Non-coding cis-regulatory variants in HK1 cause congenital hyperinsulinism with variable disease severity.

(Genome medicine, v17.1:17)

Background

We recently reported non-coding variants in a cis-regulatory element of the beta-cell disallowed gene hexokinase 1 (HK1) as a novel cause of congenital hyperinsulinism. These variants lead to a loss of repression of HK1 in pancreatic beta-cells, causing insulin secretion during hypoglycaemia. In this study, we aimed to determine the prevalence, genetics, and phenotype of HK1-hyperinsulinism by screening a large international cohort of patients living with the condition.

Methods

We screened the HK1 cis-regulatory region in 1761 probands with hyperinsulinism of unknown aetiology who had been referred to one of three large European genomics laboratories.

Results

We identified a HK1 variant in 89/1761 probands (5%) and 63 family members. Within the Exeter HI cohort, these variants accounted for 2.8% of all positive genetic diagnoses (n = 54/1913) establishing this as an important cause of HI. Individuals with a disease-causing variant were diagnosed with hyperinsulinism between birth and 26 years (median: 7 days) with variable response to treatment; 80% were medically managed and 20% underwent pancreatic surgery due to poor response to medical therapy. Glycaemic outcomes varied from spontaneous remission to hypoglycaemia persisting into adulthood. Eight probands had inherited the variant from a parent not reported to have hyperinsulinism (median current age: 39 years), confirming variable penetrance. Two of the 23 novel HK1 variants allowed us to extend the minimal cis-regulatory region from 42 to 46 bp.

Conclusions

Non-coding variants within the HK1 cis-regulatory region cause hyperinsulinism of variable severity ranging from neonatal-onset, treatment-resistant disease to being asymptomatic into adulthood. Discovering variants in 89 families confirms HK1 as a major cause of hyperinsulinism and highlights the important role of the non-coding genome in human monogenic disease.

© 2025. The Author(s).

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Overview publication

TitleNon-coding cis-regulatory variants in HK1 cause congenital hyperinsulinism with variable disease severity.
Date2025-03-03
Issue nameGenome medicine
Issue numberv17.1:17
DOI10.1186/s13073-025-01440-w
PubMed40033430
AuthorsBennett JJ, Saint-Martin C, Neumann B, Männistö JME, Houghton JAL, Empting S, Johnson MB, Laver TW, Locke JM, Spurrier B, Wakeling MN, Banerjee I, Dastamani A, Demirbilek H, Mitchell J, Stange M, Mohnike K, Arnoux JB, Owens NDL, Zenker M, Bellanné-Chantelot C & Flanagan SE
InfoInternational Congenital Hyperinsulinism Consortium, Abi Warde MT, Amrita M, Aravena R, Arion A, Atapattu N, Barić I, Bertherat J, Bilici E, Bouchereau J, Braun K, Campas-Lebecque MN, Castanet M, Cessans C, Conwell LS, Dabadghao P, Dayal Arya A, de Lonlay P, de Vries L, Droumaguet C, Faure-Galon N, Gilly O, Goldenberg A, Guemann AS, Guerrot AM, Harvengt J, Hassan SS, Hui SS, Humayun KN, Ibrahim M, Jain V, Jeevarathnam D, Loke KY, Khadilkar V, Kochar IPS, Kulkarni A, Kumbhojkar A, Lamireau D, Levy-Khademi F, Limbert C, Lindner M, Lombard C, Maillot F, Mention K, Mericq V, Mohamed Z, Mornet C, Murray P, Naccache A, Navasardyan LV, Neville K, Nicolescu R, Nicolino M, Nishimura-Meguro E, Numsriskulrat N, O'sullivan S, Ouarezki Y, Pambou A, Petit F, Praveen VP, Priou-Guesdon M, Radka S, Rami-Merhar B, Rao S, Reznik Y, Rulquin L, Salomon Estebanez M, Souto I, Tabarin A, Tangari A, Van Aken S, Verge C, Vinolas H, Voinot C, Wagner R, Walker J, Wiltshire E
KeywordsCongenital hyperinsulinism, Hexokinase 1, Monogenic disease, Non-coding, Variable penetrance
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