<i>CYP24A1</i>Mutations in a Cohort of Hypercalcemic Patients: Evidence for a Recessive Trait

Arnaud Molin; R. Baudoin; Martin Kaufmann; J.-C. Souberbielle; Amélie Ryckewaert; Marie‐Christine Vantyghem; P. Eckart; Justine Bacchetta; Georges Deschênes; G. Kesler-Roussey; Nadia Coudray; Nicolas Richard; M. Wraich; Q. Bonafiglia; Anatoly Tiulpakov; Glenville Jones; Marie‐Laure Kottler

doi:10.1210/jc.2014-4387

<i>CYP24A1</i>Mutations in a Cohort of Hypercalcemic Patients: Evidence for a Recessive Trait

Arnaud Molin(Université de Caen Normandie), R. Baudoin(Université de Bordeaux), Martin Kaufmann(Queen's University), J.-C. Souberbielle(Université de Caen Normandie), Amélie Ryckewaert(Université de Caen Normandie), Marie‐Christine Vantyghem(Université de Lille), P. Eckart(Université de Caen Normandie), Justine Bacchetta(Université de Lyon), Georges Deschênes(Assistance Publique – Hôpitaux de Paris), G. Kesler-Roussey(Nantes Université), Nadia Coudray(Université de Caen Normandie), Nicolas Richard(Université de Caen Normandie), M. Wraich(Queen's University), Q. Bonafiglia(Queen's University), Anatoly Tiulpakov(Endocrinology Research Center), Glenville Jones(Queen's University), Marie‐Laure Kottler(Inserm)

The Journal of Clinical Endocrinology & Metabolism

July 27, 2015

10.1210/jc.2014-4387

Cited by 141Open Access

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Abstract

CONTEXT: Loss-of-function mutations of CYP24A1 (which encodes the 25-OH-D3-24-hydroxylase) have recently been reported to cause hypercalcemia. OBJECTIVES: The aims of this study were: 1) to evaluate the frequency of CYP24A1 mutations in patients with medical history of hypercalcemia; 2) to show the clinical utility of a simultaneous assay of serum 25-hydroxyvitamin D3 (25-OH-D3) and 24,25-dihydroxyvitamin D3 (24,25-[OH]2D3) by liquid chromatography tandem mass spectrometry (LC-MS/MS); and 3) to investigate biochemical parameters in heterozygous gene carriers with CYP24A1 mutations. PATIENTS AND METHODS: We screened for CYP24A1 mutations in 72 patients with serum calcium levels > 2.6 mmol/L and PTH levels < 20 pg/mL and recruited 24 relatives after genetic counseling for subsequent investigations. Vitamin D metabolite concentrations were assessed in a subset of patients by LC-MS/MS and results expressed as a ratio (R) of 25-OH-D3:24,25-(OH)2D3. RESULTS: Twenty-five patients with hypercalcemia (35%) harbored CYP24A1 variations. Twenty (28%) had biallelic variations, mostly found in subjects with nephrocalcinosis or renal stones (19/20). Five patients, all neonates, were heterozygous, without renal disease. We describe 15 new variations leading to loss-of-function according to pathogenicity prediction programs, and we functionally characterized 5 of them in vitro. A dramatic increase of R, usually >80, was found in patients harboring biallelic mutations providing evidence in vivo for the loss of CYP24A1 activity. In contrast, R value remains <25 in patients without CYP24A1 mutations. Subjects carrying one mutant allele, hypercalcemic individuals, as well as gene-carrier relatives, had a detectable 24,25-(OH)2D3 level and R < 25, indicating normal 24-hydroxylase activity. CONCLUSION: CYP24A1 biallelic mutations are frequently found in patients presenting with hypercalcemia, low PTH, and renal disease. We confirm the accuracy and effectiveness of a novel blood test estimating the ratio between relevant vitamin D metabolites as a useful screening tool for CYP24A1 mutations. Haploinsufficiency is not associated with CYP24A1 deficiency.

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