首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Direct effects of 17 beta-estradiol on trabecular bone in ovariectomized rats.
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Direct effects of 17 beta-estradiol on trabecular bone in ovariectomized rats.

机译:17β-雌二醇对去卵巢大鼠小梁骨的直接作用。

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摘要

High-affinity nuclear binding sites for 17 beta-estradiol (17 beta E2) were recently found in bone cells; however, the mechanism by which estrogen exerts its effect on bone in vivo is still unknown. To study if estrogen acts on bone directly, we used an experimental model in which test substances are infused locally into rat femur trabecular bone. Sprague-Dawley rats weighing 150-160 g were ovariectomized (OVX) and 14 days later a polyethylene tube (1 mm in diameter) connected to an Alzet osmotic minipump was implanted into the distal femur 9 mm from the joint. 17 beta E2 (24 microliters/day at 0.01-1 nM), 17 alpha-estradiol (17 alpha E2) (24 microliters/day at 1 nM), or phosphate-buffered saline (NaCl, 8 g/liter; KCl, 0.2 g/liter; KH2PO4, 0.2 g/liter; Na2HPO4.7H2O, 2.16 g/liter) was infused for 8 days. The contralateral limb remained intact. Animals were sacrificed and bones were examined by histomorphometry. Ovariectomy caused a 50% loss in trabecular bone volume (TBV) in the secondary spongiosa (from 20.3% +/- 1.7% to 9.6% +/- 1.1%; mean +/- SEM), a 2-fold increase in osteoclast number (to 4.0 +/- 0.4 per mm), a 3-fold increase in relative resorption surfaces (to 24.8% +/- 2.9%), a 9-fold increase in osteoblast number (to 11.3 +/- 2.1 per mm), and an 8-fold increase in relative osteoid surface (to 9.6% +/- 1.7%). The local infusion of 17 beta E2 for 8 days into OVX rats (i) restored the TBV dose dependently to 75% and 85% of control (non-OVX) levels, at 0.1 nM and 1 nM 17 beta E2, respectively; (ii) decreased osteoclast number and the relative resorption surface to control (non-OVX) levels; and (iii) further increased osteoblast number and the relative osteoid surface dose dependently (by 5-fold at 1 nM 17 beta E2). Phosphate-buffered saline infusion was without effect. Infusion of 17 alpha E2 had no effect on TBV, osteoclast number, or resorption surface but increased slightly the osteoblast number and the osteoid surface. Its potency was 1/100 that of 17 beta E2. The local infusion of 17 beta E2 or 17 alpha E2 had no effect on body or uterine weight. We conclude from these findings that estrogen delivered directly to the bone of OVX rats in vivo at 2.4 and 24 fmol/day acted locally to inhibit bone resorption and stimulate bone formation.
机译:最近在骨细胞中发现了17β-雌二醇(17 beta E2)的高亲和力核结合位点。然而,雌激素在体内对骨骼发挥作用的机制仍然未知。为了研究雌激素是否直接作用于骨骼,我们使用了一种实验模型,其中将测试物质局部注入大鼠股骨小梁骨中。将体重150-160 g的Sprague-Dawley大鼠切除卵巢(OVX),14天后,将与Alzet渗透微型泵相连的聚乙烯管(直径1 mm)植入距关节9 mm的股骨远端。 17 beta E2(在0.01-1 nM时为24微升/天),17 alpha-雌二醇(17 alpha E2)(在1 nM时为24微升/天)或磷酸盐缓冲液(NaCl,8 g /升; KCl,0.2注入2克/升; KH2PO4,0.2克/升; Na2HPO4.7H2O,2.16克/升)注入8天。对侧肢体保持完整。处死动物并通过组织形态计量学检查骨骼。卵巢切除术导致继发性海绵体小梁骨体积(TBV)损失50%(从20.3%+/- 1.7%到9.6%+/- 1.1%;平均值+/- SEM),破骨细胞数量增加了2倍(至每毫米4.0 +/- 0.4),相对吸收表面增加3倍(至24.8%+/- 2.9%),成骨细胞数目增加9倍(至11.3 +/- 2.1每毫米),相对类骨质表面增加了8倍(达到9.6%+/- 1.7%)。在OVX大鼠中局部注入8天的17 beta E2(i)将TBV剂量依赖性地恢复至对照组(非OVX)水平的75%和85%,分别为0.1 nM和1 nM 17 beta E2; (ii)破骨细胞数量减少和相对吸收表面达到控制水平(非OVX); (iii)进一步增加成骨细胞数量和相对类骨质表面剂量的依赖性(在1 nM 17 beta E2时增加5倍)。磷酸盐缓冲盐水输注无效。输注17 alpha E2对TBV,破骨细胞数或吸收表面无影响,但会稍微增加成骨细胞数和类骨质表面。它的效力是17 beta E2的效力的1/100。局部输注17 beta E2或17 alpha E2对体重或子宫重量没有影响。我们从这些发现中得出结论,雌激素以2.4和24 fmol /天的速度直接递送至OVX大鼠体内的骨中,局部发挥抑制骨吸收和刺激骨形成的作用。

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