Short-term Effects of Raloxifene on Articular Cartilage in Ovariectomized and Trauma-induced Osteoarthritic Rabbits
碩士 === 國防醫學院 === 生物及解剖學研究所 === 98 === Osteoarthritis (OA) is characterized by slowly progression of articular cartilage degradation caused by disturbed metabolism of matrix proteins, such as type II collagen and aggrecan. After menopause, the incidence of OA affecting multiple joints increases in wo...
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ndltd-TW-098NDMC05890132015-10-13T18:16:17Z http://ndltd.ncl.edu.tw/handle/28173461884070509672 Short-term Effects of Raloxifene on Articular Cartilage in Ovariectomized and Trauma-induced Osteoarthritic Rabbits 鈣穩對卵巢切除合併外傷誘發骨關節炎大白兔之關節軟骨的短期影響 Pai-shan Hsieh 謝百善 碩士 國防醫學院 生物及解剖學研究所 98 Osteoarthritis (OA) is characterized by slowly progression of articular cartilage degradation caused by disturbed metabolism of matrix proteins, such as type II collagen and aggrecan. After menopause, the incidence of OA affecting multiple joints increases in women with greater severity, suggesting a chondroprotective effect of female sex hormone, estrogen. Estrogen acts on different tissues and organs through activation of estrogen receptors (ERs), which has been demonstrated in both subtypes (ER and ER) in articular cartilages. After menopause, ERs decreased due to estrogen deficiency, but the relative change of two ER subtypes and its effect on cartilage degradation is still unclear. The purposes of this study were to investigate possible chondroprotective effects and cellular mechanism of raloxifene, a kind of selective estrogen receptor modulator (SERM), using ovariectomized (OVX) and trauma-induced OA animal model. In the experimental rabbits, OVX and trauma surgery were performed and then followed/or not followed by oral administration of raloxifene. The synovial fluid sample from each group was collected for evaluation of C-terminal crosslinking telopeptide of type II collagen (CTX-II) levels by ELISA. The gross morphology and histological observation showed less loss of glycosaminoglycan (GAG) with raloxifene treatment in 8-week groups and less formation of clefts in 2-week groups as compared to no treatment groups. In CTX-II ELISA, four weeks after Raloxifene treatment, significant lower CTX-II expression was noted as compared to no treatment groups. Also, raloxifene treatment in 4- and 8-week groups resulted in significant decrease in CTX-II as compared to 1- and 2-week groups. Therefore, raloxifene may have chondroprotective effects in early stage OA, and the chondroprotective effects are more evident as the disease continuously progresses. Chung Shih Jia-Fwu Shyu Shyu-Yuan Hwa 史中 徐佳福 花世源 2010 學位論文 ; thesis 59 zh-TW |
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碩士 === 國防醫學院 === 生物及解剖學研究所 === 98 === Osteoarthritis (OA) is characterized by slowly progression of articular cartilage degradation caused by disturbed metabolism of matrix proteins, such as type II collagen and aggrecan. After menopause, the incidence of OA affecting multiple joints increases in women with greater severity, suggesting a chondroprotective effect of female sex hormone, estrogen. Estrogen acts on different tissues and organs through activation of estrogen receptors (ERs), which has been demonstrated in both subtypes (ER and ER) in articular cartilages. After menopause, ERs decreased due to estrogen deficiency, but the relative change of two ER subtypes and its effect on cartilage degradation is still unclear. The purposes of this study were to investigate possible chondroprotective effects and cellular mechanism of raloxifene, a kind of selective estrogen receptor modulator (SERM), using ovariectomized (OVX) and trauma-induced OA animal model. In the experimental rabbits, OVX and trauma surgery were performed and then followed/or not followed by oral administration of raloxifene. The synovial fluid sample from each group was collected for evaluation of C-terminal crosslinking telopeptide of type II collagen (CTX-II) levels by ELISA. The gross morphology and histological observation showed less loss of glycosaminoglycan (GAG) with raloxifene treatment in 8-week groups and less formation of clefts in 2-week groups as compared to no treatment groups. In CTX-II ELISA, four weeks after Raloxifene treatment, significant lower CTX-II expression was noted as compared to no treatment groups. Also, raloxifene treatment in 4- and 8-week groups resulted in significant decrease in CTX-II as compared to 1- and 2-week groups. Therefore, raloxifene may have chondroprotective effects in early stage OA, and the chondroprotective effects are more evident as the disease continuously progresses.
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author2 |
Chung Shih |
author_facet |
Chung Shih Pai-shan Hsieh 謝百善 |
author |
Pai-shan Hsieh 謝百善 |
spellingShingle |
Pai-shan Hsieh 謝百善 Short-term Effects of Raloxifene on Articular Cartilage in Ovariectomized and Trauma-induced Osteoarthritic Rabbits |
author_sort |
Pai-shan Hsieh |
title |
Short-term Effects of Raloxifene on Articular Cartilage in Ovariectomized and Trauma-induced Osteoarthritic Rabbits |
title_short |
Short-term Effects of Raloxifene on Articular Cartilage in Ovariectomized and Trauma-induced Osteoarthritic Rabbits |
title_full |
Short-term Effects of Raloxifene on Articular Cartilage in Ovariectomized and Trauma-induced Osteoarthritic Rabbits |
title_fullStr |
Short-term Effects of Raloxifene on Articular Cartilage in Ovariectomized and Trauma-induced Osteoarthritic Rabbits |
title_full_unstemmed |
Short-term Effects of Raloxifene on Articular Cartilage in Ovariectomized and Trauma-induced Osteoarthritic Rabbits |
title_sort |
short-term effects of raloxifene on articular cartilage in ovariectomized and trauma-induced osteoarthritic rabbits |
publishDate |
2010 |
url |
http://ndltd.ncl.edu.tw/handle/28173461884070509672 |
work_keys_str_mv |
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