Spontaneous Reshaping of Vertebral Fractures in an Adolescent with Osteogenesis Imperfecta

Overview

Journal Bone Rep

Date 2022 Jun 13

PMID 35693066

Authors

Rodrigo Montero-Lopez

Elisabeth Laurer

Katharina Tischlinger

Dora Nagy

Mario Scala

Wolfgang Kranewitter

Gerald Webersinke

Thomas Hortenhuber

Wolfgang Hogler

Affiliations

Soon will be listed here.

Abstract

Background: Vertebral compression fractures (VFs) are a common and severe finding in patients with osteoporosis. In children, VFs have the unique potential to reshape and regain their original configuration. Spontaneous vertebral body reshaping (, medication-unassisted) has been reported in secondary osteoporosis. Here we describe a previously unreported spontaneous vertebral reshaping in an adolescent with osteogenesis imperfecta (OI) with multiple vertebral fractures.

Case Report: A 17-year-old female was diagnosed with OI type I at 5 years of age caused by a novel frameshift variant in (NM_000088.4: c.540delC; p.Met181TrpfsTer84). Due to parental reservations about medication, she had never received bisphosphonate or any other bone active therapy. A lateral spine X-ray demonstrated transparent bones and no VF. However, previous spine X-rays taken at age of 6 years at an external institution showed VFs in T5-7 (Genant semiquantitative method grade I-II). The two lateral spine x-rays, taken 11 years apart, demonstrate that substantial spontaneous vertebral reshaping occurred without bone active therapy during puberty.

Discussion: Vertebral reshaping is explained by the stabilization of bone mineral density (BMD) and the remaining growth capacity the children. We hypothesize that spontaneous reshaping may occur in milder forms of OI, and that puberty may be a key mediator of the phenomenon. In all children with OI and vertebral fractures, we nevertheless recommend bisphosphonate therapy since it improves bone mass, BMD, vertebral shape, physical activity and reduces fracture rates.

Citing Articles

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Ward L Front Endocrinol (Lausanne). 2024; 14:1266986.

PMID: 38374961 PMC: 10875302. DOI: 10.3389/fendo.2023.1266986.

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