The effect of low dose intra-articular S(+) ketamine on osteoarthritis in rats: an experimental study.
Brazilian journal of anesthesiology (Elsevier) – January 01, 2024
Source: PubMed
Summary
A promising breakthrough in pain management shows that targeted ketamine treatment can significantly reduce joint pain without systemic effects. Using animal models, researchers found that small doses of S(+)-Ketamine directly injected into joints affected by osteoarthritis improved mobility and reduced pain sensitivity. While the treatment didn't reduce synovial membrane inflammation, it helped restore normal walking patterns and grip strength in treated subjects.
Abstract
This study aimed to investigate the analgesic impact of S(+)-ketamine on pain behavior and synovial inflammation in an osteoarthritis (OA) model. Animals were grouped as follows: OA-Saline (n = 24) and OA-Ketamine (n = 24), OA induced via intra-articular sodium monoiodoacetate (MIA); a Non-OA group (n = 24) served as the control. On the 7th day post OA induction, animals received either saline or S(+)-ketamine (0.5 mg.kg-1). Behavioral and histopathological assessments were conducted up to day 28. S(+)-ketamine reduced allodynia from day 7 to 28 and hyperalgesia from day 10 to 28. It notably alleviated weight distribution deficits from day 10 until the end of the study. Significant walking improvement was observed on day 14 in S(+)-ketamine-treated rats. Starting on day 14, OA groups showed grip force decline, which was countered by S(+)-ketamine on day 21. However, S(+)-ketamine did not diminish synovial inflammation. Low Intra-articular (IA) doses of S(+)-ketamine reduced MIA-induced OA pain but did not reverse synovial histopathological changes. 23115 012030/2009-05.