Mutation Update for Kabuki Syndrome GenesKMT2DandKDM6Aand Further Delineation of X-Linked Kabuki Syndrome Subtype 2

Bögershausen, Nina; Gatinois, Vincent; Riehmer, Vera; Kayserili, Hülya; Becker, Jutta; Thoenes, Michaela; Şimşek‐Kiper, Pelin Özlem; Barat‐Houari, Mouna; Elçioğlu, Nursel; Wieczorek, Dagmar; Tinschert, Sigrid; Sarrabay, Guillaume; Strom, Tim M.; Fabre, Aurélie; Baynam, Gareth; Sanchez, Elodie; Nürnberg, Gudrun; Altunoğlu, Umut; Capri, Yline; Isidor, Bertrand; Lacombe, Didier; Corsini, Carole; Cormier‐Daire, Valérie; Sanlaville, Damien; Giuliano, Fabienne; Sang, Kim-Hanh Le Quan; Kayirangwa, Honorine; Nürnberg, Peter; Meitinger, Thomas; Boduroğlu, Koray; Zoll, Barbara; Lyonnet, Stanislas; Tzschach, Andreas; Verloès, Alain; Donato, Nataliya Di; Touitou, Isabelle; Netzer, Christian; Li, Yun; Geneviève, David; Yiğit, Gökhan; Wollnik, Bernd

doi:10.1002/humu.23026

Cited by 156 publications

(183 citation statements)

References 66 publications

(138 reference statements)

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“…KDM6A is a lysine specific histone demethylase that controls tissue-specific expression of genes involved in development as well as the cell cycle [34–38]. Loss of function mutations of KDM6A which cause Kabuki Syndrome Type 2, KS2, are most often somatic mutations [18, 20, 22–25, 27]. Arnoux, et al, reported that hypoglycemia occurs in 11% of Kabuki Syndrome patients overall [39].…”

Section: Discussionmentioning

confidence: 99%

“…Arnoux, et al, reported that hypoglycemia occurs in 11% of Kabuki Syndrome patients overall [39]. Recent reports suggest that hypoglycemia may occur in a much higher proportion of patients with KS2 associated with KDM6A mutations [13, 20, 22, 26]. The mechanism by which haploinsufficiency for KDM6A causes hyperinsulinism in Kabuki Syndrome is not known, but has been suggested to involve disruption of epigenetic changes during pancreatic differentiation [28, 29].…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Congenital Hyperinsulinism in Infants with Turner Syndrome: Possible Association with Monosomy X and KDM6A Haploinsufficiency

Gibson

Boodhansingh

et al. 2018

Horm Res Paediatr

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Background: Previous case reports have suggested a possible association of congenital hyperinsulinism with Turner syndrome. Objective: We examined the clinical and molecular features in girls with both congenital hyperinsulinism and Turner syndrome seen at The Children’s Hospital of Philadelphia (CHOP) between 1974 and 2017. Methods: Records of girls with hyperinsulinism and Turner syndrome were reviewed. Insulin secretion was studied in pancreatic islets and in mouse islets treated with an inhibitor of KDM6A, an X chromosome gene associated with hyperinsulinism in Kabuki syndrome. Results: Hyperinsulinism was diagnosed in 12 girls with Turner syndrome. Six were diazoxide-unresponsive; 3 had pancreatectomies. The incidence of Turner syndrome among CHOP patients with hyperinsulinism (10 of 1,050 from 1997 to 2017) was 48 times more frequent than expected. The only consistent chromosomal anomaly in these girls was the presence of a 45,X cell line. Studies of isolated islets from 1 case showed abnormal elevated cytosolic calcium and heightened sensitivity to amino acid-stimulated insulin release; similar alterations were demonstrated in mouse islets treated with a KDM6A inhibitor. Conclusion: These results demonstrate a higher than expected frequency of Turner syndrome among children with hyperinsulinism. Our data suggest that haploinsufficiency for KDM6A due to mosaic X chromosome monosomy may be responsible for hyperinsulinism in Turner syndrome.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Congenital Hyperinsulinism in Infants with Turner Syndrome: Possible Association with Monosomy X and KDM6A Haploinsufficiency

