Burosumab and 1-25 (OH) Vitamin D on Human Osteoblasts (HYPO-BLASTES)
Effect of Burosumab and 1-25 (OH) Vitamin D on Human Osteoblasts From Patients Requiring Craniosynostosis Surgery for Idiopathic Reason or Due to Hypophosphatemic Rickets (HR)
Sponsor: Hospices Civils de Lyon
A observational or N/A phase clinical study on Craniosynostoses, this trial is actively recruiting participants. The trial is conducted by Hospices Civils de Lyon and has accumulated 16 data snapshots since 2020. Longitudinal tracking of this trial contributes to a broader understanding of treatment development timelines.
Status Flow
Change History
16 versions recorded-
Apr 17, 2026 — Present [daily]
Recruiting
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Feb 2026 — Apr 2026 [monthly]
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Feb 2025 — Feb 2026 [monthly]
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Sep 2024 — Feb 2025 [monthly]
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Jul 2024 — Sep 2024 [monthly]
Recruiting
▶ Show 11 earlier versions
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Apr 2024 — Jul 2024 [monthly]
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Mar 2024 — Apr 2024 [monthly]
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Mar 2023 — Mar 2024 [monthly]
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Sep 2022 — Mar 2023 [monthly]
Recruiting
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May 2022 — Sep 2022 [monthly]
Recruiting
Status: Not Yet Recruiting → Recruiting
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Dec 2021 — May 2022 [monthly]
Not Yet Recruiting
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Jan 2021 — Dec 2021 [monthly]
Not Yet Recruiting
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Nov 2020 — Jan 2021 [monthly]
Not Yet Recruiting
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Aug 2020 — Nov 2020 [monthly]
Not Yet Recruiting
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Feb 2020 — Aug 2020 [monthly]
Not Yet Recruiting
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Dec 2019 — Feb 2020 [monthly]
Not Yet Recruiting
First recorded
Eligibility Summary
FGF23 is the cornerstone of phosphate / calcium / vitamin D metabolism: it is synthesized mainly by osteocytes and acts as a phosphaturizing agent, inhibitor of dihydroxyvitamin D, and inhibitor of synthesis and secretion of PTH in most tissues. The specific role of FGF23 on bone has yet to be demonstrated. In osteoblasts, overexpression of FGF23 in vitro suppresses not only osteoblastic differentiation but also the synthesis of the mineralized matrix independently of its systemic action on phosphate metabolism. In osteoblasts, FGF23 also regulates the secretion of osteopontin by directly suppressing transcription of alkaline phosphatase. In some diseases such as hypophosphatemic rickets (HR), the direct role of FGF23 on bone has not yet been studied to our knowledge, whereas these genetic hypophosphatemias are secondary to overexpression of FGF23, whether an activating mutation of FGF23 or inhibitory mutations of its inhibitors (DMP1 and PHEX). However, patients with X-linked hypophosphatemic rickets (XLH) have higher circulating FGF23 levels than healthy controls and these levels are higher in treated patients. Management of XLH consists primarily of correcting the native vitamin D defect by prescribing active vitamin D analogs as well as phosphate supplementation to improve bone mineralization and decrease dental complications, growth, and bone deformities. Recently, a new therapeutic option has been developed for XLH, burosumab, a human monoclonal antibody that binds and inhibits FGF23 activity. The use of burosumab is currently authorized in France in some pediatric patients with severe forms of XLH. Independently of the indirect bone effects of phosphate correction and vitamin D levels, the direct role of burosumab on bone cells has never been studied. The objective of this project is to study the osteoblastic biology of patients with RH compared to control patients, and to evaluate the direct impact of the treatments used in this pathology on human osteoblasts.
Contact Information
- Hospices Civils de Lyon
For direct contact, visit the study record on ClinicalTrials.gov .