Metabolic dysregulation accelerates injury-induced joint degeneration, driven by local inflammation; an in vivo rat study

Huub M. de Visser, Simon C. Mastbergen*, Anne E. Kozijn, Katja Coeleveld, Behdad Pouran, Mattie H. van Rijen, Floris P.J.G. Lafeber, Harrie Weinans

*Corresponding author for this work

Research output: Contribution to journalArticleAcademicpeer-review

Abstract

Evidence is growing for the existence of an obesity-related phenotype of osteoarthritis in which low-grade inflammation and a disturbed metabolic profile play a role. The contribution of an obesity-induced metabolic dysbalance to the progression of the features of osteoarthritis upon mechanically induced cartilage damage was studied in a rat in vivo model. Forty Wistar rats were randomly allocated 1:1 to a standard diet or a high-fat diet. After 12 weeks, in 14 out of 20 rats in each group, cartilage was mechanically damaged in the right knee joint. The remaining six animals in each group served as controls. After a subsequent 12 weeks, serum was collected for metabolic state, subchondral bone changes assessed by μCT imaging, osteoarthritis severity determined by histology, and macrophage presence assessed by CD68 staining. The high-fat diet increased statistically all relevant metabolic parameters, resulting in a dysmetabolic state and subsequent synovial inflammation, whereas cartilage degeneration was hardly influenced. The high-fat condition in combination with mechanical cartilage damage resulted in a clear statistically significant progression of the osteoarthritic features, with increased synovitis and multiple large osteophytes. Both the synovium and osteophytes contained numerous CD68 positive cells. It is concluded that a metabolic dysbalance due to a high-fat diet increases joint inflammation without cartilage degeneration. The dysmetabolic state clearly accelerates progression of osteoarthritis upon surgically induced cartilage damage supported by inflammatory responses as demonstrated by histology and increased CD68 expressing cells localized on the synovial membrane and osteophytes.

Original languageEnglish
Pages (from-to)881-890
Number of pages10
JournalJournal of Orthopaedic Research
Volume36
Issue number3
DOIs
Publication statusPublished - Mar 2018

Keywords

  • Animal model
  • Inflammation
  • Metabolic syndrome
  • Osteoarthritis
  • Synovitis

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