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雌激素诱导小鼠骨量增加过程中的骨细胞变化:破骨细胞与骨表面的分离

Bone-cell changes in estrogen-induced bone-mass increase in mice: dissociation of osteoclasts from bone surfaces.

作者信息

Liu C C, Howard G A

机构信息

Research Service, American Lake VA Medical Center, Tacoma, Washington 98493.

出版信息

Anat Rec. 1991 Feb;229(2):240-50. doi: 10.1002/ar.1092290211.

Abstract

Early studies in certain avian and mammalian species have described estrogen-associated bone-cell changes, which were based on bone cells that were neither quantified nor identified histochemically (osteoclasts). In the experiments described here, weanling female mice were given a pharmacological dose of 17 beta-estradiol benzoate (1 mg/week) for 1 and 4 weeks, and changes in osteoclasts and osteoblasts were assessed in tibial metaphyses and diaphyses. In the proximal metaphysis, the number of osteoclasts/mm surface length was significantly reduced by estrogen at 1 week (43%) and 4 weeks (64%), which was accompanied by significant increases in the number of osteoclasts in the marrow space not in contact with bone surfaces (no./mm2: 382% and 999%, respectively). These increases, along with observations of decreased osteoclast size (19%), of changes in osteoclast morphology, and of numerous acid-phosphatase-positive fragments in the marrow space, suggest that estrogen treatment causes the dissociation and disintegration, and thus decreased activity, of osteoclasts. The above changes were accompanied by more than 48% increases in the number of trabecular osteoblasts. In the diaphysis, the number of endosteal osteoclasts was significantly decreased by estrogen at 1 week (32%), but was not significantly changed at 4 weeks. These changes were attended by significant increases in the number of osteoclasts in the marrow space not in contact with bone surfaces (no./mm2: 393% at 1 week and 342% at 4 weeks). The number of endosteal osteoblasts was also increased by estrogen at 1 week (132%), and so was the size of endosteal osteoblasts (39% at 1 week and 81% at 4 weeks). Comparable results were obtained when a lower dose of 17 beta-estradiol benzoate (20 micrograms/week) was given to ovariectomized mice. The increase in bone mass and its associated cell changes following estrogen treatment were also found in athymic nude mice, suggesting that these bone/bone cell changes are independent of the thymus.

摘要

早期针对某些鸟类和哺乳动物的研究描述了与雌激素相关的骨细胞变化,这些研究基于未进行定量分析或组织化学鉴定(破骨细胞)的骨细胞。在本文所述的实验中,给断奶雌性小鼠给予药理剂量的苯甲酸雌二醇(1毫克/周),持续1周和4周,并评估胫骨近端干骺端和骨干中破骨细胞和成骨细胞的变化。在近端干骺端,雌激素在1周(43%)和4周(64%)时使每毫米表面长度的破骨细胞数量显著减少,同时未与骨表面接触的骨髓腔中的破骨细胞数量显著增加(每平方毫米数量分别增加382%和999%)。这些增加,以及破骨细胞大小减小(19%)、破骨细胞形态变化以及骨髓腔中大量酸性磷酸酶阳性碎片的观察结果,表明雌激素治疗导致破骨细胞解离和崩解,从而使其活性降低。上述变化伴随着小梁成骨细胞数量增加超过48%。在骨干中,雌激素在1周时使骨内膜破骨细胞数量显著减少(32%),但在4周时无显著变化。这些变化伴随着未与骨表面接触的骨髓腔中的破骨细胞数量显著增加(每平方毫米数量在1周时增加393%,在4周时增加342%)。雌激素在1周时也使骨内膜成骨细胞数量增加(132%),骨内膜成骨细胞大小也增加(1周时增加39%,4周时增加81%)。给去卵巢小鼠给予较低剂量的苯甲酸雌二醇(20微克/周)时也获得了类似结果。雌激素治疗后骨量增加及其相关的细胞变化在无胸腺裸鼠中也有发现,这表明这些骨/骨细胞变化与胸腺无关。

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