| Literature DB >> 27312650 |
Rondinelle R Castro1, Christine Maria M Silva2, Rodolfo M Nunes2, Pablyana L R Cunha3, Regina Celia M de Paula3, Judith P A Feitosa3, Virgínia C C Girão4, Margarida M L Pompeu5, José Alberto D Leite6, Francisco A C Rocha7.
Abstract
Protein-free guar gum (DGG) was oxidized (DGGOX) or sulfated (DGGSU) by insertion of new groups in C-6 (manose) and C-6 (galactose), for DGGOX and DGGSU, respectively. Rats were subjected to anterior cruciate ligament transection (ACLT) of the knee, joint pain recorded using the articular incapacitation test, and the analgesic effect of intraarticular 100μg DGG, DGGOX or DGGSU solutions at days 4-7 was evaluated. Other groups received DGG or saline weekly, from days 7 to 70 and joint damage assessed using histology and biochemistry as the chondroitin sulfate (CS) content of cartilage. The molar mass of CS samples was obtained by comparing their relative electrophoretic mobility to standard CS. DGG but not DGGOX or DGGSU significantly inhibited joint pain. DGG significantly reversed the increase in CS, its reduced electrophoretic mobility, and histological changes following ACLT, as compared to vehicle. Structural integrity accounts for DGG benefits in experimental osteoarthritis.Entities:
Keywords: Chonsurid (PUBCHEM CID: 24766); Galactomannan (PUBCHEM CID: 439336); Guar gum; Osteoarthritis; Oxidation; Pain; Sulfation
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Year: 2016 PMID: 27312650 DOI: 10.1016/j.carbpol.2016.05.031
Source DB: PubMed Journal: Carbohydr Polym ISSN: 0144-8617 Impact factor: 9.381