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联合使用雷洛昔芬-雌激素对骨骼和生殖组织的生物力学和组织学结果。

Biomechanical and histological outcome of combined raloxifene-estrogen therapy on skeletal and reproductive tissues.

机构信息

University of Bern, Institute for Surgical Technology and Biomechanics, Bern, Switzerland.

出版信息

Eur J Pharmacol. 2010 Feb 10;627(1-3):354-61. doi: 10.1016/j.ejphar.2009.11.002. Epub 2009 Nov 10.

Abstract

Estrogen replacement is a potent therapy for postmenopausal osteoporosis. However, its carcinogenic effects on breasts and the uterus limit its utilization. Raloxifene has estrogen-like effects on bones without the carcinogenic symptoms on breast or uterine tissue. Their individual effects are well characterized, but the results of their interaction remains elusive. In this work, we investigate the consequences of a combined raloxifene/estrogen therapy on bone and uterus with experimental osteoporosis. 40 Wistar rats began treatment 3 months post-ovariectomy. Estrogen and raloxifene were administered 0.03 mg/kg/day and 1.5mg/kg/day separately and together for 5 times per week for 12 weeks. Biomechanical tests and bone mineral density measurements, histology of uterus, and blood markers were analyzed. The co-administration group had higher toughness and ultimate strength than the ovariectomized controls (P<0.01). E+R had better biomechanical properties than the single treatments; yet the differences were not significant. Uterus histology signified high degeneration in the estrogen group. The raloxifene group had less degeneration but higher vascularization. Less immune reaction and vascularization were observed in the group with combined dosage than in those with individual treatments. Hence, the uterus of the combined treatment had fewer side effects than the ones that were individually treated. Mutual antagonization might be possible between raloxifene and estrogen, and that might have caused a decrease in the adverse effects. Overall, combined therapy might be useful to minimize the individual side effects of raloxifene and estrogen on the uterus and still provide bone strength and toughness.

摘要

雌激素替代疗法是治疗绝经后骨质疏松症的有效方法。然而,它对乳房和子宫的致癌作用限制了其应用。雷洛昔芬对骨骼具有类雌激素作用,而对乳腺或子宫组织没有致癌症状。它们各自的作用已得到很好的描述,但它们相互作用的结果仍不清楚。在这项工作中,我们用实验性骨质疏松症研究了联合雷洛昔芬/雌激素治疗对骨骼和子宫的影响。40 只 Wistar 大鼠在卵巢切除后 3 个月开始治疗。雌激素和雷洛昔芬分别以 0.03mg/kg/天和 1.5mg/kg/天的剂量每周 5 次给药,共 12 周。对生物力学测试和骨密度测量、子宫组织学和血液标志物进行了分析。联合给药组的韧性和极限强度均高于卵巢切除对照组(P<0.01)。E+R 的生物力学性能优于单一治疗;然而,差异并不显著。雌激素组子宫组织学显示出高度退化。雷洛昔芬组退化程度较低,但血管化程度较高。与单独治疗相比,联合剂量组观察到免疫反应和血管化较少。因此,联合治疗组的子宫副作用比单独治疗组少。雷洛昔芬和雌激素之间可能存在相互拮抗作用,这可能导致不良反应减少。总的来说,联合治疗可能有助于减少雷洛昔芬和雌激素对子宫的个体副作用,同时提供骨骼强度和韧性。

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