Type II collagen peptide stimulates Akt leading to nuclear factor-κB activation: Its inhibition by hyaluronan

抄録

While nuclear factor (NF)-κB is a critical pathway for matrix metalloproteinase (MMP)-13 inductionin chondrocytes, intracellular upstream events for NF-κB activation by the type II collagenpeptide (CB12-II) with catabolic activities remain unclear. Hyaluronan (HA) of high molecularweight is clinically used for treatment of osteoarthritis (OA) by intra-articular injection. AlthoughHA can suppress NF-κB activation by CB12-II, it is still obscure how HA affects intracellular upstreampathways leading to NF-κB up-regulation in response to CB12-II. Thus, this study wasaimed to investigate the involvement of phosphoinositide-3-OH kinase (PI3K)/Akt in the inhibitionof CB12-II-activated NF-κB pathway by HA in OA chondrocytes. In monolayer cultures, pretreatmentwith HA of 2700 kDa significantly inhibited MMP-13 production by CB12-II-stimulatedchondrocytes. CB12-II activated Akt and NF-κB whereas HA down-regulated CB12-II-stimulatedphosphorylation of Akt and NF-κB. Inhibition studies using LY294002 revealed the requirementof PI3K/Akt pathway for CB12-II-stimulated NF-κB activation in association with MMP-13 production.Pretreatment with anti-CD44 antibody reversed the inhibitory effects of HA on CB12-IIinducedproduction of MMP-13 and activation of Akt and NF-κB. Herein, we provided the firstevidence that HA suppresses CB12-II-activated PI3K/Akt pathway leading to down-regulation ofNF-κB with diminished MMP-13 production through interaction with CD44.