Subchondral bone remodelling and osteoarthritis

ar37131478-6354 Meeting abstract Subchondral bone remodelling and osteoarthritis Román-BlasAJorge CastañedaSantos LargoRaquel Herrero-BeaumontGabriel

Bone and Joint Research Unit, Service of Rheumatology, IIS Fundación Jiménez Díaz, Universidad Autónoma, Madrid, Spain

Department of Rheumatology, Hospital de la Princesa, IIS Princesa, Universidad Autónoma, Madrid, Spain

Arthritis Research & Therapy Proceedings of Osteorheumatology 2011: International Congress on Bone Involvement in ArthritisGerolamo Bianchi and Luigi SinigagliaMeeting abstractsOsteoRheumatology 2011, International Congress on Bone Involvement in ArthritisSanta Margherita Ligure, Italy

13-14 October 2011

http://www.osteo-rheumatology.it1478-6354 2012 14 Suppl 2 A6 http://arthritis-research.com/content/14/S2/A6 10.1186/ar3713 832012 2012Román-Blas et al; licensee BioMed Central Ltd.This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

Osteoarthritis (OA) emerges of the inharmonious functioning of joint tissues, particularly subchondral bone (SB) and articular cartilage that are two mechanically and biologically intertwined tissues 1 . Thus, biomechanical, biochemical and/or genetic alterations affecting any joint tissue may cause anomalous intra-articular stresses and subsequent tissue damage associated to a failure of repair 2 . Specific anatomical regions have been described in the bone underlying joint cartilage, including the subchondral cortical plate, subchondral trabecular bone and sub-articular bone 3 . Each region likely contributes differently to cartilage pathology. However, a lack of clear boundaries between these tissues by current imaging techniques generates some confusion in their study and thorough research will help to improve our understanding of SB properties. In addition, bone at the joint margins is markedly active since is the site of osteophyte development in OA. The close relationship between SB and joint cartilage evokes an unanswered question with valuable therapeutic implications 4 . In this context, the relationship among SB microstructure and remodeling, and cartilage destruction becomes important.

Yet, it remains controversial whether SB alterations precede the cartilage damage or they further appear during the evolution of the disease. In fact, SB remodeling abnormalities, especially increased bone turnover, have been detected early in the evolution of some forms of OA in animal models 5 6 and humans 7 8 . On the other hand, OA and systemic osteoporosis (OP) share a paradoxical relationship, being probable that high as well as low bone mass conditions result in induction and/or OA progression 4 . Interestingly, improving SB integrity showed to reduce the progression of cartilage damage in an animal model of OA preceded by OP 9 . Therefore, both bone mass phenotypes may be considered risk factors for OA initiation. The presence of other risk factors such as skeletal shape abnormalities, joint overload or obesity may have a synergistic effect for OA initiation. In addition, inflammatory mediators released by the articular cartilage may lead to SB loss by increasing bone remodeling in OA. Accordingly, OA treatment goals must consider the improvement of SB integrity. This therapeutic approach should be individualized depending on the patient BMD status and OA phenotype, and subsequently the use of drugs should also be individualized for each patient 10 . Recent findings suggest that the same drugs could be useful for treating simultaneously both processes, at least in a subgroup of patients with OA and concomitant OP.

Articular cartilage and subchondral bone in the pathogenesis of osteoarthritisGoldringMBGoldringSRAnn NY Acad Sci2010119223023710.1111/j.1749-6632.2009.05240.x20392241OARSI-FDA initiative: defining the disease state of osteoarthritisLaneNEBrandtKHawkerGOsteoarthritis Cartilage20111947848210.1016/j.joca.2010.09.01321396464Anatomy and physiology of the mineralized tissues: role in the pathogenesis of osteoarthrosisBurrDBOsteoarthritis Cartilage200412Suppl AS20S3014698637Bone mineral density and joint cartilage: four clinical settings of a complex relationship in osteoarthritisHerrero-BeaumontGRoman-BlasJALargoRAnn Rheum Dis2011701523152510.1136/ard.2011.15123321742638Evidence of early subchondral bone changes in the meniscectomized guinea pig. A densitometric study using dual-energy X-ray absorptiometry subregional analysisPastoureauPCChomelACBonnetJOsteoarthritis Cartilage1999746647310.1053/joca.1999.024110489319Characterization of articular cartilage and subchondral bone changes in the rat anterior cruciate ligament transection and meniscectomized models of osteoarthritisHayamiTPickarskiMZhuoYBone20063823424310.1016/j.bone.2005.08.00716185945A decreased subchondral trabecular bone tissue elastic modulus is associated with pre-arthritic cartilage damageDayJSDingMvan der LindenJCJ Orthop Res20011991491810.1016/S0736-0266(01)00012-211562141Upper extremity bone mass and osteoarthritis of the knees: data from the Baltimore Longitudinal Study of AgingHochbergMCLethbridge-CejkuMScottWWJrJ Bone Miner Res1995104324387785465Improving subchondral bone integrity reduces progression of cartilage damage in experimental osteoarthritis preceded by osteoporosisBellidoMLugoLRoman-BlasJAOsteoarthritis Cartilage2011191228123610.1016/j.joca.2011.07.00321820069Subchondral bone as a key target for osteoarthritis treatmentCastañedaSRoman-BlasJALargoRBiochem Pharmacol20118331532321964345