The role of Kabuki Syndrome genes KMT2D and KDM6A in development: Analysis in Human sequencing data and compared to mice and zebrafish

KMT2D and KDM6A are epigenetic regulators that have been implicated in Kabuki Syndrome, a rare congenital birth defect with multiple tissue and organ abnormalities, including craniofacial and heart defects. Our previous study identified human families with mutations in the epigenetic modifiers KMT2D and KDM6A, which is implicated in 32% and 10% of Kabuki Syndrome patients respectively. To understand the connection to Kabuki syndrome patients, and the transcriptional targets of KMT2D and KDM6A in humans, we performed RNA sequencing (seq) of lymphoblastoid cells from Kabuki Syndrome patients carrying mutations in KMT2D and KDM6A. We identified 1995 significant changes in transcriptional targets for KMT2D and 1917 for KDM6A, as compared to control. When compared with RNA-seq datasets obtained from other mouse and zebrafish studies, our analysis revealed KMT2D mutations affect the expression of 76 orthologous genes across all three datasets. Similarliy, KDM6A afftects the expprssion of 7 orthologous genes across three datasets. Despite the differences in cell types, stages, and species in the comparison between the transcriptomic datasets, there are common gene expression changes associated with KMT2D and KDM6A mutations. qPCR on novel zebrafish mutants confirmed the differentially expression in KMT2D or KDM6A mutant backgrounds. Taken together, our results show that KMT2D and KDM6A regulate common and unique genes across humans, mice, and zebrafish for early craniofacial and cardiac development and this information contributes to the understanding of epigenetic dysregulation during development of Kabuki syndrome.

• Publication year

  2020

• Venue

  bioRxiv

• Publication date

  2020-04-04

• Fields of study

  Biology, Medicine

• Identifiers
  DOI 10.1101/2020.04.03.024646
• External record

  Open on Semantic Scholar

• Source metadata

  Semantic Scholar

• No claims are published for this paper.

• No concepts are published for this paper.

• Identification of KMT2D and KDM6A variants by targeted sequencing from patients with Kabuki syndrome and other congenital disorders.

  2020cited by this paper
• Dysregulated micro-RNAs and long noncoding RNAs in cardiac development and pediatric heart failure

  2020cited by this paper
• Sequence Analysis

  2020cited by this paper
• The KMT2D Kabuki syndrome histone methylase controls neural crest cell differentiation and facial morphology.

  2020cited by this paper
• Inhibitor of DNA binding in heart development and cardiovascular diseases

  2019cited by this paper
• Why are so many MLL lysine methyltransferases required for normal mammalian development?

  2019cited by this paper
• YAP Partially Reprograms Chromatin Accessibility to Directly Induce Adult Cardiogenesis In Vivo.

  2019cited by this paper
• Kabuki syndrome: novel pathogenic variants, new phenotypes and review of literature

  2019cited by this paper
• H3K27me3-mediated silencing of structural genes is required for zebrafish heart regeneration

  2019cited by this paper
• The X-linked histone demethylase Kdm6a in CD4+ T lymphocytes modulates autoimmunity.

  2019cited by this paper
• Loss of function of Kmt2d, a gene mutated in Kabuki syndrome, affects heart development in Xenopus laevis

  2019cited by this paper
• Precocious Chondrocyte Differentiation Disrupts Skeletal Growth in Kabuki Syndrome Mice

  2019cited by this paper
• Novel heterozygous variants in KMT2D associated with holoprosencephaly

  2019cited by this paper
• The Kdm/Kmt gene families in the self-fertilizing mangrove rivulus fish, Kryptolebias marmoratus, suggest involvement of histone methylation machinery in development and reproduction.

  2019cited by this paper
• Mixed-lineage leukemia protein 2 suppresses ciliary assembly by the modulation of actin dynamics and vesicle transport

  2019cited by this paper
• Lysine demethylases KDM6A and UTY: The X and Y of histone demethylation.

