Computed tomography detects changes in contrast agent diffusion after collagen cross-linking typical to natural aging of articular cartilage

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RESEARCH PRODUCT

Computed tomography detects changes in contrast agent diffusion after collagen cross-linking typical to natural aging of articular cartilage

Lassi Rieppo Harri T. Kokkonen Virpi Tiitu Rami K. Korhonen Jukka S. Jurvelin Hannu M. Karjalainen Vuokko Kovanen Juha Töyräs K.a.m. Kulmala Janne T. A. Mäkelä

subject

Cartilage Articular Aging 0206 medical engineering Biomedical Engineering Contrast Media Mineralogy 02 engineering and technology Osteoarthritis Arginine Diffusion 03 medical and health sciences chemistry.chemical_compound 0302 clinical medicine Rheumatology Collagen network Ioxaglic Acid medicine Animals Orthopedics and Sports Medicine Amino Acids Pentosidine Computed tomography 030203 arthritis & rheumatology Pyridinoline biology Threose Chemistry Lysine Cartilage Cartilage aging Delayed Gadolinium Enhanced Magnetic Resonance Imaging of Cartilage Patella medicine.disease Cartilage injury 020601 biomedical engineering Hindlimb Contrast agent medicine.anatomical_structure Proteoglycan Case-Control Studies biology.protein Cattle Collagen Tetroses Tomography X-Ray Computed Cross-linking Biomedical engineering

description

SummaryObjectiveThe effect of threose-induced collagen cross-linking on the mechanical and diffusive properties of cartilage was investigated in vitro. In particular, we investigated the potential of Contrast Enhanced Computed Tomography (CECT) to detect changes in articular cartilage after increased collagen cross-linking, which is an age-related phenomenon.MethodsOsteochondral plugs (Ø=6.0mm, n=28) were prepared from intact bovine patellae (n=7). Two of the four adjacent samples, prepared from each patella, were treated with threose to increase the collagen cross-linking, while the other two specimen served as paired controls. One sample pair was mechanically tested and then mechanically injured using a material testing device. Contrast agent [ioxaglate (Hexabrix™)] diffusion was imaged in the other specimen pair for 25h using CECT. Water fraction, collagen and proteoglycan content, collagen network architecture and the amount of cross-links [hydroxylysyl pyridinoline (HP), lysyl pyridinoline (LP) and pentosidine (Pent)] of the samples were also determined.ResultsCartilage collagen cross-linking, both Pent and LP, were significantly (P<0.001) increased due to threose treatment. CECT could detect the increased cross-links as the contrast agent penetration and the diffusion flux were significantly (P<0.05) lower in the threose treated than in untreated samples. The equilibrium modulus (+164%, P<0.05) and strain dependent dynamic modulus (+47%, P<0.05) were both significantly greater in the threose treated samples than in reference samples, but there was no association between the initial dynamic modulus and the threose treatment. The water fraction, proteoglycan and collagen contents, as well as collagen architecture, were not significantly altered by the threose treatment.ConclusionsTo conclude, the CECT technique was found to be sensitive at detecting changes in cartilage tissue due to increased collagen cross-linking. This is important since increased cross-linking has been proposed to be related to the increased injury susceptibility of tissue.

year	journal	country	edition	language
2011-10-01	Osteoarthritis and Cartilage

https://doi.org/10.1016/j.joca.2011.07.008