AI Article Synopsis

  • Preclinical models of osteochondral defects (OCDs) in rats are used to study treatment effects and disease progression for osteoarthritis before moving to human trials.* -
  • Two OCD rat models with the same defect size were created in different areas of the femur: one in the trochlea and one in the medial condyle, revealing only minor gait changes and no pain difference in the trochlear defect.* -
  • Evaluations indicated that the trochlear defects led to more severe osteoarthritis changes over time, suggesting that future treatments should focus on both repairing the defects and addressing the joint degeneration.*

Article Abstract

Preclinical models of osteochondral defects (OCDs) are fundamental test beds to evaluate treatment modalities before clinical translation. To increase the rigor and reproducibility of translational science for a robust "go or no-go," we evaluated disease progression and pain phenotypes within the whole joint for two OCD rat models with same defect size (1.5 x 0.8 mm) placed either in the trochlea or medial condyle of femur. Remarkably, we only found subtle transitory changes to gaits of rats with trochlear defect without any discernible effect to allodynia. At 8-weeks post-surgery, anatomical evaluations of joint showed early signs of osteoarthritis with EPIC-microCT. For the trochlear defect, cartilage attenuation was increased in trochlear, medial, and lateral compartments of the femur. For condylar defect, increased cartilage attenuation was isolated to the medial condyle of the femur. Further, the medial ossicle showed signs of deterioration as indicated with decreased bone mineral density and increased bone surface area to volume ratio. Thus, OCD in a weight-bearing region of the femur gave rise to more advanced osteoarthritis phenotype within a unilateral joint compartment. Subchondral bone remodeling was evident in both models without any indication of closure of the articular cartilage surface. We conclude that rat OCD, placed in the trochlear or condylar region of the femur, leads to differing severity of osteoarthritis progression. As found herein, repair of the defect with fibrous tissue and subchondral bone is insufficient to alleviate onset of osteoarthritis. Future therapies using rat OCD model should address joint osteoarthritis in addition to repair itself.

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Source
http://dx.doi.org/10.1002/jor.25930DOI Listing

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