  2019cited by this paper
• Haploinsufficiency of KMT2D is sufficient to cause Kabuki syndrome and is compatible with life

  2019cited by this paper
• The histone methyltransferase KMT2D, mutated in Kabuki syndrome patients, is required for neural crest cell formation and migration

  2019cited by this paper
• UTX Affects Neural Stem Cell Proliferation and Differentiation through PTEN Signaling

  2018cited by this paper
• Kabuki syndrome: international consensus diagnostic criteria

  2018cited by this paper
• Investigation of the SLC22A23 gene in laryngeal squamous cell carcinoma

  2018cited by this paper
• Dissecting KMT2D missense mutations in Kabuki syndrome patients

  2018cited by this paper
• Lysine methyltransferase 2D regulates pancreatic carcinogenesis through metabolic reprogramming

  2018cited by this paper
• Lsd1 interacts with cMyb to demethylate repressive histone marks and maintain inner ear progenitor identity

  2018cited by this paper
• Direct Cardiac Reprogramming: Progress and Promise

  2018cited by this paper
• Inhibition of Notch signaling rescues cardiovascular development in Kabuki Syndrome

  2018cited by this paper
• High-Resolution Epigenomic Atlas of Human Embryonic Craniofacial Development

  2018cited by this paper
• UTX-guided neural crest function underlies craniofacial features of Kabuki syndrome

  2017influential reference
• Histone demethylases Kdm6ba and Kdm6bb redundantly promote cardiomyocyte proliferation during zebrafish heart ventricle maturation.

  2017cited by this paper
• Id genes are essential for early heart formation

  2017cited by this paper
• Congenital heart defects in molecularly proven Kabuki syndrome patients

  2017cited by this paper
• UTX demethylase activity is required for satellite cell-mediated muscle regeneration.

  2016influential reference
• Re-patterning of H3K27me3, H3K4me3 and DNA methylation during fibroblast conversion into induced cardiomyocytes.

  2016cited by this paper
• KMT2D regulates specific programs in heart development via histone H3 lysine 4 di-methylation

  2016influential reference
• Targeting Mll1 H3K4 methyltransferase activity to guide cardiac lineage specific reprogramming of fibroblasts

  2016cited by this paper
• Improving cardiac reprogramming for heart regeneration

  2016cited by this paper
• Role of Histone Demethylases in Cardiomyocytes Induced to Hypertrophy

  2016cited by this paper
• Evolutionarily conserved role for SoxC genes in neural crest specification and neuronal differentiation.

  2015cited by this paper
• Histone methylations in heart development, congenital and adult heart diseases.

  2015cited by this paper
• Histone Demethylases KDM4A and KDM4C Regulate Differentiation of Embryonic Stem Cells to Endothelial Cells

  2015cited by this paper
• DNA methylation abnormalities in congenital heart disease

  2015cited by this paper
• Disrupted intricacy of histone H3K4 methylation in neurodevelopmental disorders.

  2015cited by this paper
• Emerging Roles of JmjC Domain-Containing Proteins.

  2015cited by this paper
• Efficient Mutagenesis by Cas9 Protein-Mediated Oligonucleotide Insertion and Large-Scale Assessment of Single-Guide RNAs

  2014cited by this paper
• Human UTY(KDM6C) Is a Male-specific Nϵ-Methyl Lysyl Demethylase

  2014cited by this paper
• Orphan nuclear receptor NR2F6 acts as an essential gatekeeper of Th17 CD4+ T cell effector functions

  2014cited by this paper
• Prdm1 functions in the mesoderm of the second heart field, where it interacts genetically with Tbx1, during outflow tract morphogenesis in the mouse embryo.

  2014cited by this paper
• KDM6 Demethylase Independent Loss of Histone H3 Lysine 27 Trimethylation during Early Embryonic Development

  2014cited by this paper
• Diverse functions of PHD fingers of the MLL/KMT2 subfamily.

  2014cited by this paper
• A Hypomorphic Lsd1 Allele Results in Heart Development Defects in Mice

  2013cited by this paper
• De novo mutations in histone modifying genes in congenital heart disease

  2013cited by this paper
• Cardiac outflow tract development relies on the complex function of Sox4 and Sox11 in multiple cell types

  2013cited by this paper
• Direct cardiac reprogramming

  2013cited by this paper
• Conditional Ablation of Ezh2 in Murine Hearts Reveals Its Essential Roles in Endocardial Cushion Formation, Cardiomyocyte Proliferation and Survival

  2012cited by this paper
• Polycomb Repressive Complex 2 Regulates Normal Development of the Mouse Heart

  2012cited by this paper
• Multiple essential roles for primary cilia in heart development

  2012cited by this paper
• UTX, a histone H3-lysine 27 demethylase, acts as a critical switch to activate the cardiac developmental program.

