Clinically, due to hormones changing around menopause, women have thought to have higher risk of osteoarthritis increasing with the age. In vitro studies have reported that estrogen could down-regulates the expression of matrix metalloproteinases (MMPs) and tissue inhibitor of metalloproteinase-1 (TIMP-1) in osteoarthritis chondrocytes. Bisphenol A is one of the endocrine-disrupting chemicals, which mimic the estrogen binding and confluence the hormone signaling in the body. Therefore, in this study we explore the effects of BPA and estradiol on the expression of MMP-1 and nitric oxide (NO) in vitro. The data shows that high concentration of BPA could reduce NO production, and could suppress the cell viability in SW1353 chondrosarcoma cell line and in human primary chondrocyte. But low concentration of BPA couldn’t exhibit this effect. However, in human primary chondrocyte, 0.1 nM estrogen could effectively reduce MMP-1 production that stimulation by IL-1 beta??, but 10 nM estrogen could reverse the effect, suggesting that through the NF-kappa B pathway. The present study also shows that 100 nM BPA could interfere with the protective effect of estrogen on the cartilage, and could stimulate NF-kappa B activation. This study also detect the concentration of BPA in serum and in synovial fluid by HPLC-UV, finding that BPA both exist in serum and synovial fluid of the patient who undergoes the knee replacement arthroplasty. In conclusion, BPA would be one of the factors improving the progression of osteoarthritis; otherwise, high dose of estrogen would cause the high severity of osteoarthritis.