Fracture risk reduction during treatment with teriparatide is independent of pretreatment bone turnover

P D Delmas; A A Licata; J Y Reginster; G G Crans; P Chen; D A Misurski; R B Wagman; B H Mitlak

doi:10.1016/j.bone.2006.02.003

Fracture risk reduction during treatment with teriparatide is independent of pretreatment bone turnover

Bone. 2006 Aug;39(2):237-43. doi: 10.1016/j.bone.2006.02.003. Epub 2006 Mar 24.

Authors

P D Delmas¹, A A Licata, J Y Reginster, G G Crans, P Chen, D A Misurski, R B Wagman, B H Mitlak

Affiliation

¹ INSERM Research Unit 403, Claude Bernard University of Lyon, Lyon, France. delmas@lyon.inserm.fr

PMID: 16563890
DOI: 10.1016/j.bone.2006.02.003

Abstract

Introduction: Teriparatide is a bone formation agent that increases bone turnover and mass, resulting in an increase in bone strength and a decrease in fracture risk.

Methods: The primary purpose of this analysis was to evaluate the association between pretreatment bone turnover marker (BTM) concentrations and the absolute and relative fracture risks after adjusting for baseline femoral neck BMD, number of prevalent vertebral fractures, and age. Because femoral neck BMD is commonly attained in the assessment of patients at risk for osteoporosis, we examined the ability of a multivariate assessment including pretreatment BTM concentration and femoral neck BMD to predict future fracture risk after adjusting for the number of prevalent vertebral fractures. We examined data from the Fracture Prevention Trial, a study designed to determine the effect of teriparatide 20 mcg/day and teriparatide 40 mcg/day on vertebral and nonvertebral fracture risk in postmenopausal women with osteoporosis. BTM were analyzed in two subsets of women within the Fracture Prevention Trial, and included serum bone-specific alkaline phosphatase (BSAP), serum carboxy-terminal extension peptide of procollagen type I (PICP), serum amino-terminal extension peptide of procollagen type I (PINP), urinary free deoxypyridinoline (DPD), and urinary N-terminal telopeptide (NTX).

Results: Teriparatide significantly reduced the risk of fracture [four BTM subset (n = 520), placebo = 14.3%, teriparatide = 5.8%, P < 0.05; PINP subset (n = 771), placebo = 17.7%, teriparatide = 5.5%, P < 0.05]. Subjects with the highest pretreatment BTM concentrations had the greatest fracture risk. Teriparatide-mediated absolute risk reduction was greatest for women with high pretreatment bone turnover; however, the relative fracture risk reduction was independent of pretreatment bone turnover. After adjusting for pretreatment BTM and number of prevalent vertebral fractures, baseline femoral neck BMD was not a significant predictor of fracture risk.

Conclusion: Teriparatide-mediated relative fracture risk reduction was independent of pretreatment bone turnover, demonstrating that this therapy offers clinical benefit to patients across a range of disease severity.

Publication types

Clinical Trial
Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Aged
Aged, 80 and over
Alkaline Phosphatase / blood
Amino Acids / urine
Biomarkers / blood
Biomarkers / urine
Bone Density / drug effects
Bone Density Conservation Agents / therapeutic use*
Bone and Bones / drug effects*
Cohort Studies
Collagen Type I / blood
Collagen Type I / urine
Dose-Response Relationship, Drug
Female
Femur Neck / pathology
Fractures, Bone / prevention & control*
Humans
Middle Aged
Osteoporosis, Postmenopausal / drug therapy*
Peptide Fragments / blood
Peptides / urine
Procollagen / blood
Risk
Risk Factors
Teriparatide / therapeutic use*
Treatment Outcome

Substances

Amino Acids
Biomarkers
Bone Density Conservation Agents
Collagen Type I
Peptide Fragments
Peptides
Procollagen
collagen type I trimeric cross-linked peptide
procollagen type I carboxy terminal peptide
Teriparatide
deoxypyridinoline
Alkaline Phosphatase