Gibson

Boodhansingh

et al. 2018

Horm Res Paediatr

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“…After BWS, Kabuki syndrome is the second most common syndromic form of HI. Kabuki syndrome is caused by inactivating mutations in 2 genes: autosomal recessive mutations in KMT2D ( Lysine‐specific methyltransferase 2D ), which account for 70%‐75% of cases, and X‐linked mutations in KDM6A ( Lysine‐specific demethylase 6A ), which account for 1%‐9% of cases. These 2 genes encode a DNA methyltransferase and demethylase, respectively.…”

Section: Highlights From the Conferencementioning

confidence: 99%

Congenital Hypoglycemia Disorders: New Aspects of Etiology, Diagnosis, Treatment and Outcomes

León

Stanley

2016

Pediatr Diabetes

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Hypoglycemia continues to be an important cause of morbidity in neonates and children. Prompt diagnosis and management of the underlying hypoglycemia disorder is critical for preventing brain damage and improving outcomes. Congenital hyperinsulinism is the most common and severe cause of persistent hypoglycemia in neonates and children. Recent discoveries of the genetic causes of hyperinsulinism have improved our understanding of the pathophysiology, but its management is complex and requires the integration of clinical, biochemical, molecular and imaging findings to establish the appropriate treatment according to the subtype. Here we present a summary of a recent international symposium on congenital hypoglycemia disorders with emphasis on novel molecular mechanisms resulting in hyperinsulinism, genetic diagnosis, overall approach to management, novel therapies under development, and current outcomes.

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“…Heterozygous or hemizygous, pathogenic variants in either KMT2D (OMIM: 147920; 80% of cases) or KDM6A (OMIM: 300867; 8%), respectively, cause Kabuki syndrome (Banka et al, ; Bogershausen et al, ; Lederer et al, ; Miyake et al, ; Ng et al, ; Van Laarhoven et al, ). KMT2D encodes a H3K4 methyltransferase that associates with KDM6A, an H3K27 demethylase, and other proteins to form the activating signal co‐integrator 2 containing complex (ASCOM) responsible for chromatin regulation and transcription activation where loss of function leads to repressed transcription in a wide range of downstream genes (Demers, Chaturvedi, Ranish, et al, ; Van Laarhoven et al, ).…”

Section: Introductionmentioning

confidence: 99%

Holoprosencephaly in Kabuki syndrome

Daly

Roberts

Yang

et al. 2019

American J of Med Genetics Pt A

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Kabuki syndrome is a rare, multi‐systemic disorder of chromatin regulation due to mutations in either KMT2D or KDM6A that encode a H3K4 methyltransferase and an H3K27 demethylase, respectively. The associated clinical phenotype is a direct result of temporal and spatial changes in gene expression in various tissues including the brain. Although mild to moderate intellectual disability is frequently recognized in individuals with Kabuki syndrome, the identification of brain anomalies, mostly involving the hippocampus and related structures remains an exception. Recently, the first two cases with alobar holoprosencephaly and mutations in KMT2D have been reported in the medical literature. We identified a de novo, pathogenic KMT2D variant (c.6295C > T; p.R2099X) using trio whole‐exome sequencing in a 2‐year‐old female with lobar holoprosencephaly, microcephaly and cranio‐facial features of Kabuki syndrome. This report expands the spectrum of brain anomalies associated with Kabuki syndrome underscoring the important role of histone modification for early brain development.

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Mutation Update for Kabuki Syndrome GenesKMT2DandKDM6Aand Further Delineation of X-Linked Kabuki Syndrome Subtype 2

Cited by 156 publications

References 66 publications

Congenital Hyperinsulinism in Infants with Turner Syndrome: Possible Association with Monosomy X and <b><i>KDM6A</i></b> Haploinsufficiency

Congenital Hyperinsulinism in Infants with Turner Syndrome: Possible Association with Monosomy X and <b><i>KDM6A</i></b> Haploinsufficiency

Congenital Hypoglycemia Disorders: New Aspects of Etiology, Diagnosis, Treatment and Outcomes

Holoprosencephaly in Kabuki syndrome

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