  2012influential reference
• The KAT6B‐related disorders genitopatellar syndrome and Ohdo/SBBYS syndrome have distinct clinical features reflecting distinct molecular mechanisms

  2012cited by this paper
• [Direct reprogramming of fibroblasts into functional cardiomyocytes by defined factors].

  2011cited by this paper
• The histone trimethyllysine demethylase JMJD2A promotes cardiac hypertrophy in response to hypertrophic stimuli in mice.

  2011cited by this paper
• Epigenetic repression of cardiac progenitor gene expression by Ezh2 is required for postnatal cardiac homeostasis

  2011cited by this paper
• Loss of H3K4 methylation destabilizes gene expression patterns and physiological functions in adult murine cardiomyocytes.

  2011cited by this paper
• Genome-wide association study of antipsychotic induced QTc interval prolongation

  2010cited by this paper
• Organogenesis relies on SoxC transcription factors for the survival of neural and mesenchymal progenitors

  2010cited by this paper
• Chromatin regulation by Brg1 underlies heart muscle development and disease

  2010cited by this paper
• Chromatin remodeling in heart development.

  2010cited by this paper
• Foxp1 coordinates cardiomyocyte proliferation through both cell-autonomous and nonautonomous mechanisms.

  2010cited by this paper
• Clinical spectrum of SIX3-associated mutations in holoprosencephaly: correlation between genotype, phenotype and function

  2009cited by this paper
• Developmental roles of the histone lysine demethylases

  2009cited by this paper
• Critical Role of Transcription Factor Cyclic AMP Response Element Modulator in &bgr;1-Adrenoceptor–Mediated Cardiac Dysfunction

  2009cited by this paper
• Sox12 Deletion in the Mouse Reveals Nonreciprocal Redundancy with the Related Sox4 and Sox11 Transcription Factors

  2008cited by this paper
• Dynamic regulation of histone lysine methylation

  2008cited by this paper
• Mouse ES cell-derived cardiac precursor cells are multipotent and facilitate identification of novel cardiac genes.

  2008cited by this paper
• A histone H3 lysine 27 demethylase regulates animal posterior development

  2007cited by this paper
• Dynamic regulation of histone lysine methylation by demethylases.

  2007cited by this paper
• Identification of JmjC domain-containing UTX and JMJD3 as histone H3 lysine 27 demethylases

  2007cited by this paper
• Six3 represses nodal activity to establish early brain asymmetry in zebrafish.

  2007cited by this paper
• UTX and JMJD3 are histone H3K27 demethylases involved in HOX gene regulation and development

  2007cited by this paper
• JmjC-domain-containing proteins and histone demethylation

  2006cited by this paper
• Chromatin Modification and Remodeling in Heart Development

  2006cited by this paper
• Mutations in a new member of the chromodomain gene family cause CHARGE syndrome

  2004cited by this paper
• Rescue of Cardiac Defects in Id Knockout Embryos by Injection of Embryonic Stem Cells

  2004cited by this paper
• Advanced Cardiac Morphogenesis Does Not Require Heart Tube Fusion

  2004cited by this paper
• ALK4 functions as a receptor for multiple TGF beta-related ligands to regulate left-right axis determination and mesoderm induction in Xenopus.

  2004cited by this paper
• Baf60c is essential for function of BAF chromatin remodelling complexes in heart development

  2004cited by this paper
• Friend of GATA 2 Physically Interacts with Chicken Ovalbumin Upstream Promoter-TF2 (COUP-TF2) and COUP-TF3 and Represses COUP-TF2-dependent Activation of the Atrial Natriuretic Factor Promoter*

  2001cited by this paper
• Proper coronary vascular development and heart morphogenesis depend on interaction of GATA-4 with FOG cofactors.

  2001cited by this paper
• Immunolocalization of annexins IV, V and VI in the failing and non-failing human heart.

  2000cited by this paper
• The zebrafish book : a guide for the laboratory use of zebrafish (Danio rerio)

  1995cited by this paper
• Stages of embryonic development of the zebrafish

  1995cited by this paper
• [Mixed lineage leukemia].

  1990cited by this paper

• Loss of function of the zinc finger homeobox 4 gene, ZFHX4, underlies a neurodevelopmental disorder.

  2025cites this paper