Clinical evaluation of medicinal products for acceleration of fracture healing in patients with osteoporosis

Jörg Goldhahn; Wim H Scheele; Bruce H Mitlak; Eric Abadie; Per Aspenberg; Peter Augat; Maria-Luisa Brandi; Nansa Burlet; Arkadi Chines; Pierre D Delmas; Isabelle Dupin-Roger; Dominique Ethgen; Beate Hanson; Florian Hartl; John A Kanis; Reshma Kewalramani; Andrea Laslop; David Marsh; Sif Ormarsdottir; René Rizzoli; Art Santora; Gerhard Schmidmaier; Michael Wagener; Jean-Yves Reginster

doi:10.1016/j.bone.2008.04.017

Clinical evaluation of medicinal products for acceleration of fracture healing in patients with osteoporosis

Bone. 2008 Aug;43(2):343-347. doi: 10.1016/j.bone.2008.04.017. Epub 2008 May 7.

Authors

Jörg Goldhahn¹, Wim H Scheele², Bruce H Mitlak³, Eric Abadie⁴, Per Aspenberg⁵, Peter Augat⁶, Maria-Luisa Brandi⁷, Nansa Burlet⁸, Arkadi Chines², Pierre D Delmas⁹, Isabelle Dupin-Roger¹⁰, Dominique Ethgen¹¹, Beate Hanson¹², Florian Hartl¹³, John A Kanis¹⁴, Reshma Kewalramani¹⁵, Andrea Laslop¹⁶, David Marsh¹⁷, Sif Ormarsdottir¹⁸, René Rizzoli¹⁹, Art Santora²⁰, Gerhard Schmidmaier²¹, Michael Wagener²², Jean-Yves Reginster²³

Affiliations

¹ Schulthess Clinic Zurich and Clinical Priority Program "Fracture Fixation in Osteoporotic, Bone" of AO Foundation, Davos, Switzerland. Electronic address: joerg.goldhahn@kws.ch.
² Wyeth Research, Cambridge, MA, USA.
³ Eli Lilly and Company, Indianapolis, IN, USA.
⁴ Département de l'Enregistrement et des Etudes Cliniques, AFSSAPS, Saint Denis, France.
⁵ Division of Orthopedics and Sports Medicine, Department of Neuroscience and Locomotion, Faculty of Health Sciences, Linköping University, Linkoping, Sweden.
⁶ Biomechanics Laboratory Paracelsus Medical University, Salzburg, Austria; Biomechanics Laboratory Paracelsus Medical University, Salzburg, Austria.
⁷ Metabolic Bone Unit, Laboratory of Molecular Genetics, Department of Internal Medicine, University of Florence, Florence, Italy.
⁸ International Osteoporosis Foundation, Nyon, Switzerland.
⁹ Hôpital Edouard Herriot, Lyon, France.
¹⁰ IRIS-Servier, Paris, France.
¹¹ Clinical Development, GSK, Philadelphia, PA, USA.
¹² AO Clinical Investigation and Documentation, Davos Platz, Davos, Switzerland.
¹³ F. Hoffmann-La Roche AG, Basel, Switzerland.
¹⁴ Centre for Metabolic Bone Diseases (WHO Collaborating Centre), University of Sheffield Medical School, Sheffield, UK.
¹⁵ Amgen Inc., Thousand Oaks, CA, USA.
¹⁶ AGES PharmMed, Vienna, Austria.
¹⁷ Queen's University Belfast, Division of Surgery and Perioperative Care, Department of Orthopaedic Surgery, Musgrave Park Hospital, Stockman's Lane, Belfast, Ulster, UK.
¹⁸ Senior Expert, Icelandic Medicines Control Agency, Seltjarnarnes, Iceland.
¹⁹ Centre Collaborateur de l'Oms pour la prevention de l'osteoporose, Geneva, Switzerland.
²⁰ Merck & Co., Whitehouse Station, NJ, USA.
²¹ Center for Musculoskeletal Surgery, Charité-Universitätsmedizin Berlin, Germany.
²² Novartis Pharma AG, Basel, Switzerland.
²³ Department of Public Health Sciences, University of Liège, Liège, Belgium, Chairman GREES, President ESCEO.

PMID: 18544475
DOI: 10.1016/j.bone.2008.04.017

Abstract

Pre-clinical studies indicate that pharmacologic agents can augment fracture union. If these pharmacologic approaches could be translated into clinical benefit and offered to patients with osteoporosis or patients with other risks for impaired fracture union (e.g. in subjects with large defects or open fractures with high complication rate), they could provide an important adjunct to the treatment of fractures. However, widely accepted guidelines are important to encourage the conduct of studies to evaluate bioactive substances, drugs, and new agents that may promote fracture union and subsequent return to normal function. A consensus process was initiated to provide recommendations for the clinical evaluation of potential therapies to augment fracture repair in patients with meta- and diaphyseal fractures. Based on the characteristics of fracture healing and fixation, the following study objectives of a clinical study may be appropriate: a) acceleration of fracture union, b) acceleration of return to normal function and c) reduction of fracture healing complications. The intended goal(s) should determine subsequent study methodology. While an acceleration of return to normal function or a reduction of fracture healing complications in and of themselves may be sufficient primary study endpoints for a phase 3 pivotal study, acceleration of fracture union alone is not. Radiographic evaluation may either occur at multiple time points during the healing process with the aim of measuring the time taken to reach a defined status (e.g. cortical bridging of three cortices or disappearance of fracture lines), or could be obtained at a single pre-determined timepoint, were patients are expected to reach a common clinical milestone (i.e. pain free full weight-bearing in weight-bearing fracture cases). Validated Patient Reported Outcomes (PRO's) measures will need to support the return to normal function co-primary endpoints. If reduction of complication rate (e.g. non-union) is the primary objective, the anticipated complications must be defined in the study protocol, along with their possible associations with the specified fracture type and fixation device. The study design should be randomized, parallel, double-blind, and placebo-controlled, and all fracture subjects should receive a standardized method of fracture fixation, defined as Standard of Care.

Publication types

Review

MeSH terms

Clinical Trials as Topic
Drug Evaluation, Preclinical*
Fracture Healing*
Humans
Osteoporosis / drug therapy*
Pharmaceutical Preparations*
Treatment Outcome

Substances

Pharmaceutical Preparations