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ASSAY and Drug Development Technologies
In Vitro, Ex Vivo, and In Vivo Methodological Approaches for Studying Therapeutic Targets of Osteoporosis and Degenerative Joint Diseases: How Biomarkers Can Assist?
To cite this article:
S. Schaller, K. Henriksen, P. Hoegh-Andersen, B.C. Søndergaard, E.U. Sumer, L.B. Tanko, P. Qvist, M.A. Karsdal.
ASSAY and Drug Development Technologies.
October 2005,
3(5): 553-580.
doi:10.1089/adt.2005.3.553.
S. Schaller Pharmos Bioscience A/S, Herlev, Denmark. K. Henriksen Pharmos Bioscience A/S, Herlev, Denmark. P. Hoegh-Andersen Pharmos Bioscience A/S, Herlev, Denmark. B.C. Søndergaard Nordic Bioscience Diagnostics A/S, Herlev, Denmark. E.U. Sumer Nordic Bioscience Diagnostics A/S, Herlev, Denmark. L.B. Tanko Center for Clinical and Basic Research, Ballerup, Denmark. P. Qvist Nordic Bioscience Diagnostics A/S, Herlev, Denmark. M.A. Karsdal, Ph.D.Pharmos Bioscience A/S, Herlev, Denmark. Nordic Bioscience Diagnostics A/S, Herlev, Denmark. Although our approach to the clinical management of osteoporosis (OP) and degenerative joint diseases (DJD)—major causes of disability and morbidity in the elderly—has greatly advanced in the past decades, curative treatments that could bring ultimate solutions have yet to be found or developed. Effective and timely development of candidate drugs is a critical function of the availability of sensitive and accurate methodological arsenal enabling the recognition and quantification of pharmacodynamic effects. The established concept that both OP and DJD arise from an imbalance in processes of tissue formation and degradation draws attention to need of establishing in vitro, ex vivo, and in vivo experimental settings, which allow obtaining insights into the mechanisms driving increased bone and cartilage degradation at cellular, organ, and organism levels. When addressing changes in bone or cartilage turnover at the organ or organism level, monitoring tools adequately reflecting the outcome of tissue homeostasis become particularly critical. In this context, bioassays targeting the quantification of various degradation and formation products of bone and cartilage matrix elements represent a useful approach. In this review, a comprehensive overview of widely used and recently established in vitro, ex vivo, and in vivo setups is provided, which in many cases effectively take advantage of the potentials of biomarkers. In addition to describing and discussing the advantages and limitations of each assay and their methods of evaluation, we added experimental and clinical data illustrating the utility of biomarkers for these methodological approaches.  This paper was cited by:Low-dose transdermal estradiol induces breast density and heterogeneity changes comparable to those of raloxifene Mads Nielsen, Jakob Raundahl, Paola C. Pettersen, Marco Loog, Gopal Karemore, Morten A. Karsdal, Claus Christiansen Menopause. Aug 2009, Vol. 16, No. 4: 785-791 CrossRef Influence of food intake on the bioavailability and efficacy of oral calcitonin Morten A. Karsdal, Inger Byrjalsen, Möise Azria, Michel Arnold, Les Choi, Bente J. Riis, Claus Christiansen British Journal of Clinical Pharmacology. May 2009, Vol. 67, No. 4: 413-420 CrossRef The effects of oral calcitonin on bone collagen maturation: implications for bone turnover and quality M. A. Karsdal, I. Byrjalsen, D. J. Leeming, P. D. Delmas, C. Christiansen Osteoporosis International. Oct 2008, Vol. 19, No. 9: 1355-1361 CrossRef Serum biomarkers as signals for risk and severity of work-related musculoskeletal injury Stephen J Carp, Ann E Barr, Mary F Barbe Biomarkers in Medicine. Mar 2008, Vol. 2, No. 1: 67-79 CrossRef Cartilage proteomics: Challenges, solutions and recent advances Richard Wilson, John F. Bateman PROTEOMICS – Clinical Applications. 2008, Vol. 2, No. 2: 251 CrossRef The chemical biomarkers C2C, Coll2-1, and Coll2-1NO2 provide complementary information on type II collagen catabolism in healthy and osteoarthritic mice L. G. Ameye, M. Deberg, M. Oliveira, A. Labasse, J. M. Aeschlimann, Y. Henrotin Arthritis & Rheumatism. Nov 2007, Vol. 56, No. 10: 3336-3346 CrossRef Induction of increased cAMP levels in articular chondrocytes blocks matrix metalloproteinase–mediated cartilage degradation, but not aggrecanase-mediated cartilage degradation Morten Asser Karsdal, Eren Ufuk Sumer, Helle Wulf, Suzi H. Madsen, Claus Christiansen, Amanda J. Fosang, Bodil-Cecilie Sondergaard Arthritis & Rheumatism. Jun 2007, Vol. 56, No. 5: 1549-1558 CrossRef Matrix metalloproteinase and aggrecanase generated aggrecan fragments: implications for the diagnostics and therapeutics of destructive joint diseases Eren U. Sumer, Per Qvist, László B. Tankó Drug Development Research. Mar 2007, Vol. 68, No. 1: 1-13 CrossRef Strontium ranelate: a new alternative treatment for postmenopausal osteoporosis Morten A Karsdal, Claus Christiansen Future Rheumatology. Jan 2007, Vol. 1, No. 6: 683-692 CrossRef An update on biomarkers of bone turnover and their utility in biomedical research and clinical practice D. J. Leeming, P. Alexandersen, M. A. Karsdal, P. Qvist, S. Schaller, L. B. Tankó European Journal of Clinical Pharmacology. Nov 2006, Vol. 62, No. 10: 781-792 CrossRef |
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