posted on 2012-04-29, 00:00authored byAlfonse T.Masi, Kalyani Nair, Brian J. Andonian, Kristina M. Prus, Joseph Kelly, Jose R. Sanchez, Jacqueline Henderson
Ankylosing spondylitis (AS) is not fully explained by inflammatory processes. Clinical, epidemiological, genetic, and course of disease features indicate additional host-related risk processes and predispositions. Collectively, the pattern of predisposition to
onset in adolescent and young adult ages, male preponderance, and widely varied severity of AS is unique among rheumatic
diseases. However, this pattern could reflect biomechanical and structural differences between the sexes, naturally occurring
musculoskeletal changes over life cycles, and a population polymorphism. During juvenile development, the body is more flexible and weaker than during adolescent maturation and young adulthood, when strengthening and stiffening considerably
increase. During middle and later ages, the musculoskeletal system again weakens. The novel concept of an innate axial myofascial
hypertonicity reflects basic echanobiological principles in human function, tissue reactivity, and pathology. However, these
processes have been little studied and require critical testing. The proposed physical mechanisms likely interact with recognized immunobiological pathways. The structural biomechanical processes and tissue reactionsmight possibly precede initiation of other
AS-related pathways. Research in the combined structural mechanobiology and immunobiology processes promises to improve understanding of the initiation and perpetuation of AS than prevailing concepts. The combined processes might better explain characteristic enthesopathic and inflammatory processes in AS.
Funding
Support for this project was provided by the Department of Medicine, University of Illinois College of Medicine at Peoria, and by the MTM Foundation.