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骨重塑率的变化会影响骨矿化程度。

Changes in bone remodeling rate influence the degree of mineralization of bone.

作者信息

Boivin G, Meunier P J

机构信息

INSERM Unité 403, Faculté de Médecine R. Laennec, Hôpital Edouard Herriot, Lyon, France.

出版信息

Connect Tissue Res. 2002;43(2-3):535-7. doi: 10.1080/03008200290000934.

Abstract

Mineralization of bone matrix implies two successive steps, a primary mineralization on the calcification front followed by a slow process of secondary mineralization progressively adding about 50-60% of the mineral content on bone matrix. Our model is that antiresorptive agents prolong the lifetime of the basic structural units (BSUs) by causing a marked reduction in the birth rate of basic multicellular units (BMUs), and increase the degree of mineralization of bone (DMB) by allowing a more complete secondary mineralization. Conversely, agents or events provoking an augmentation of the birthrate of BMUs and a decrease of the lifetime of BSUs lead to resorption of new BSUs before they have fully completed their secondary mineralization, leading to the presence of incompletely mineralized BSUs and a low mean DMB value, as measured by quantitative microradiography. Measurements of DMB (distribution and mean value) under circumstances with various remodeling activities favor our model. In postmenopausal osteoporotic women treated during 2 or 3 years with alendronate (10 mg/day), an increase of the mean DMB of approximately 7 to 10% was found, due to a marked reduction in the bone remodeling. In contrast, an activation of bone remodeling as in primary hyperparathyroidism lowered the mean DMB.

摘要

骨基质矿化包括两个连续的步骤,首先是在钙化前沿进行初级矿化,随后是一个缓慢的次级矿化过程,该过程会逐渐使骨基质中的矿物质含量增加约50% - 60%。我们的模型认为,抗吸收剂通过显著降低基本多细胞单位(BMUs)的生成率来延长基本结构单位(BSUs)的寿命,并通过允许更完全的次级矿化来增加骨矿化程度(DMB)。相反,促使BMUs生成率增加和BSUs寿命缩短的因素或事件会导致新的BSUs在完全完成次级矿化之前就被吸收,导致存在矿化不完全的BSUs以及较低的平均DMB值,这可通过定量显微放射照相术进行测量。在各种重塑活动情况下对DMB(分布和平均值)的测量结果支持我们的模型。在绝经后骨质疏松症女性中,使用阿仑膦酸钠(10毫克/天)进行2或3年治疗后,由于骨重塑显著减少,发现平均DMB增加了约7%至10%。相比之下,如在原发性甲状旁腺功能亢进症中出现的骨重塑激活则降低了平均DMB。

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