Treatment of Autosomal Dominant Hypocalcemia Type 1 with the Calcilytic NPSP795 (SHP635)

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Abstract

Autosomal dominant hypocalcemia type 1 (ADH1) is a rare form of hypoparathyroidism caused by heterozygous, gain-of-function mutations of the calcium-sensing receptor gene ( CAR). Individuals are hypocalcemic with inappropriately low parathyroid hormone (PTH) secretion and relative hypercalciuria. Calcilytics are negative allosteric modulators of the extracellular calcium receptor (CaR) and therefore may have therapeutic benefits in ADH1. Five adults with ADH1 due to 4 distinct CAR mutations received escalating doses of the calcilytic compound NPSP795 (SHP635) on 3 consecutive days. Pharmacokinetics, pharmacodynamics, efficacy, and safety were assessed. Parallel in vitro testing with subject CaR mutations assessed the effects of NPSP795 on cytoplasmic calcium concentrations (Ca ²⁺ _i), and ERK and p38 ^MAPK phosphorylation. These effects were correlated with clinical responses to administration of NPSP795. NPSP795 increased plasma PTH levels in a concentration-dependent manner up to 129% above baseline (p=0.013) at the highest exposure levels. Fractional excretion of calcium (FECa) trended down but not significantly so. Blood ionized calcium levels remained stable during NPSP795 infusion despite fasting, no calcitriol and little calcium supplementation. NPSP795 was generally safe and well-tolerated. There was significant variability in response clinically across genotypes. In vitro, all mutant CaRs were half-maximally activated (EC ₅₀) at lower concentrations of extracellular calcium (Ca ²⁺ _o) compared to wild type (WT) CaR; NPSP795 exposure increased the EC ₅₀ for all CaR activity readouts. However, the in vitro responses to NPSP795 did not correlate with any clinical parameters. NPSP795 increased plasma PTH levels in subjects with ADH1 in a dose-dependent manner, and thus, serves as proof-of-concept that calcilytics could be an effective treatment for ADH1. Albeit all mutations appear to be activating at the CaR, in vitro observations were not predictive of the in vivo phenotype, or the response to calcilytics, suggesting that other parameters impact the response to the drug.

TRIAL REGISTRATION.

ClinicalTrials.gov Identifier: NCT02204579

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Author and article information

Journal

Journal ID (nlm-journal-id): 8610640

Journal ID (pubmed-jr-id): 104

Journal ID (nlm-ta): J Bone Miner Res

Journal ID (iso-abbrev): J. Bone Miner. Res.

Title: Journal of bone and mineral research : the official journal of the American Society for Bone and Mineral Research

ISSN (Print): 0884-0431

ISSN (Electronic): 1523-4681

Publication date Nihms-submitted: 2 May 2019

Publication date (Electronic): 26 July 2019

Publication date (Print): September 2019

Publication date PMC-release: 01 September 2020

Volume: 34

Issue: 9

Pages: 1609-1618

Affiliations

[1 ]Skeletal Disorders and Mineral Homeostasis Section, National Institute of Dental and Craniofacial Research (NIDCR), National Institutes of Health (NIH), Bethesda, MD, USA

[2 ]NPS Pharmaceuticals, Inc., Bedminster, NJ

[3 ]School of Biosciences, Cardiff University, Cardiff, UK

[4 ]School of Life and Environmental Science, University of Sydney, NSW, Australia

[5 ]Institute of Pathophysiology and Allergy Research, Medical University of Vienna, Vienna, AT

[6 ]Faculty of Biology, Medicine and Health, The University of Manchester, Manchester, UK

[7 ]Faculty of Biotechnology and Biomolecular Sciences, Universiti Putra Malaysia, Selangor, Malaysia

[8 ]MetisMedica, Toronto, ON, Canada

Author notes

AUTHOR CONTRIBUTIONS:

MSR, RIG, BB, LG, and MTC conducted the clinical trial and acquired data. MSR, RIG, DG, EN, RR, and MTC contributed to designing the study and analyzing data. EK contributed to performing the statistical analysis for the clinical research study. JG contributed to analyzing data. SCB, DR, MS, MBK, DTW, and EN contributed to designing and analyzing the data from the in vitro studies. SCB, MS, DR, MBK, and DTW carried out the in vitro studies. MSR, RIG, SCB and MTC wrote the manuscript, and all remaining authors reviewed/revised the manuscript prior to publication.

Corresponding author and person to whom reprint requests should be addressed: Michael T. Collins, MD, Skeletal Disorders and Mineral Homeostasis Section, NIDCR, National Institutes of Health, Building 30, Room 228, 30 Convent Dr. MSC 4320, Bethesda, MD 20892-4320, 301-496-4913 (tel), Mc247k@ 123456nih.gov

Article

Accession ID: PMC6744344 Pmcid ID: PMC6744344 Pmc-uid ID: 6744344 Manuscript ID: nihpa1025340

DOI: 10.1002/jbmr.3747

PMC ID: 6744344

PubMed ID: 31063613

SO-VID: 386c2ffa-c4aa-4a7d-b91a-dc4d4bbf42ed

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