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Germline mutations affecting the histone H4 core cause a developmental syndrome by altering DNA damage response and cell cycle control

Missense mutations affecting lysine 91 in the histone H4 core cause a developmental syndrome marked by growth delay, microcephaly and intellectual disability. These mutations cause genomic instability by interfering with H4K91 ubiquitination, leading to abnormal cell cycle progression and apoptosis during early development.

Federico Tessadori
Jacques C Giltay
Gijs van Haaften
Research18 Sept 2017
Nature Genetics

Volume: 49, P: 1642-1646
Biallelic variants in CSMD1 are implicated in a neurodevelopmental disorder with intellectual disability and variable cortical malformations

Elizabeth A. Werren
Emily R. Peirent
Stephanie L. Bielas
ResearchOpen Access30 May 2024
Cell Death & Disease

Volume: 15, P: 1-15
A de novo variant in the human HIST1H4J gene causes a syndrome analogous to the HIST1H4C-associated neurodevelopmental disorder

Federico Tessadori
Atteeq U. Rehman
Gijs van Haaften
ResearchOpen Access05 Dec 2019
European Journal of Human Genetics

Volume: 28, P: 674-678
LINE1-mediated epigenetic repression of androgen receptor transcription causes androgen insensitivity syndrome

Jelena Pozojevic
Radhika Sivaprasad
Nadine C. Hornig
ResearchOpen Access15 Jul 2024
Scientific Reports

Volume: 14, P: 1-9
Further confirmation of the MED13L haploinsufficiency syndrome

Mieke M van Haelst
Glen R Monroe
Gijs van Haaften
Research30 Apr 2014
European Journal of Human Genetics

Volume: 23, P: 135-138
Deficiency of TET3 leads to a genome-wide DNA hypermethylation episignature in human whole blood

Michael A. Levy
David B. Beck
Jill A. Fahrner
ResearchOpen Access08 Nov 2021
npj Genomic Medicine

Volume: 6, P: 1-15
A paternal deletion of MKRN3, MAGEL2 and NDN does not result in Prader–Willi syndrome

Deniz Kanber
Jacques Giltay
Karin Buiting
Research10 Dec 2008
European Journal of Human Genetics

Volume: 17, P: 582-590
Author Correction: Deficiency of TET3 leads to a genome-wide DNA hypermethylation episignature in human whole blood

Michael A. Levy
David B. Beck
Jill A. Fahrner
Amendments and CorrectionsOpen Access24 Nov 2021
npj Genomic Medicine

Volume: 6, P: 1

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Germline mutations affecting the histone H4 core cause a developmental syndrome by altering DNA damage response and cell cycle control

Biallelic variants in CSMD1 are implicated in a neurodevelopmental disorder with intellectual disability and variable cortical malformations

A de novo variant in the human HIST1H4J gene causes a syndrome analogous to the HIST1H4C-associated neurodevelopmental disorder

LINE1-mediated epigenetic repression of androgen receptor transcription causes androgen insensitivity syndrome

Further confirmation of the MED13L haploinsufficiency syndrome

Deficiency of TET3 leads to a genome-wide DNA hypermethylation episignature in human whole blood

A paternal deletion of MKRN3, MAGEL2 and NDN does not result in Prader–Willi syndrome

Author Correction: Deficiency of TET3 leads to a genome-wide DNA hypermethylation episignature in human whole blood

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