, K, Gruber, K, Speicher, MR, Malle, E, Macheroux, P, Ayub, M, Vincent, JB, Windpassinger, C & Duba, H-C 2014, 'Disruption of the methyltransferase-like 23 gene METTL23 causes mild autosomal recessive intellectual disability', Human Molecular Genetics, Jg. 23, Nr. 15, S. 4015-4023. https://doi.org/10.1093/hmg/ddu115

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title = "Disruption of the methyltransferase-like 23 gene METTL23 causes mild autosomal recessive intellectual disability",

abstract = "We describe the characterization of a gene for mild nonsyndromic autosomal recessive intellectual disability (ID) in two unrelated families, one from Austria, the other from Pakistan. Genome-wide single nucleotide polymorphism microarray analysis enabled us to define a region of homozygosity by descent on chromosome 17q25. Whole-exome sequencing and analysis of this region in an affected individual from the Austrian family identified a 5 bp frameshifting deletion in the METTL23 gene. By means of Sanger sequencing of METTL23, a nonsense mutation was detected in a consanguineous ID family from Pakistan for which homozygosity-by-descent mapping had identified a region on 17q25. Both changes lead to truncation of the putative METTL23 protein, which disrupts the predicted catalytic domain and alters the cellular localization. 3D-modelling of the protein indicates that METTL23 is strongly predicted to function as an S-adenosyl-methionine (SAM)-dependent methyltransferase. Expression analysis of METTL23 indicated a strong association with heat shock proteins, which suggests that these may act as a putative substrate for methylation by METTL23. A number of methyltransferases have been described recently in association with ID. Disruption of METTL23 presented here supports the importance of methylation processes for intact neuronal function and brain development.",

author = "Marie Bernkopf and Gerald Webersinke and Chanakan Tongsook and Koyani, {Chintan N.} and Muhammed Arshad and Muhammed Ayaz and Doris M{\"u}ller and Christian Enzinger and Muhammed Aslam and Farooq Naeem and Kurt Schmidt and Karl Gruber and Speicher, {Michael R.} and Ernst Malle and Peter Macheroux and Muhammed Ayub and Vincent, {John B.} and Christian Windpassinger and Hans-Christoph Duba",

year = "2014",

doi = "10.1093/hmg/ddu115",

language = "English",

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pages = "4015--4023",

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T1 - Disruption of the methyltransferase-like 23 gene METTL23 causes mild autosomal recessive intellectual disability

AU - Bernkopf, Marie

AU - Webersinke, Gerald

AU - Tongsook, Chanakan

AU - Koyani, Chintan N.

AU - Arshad, Muhammed

AU - Ayaz, Muhammed

AU - Müller, Doris

AU - Enzinger, Christian

AU - Aslam, Muhammed

AU - Naeem, Farooq

AU - Schmidt, Kurt

AU - Gruber, Karl

AU - Speicher, Michael R.

AU - Malle, Ernst

AU - Macheroux, Peter

AU - Ayub, Muhammed

AU - Vincent, John B.

AU - Windpassinger, Christian

AU - Duba, Hans-Christoph

PY - 2014

Y1 - 2014

N2 - We describe the characterization of a gene for mild nonsyndromic autosomal recessive intellectual disability (ID) in two unrelated families, one from Austria, the other from Pakistan. Genome-wide single nucleotide polymorphism microarray analysis enabled us to define a region of homozygosity by descent on chromosome 17q25. Whole-exome sequencing and analysis of this region in an affected individual from the Austrian family identified a 5 bp frameshifting deletion in the METTL23 gene. By means of Sanger sequencing of METTL23, a nonsense mutation was detected in a consanguineous ID family from Pakistan for which homozygosity-by-descent mapping had identified a region on 17q25. Both changes lead to truncation of the putative METTL23 protein, which disrupts the predicted catalytic domain and alters the cellular localization. 3D-modelling of the protein indicates that METTL23 is strongly predicted to function as an S-adenosyl-methionine (SAM)-dependent methyltransferase. Expression analysis of METTL23 indicated a strong association with heat shock proteins, which suggests that these may act as a putative substrate for methylation by METTL23. A number of methyltransferases have been described recently in association with ID. Disruption of METTL23 presented here supports the importance of methylation processes for intact neuronal function and brain development.

AB - We describe the characterization of a gene for mild nonsyndromic autosomal recessive intellectual disability (ID) in two unrelated families, one from Austria, the other from Pakistan. Genome-wide single nucleotide polymorphism microarray analysis enabled us to define a region of homozygosity by descent on chromosome 17q25. Whole-exome sequencing and analysis of this region in an affected individual from the Austrian family identified a 5 bp frameshifting deletion in the METTL23 gene. By means of Sanger sequencing of METTL23, a nonsense mutation was detected in a consanguineous ID family from Pakistan for which homozygosity-by-descent mapping had identified a region on 17q25. Both changes lead to truncation of the putative METTL23 protein, which disrupts the predicted catalytic domain and alters the cellular localization. 3D-modelling of the protein indicates that METTL23 is strongly predicted to function as an S-adenosyl-methionine (SAM)-dependent methyltransferase. Expression analysis of METTL23 indicated a strong association with heat shock proteins, which suggests that these may act as a putative substrate for methylation by METTL23. A number of methyltransferases have been described recently in association with ID. Disruption of METTL23 presented here supports the importance of methylation processes for intact neuronal function and brain development.

U2 - 10.1093/hmg/ddu115

DO - 10.1093/hmg/ddu115

M3 - Article

SN - 1460-2083

VL - 23

SP - 4015

EP - 4023

JO - Human Molecular Genetics

JF - Human Molecular Genetics

IS - 15

ER -

Disruption of the methyltransferase-like 23 gene METTL23 causes mild autosomal recessive intellectual disability

Abstract

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