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维生素D缺乏大鼠脱矿同种异体骨基质中促有丝分裂和骨诱导活性降低的证明。

Demonstration of reduced mitogenic and osteoinductive activities in demineralized allogeneic bone matrix from vitamin D-deficient rats.

作者信息

Turner R T, Farley J, Vandersteenhoven J J, Epstein S, Bell N H, Baylink D J

机构信息

Veterans Administration Medical Center, Charleston, South Carolina 29403.

出版信息

J Clin Invest. 1988 Jul;82(1):212-7. doi: 10.1172/JCI113573.

Abstract

Osteoinduction is the formation of ectopic bone that follows implantation of demineralized allogeneic bone matrix (DABM) and is believed to be secondary to the release of associated inductive factors from bone matrix. To clarify the role of vitamin D in osteoinduction, we implanted DABM from vitamin D-deficient rats (-D rats) into normal rats (+D rats). Because mitogens and osteocalcin might be involved in osteoinduction, these were measured. Mitogenic activity in extracts from mineralized allogeneic bone matrix (ABM) and DABM from both +D and -D rats was determined with an assay that utilizes monolayer cultures of embryonic chick calvarial cells. Osteocalcin in serum and DABM was measured by radioimmunoassay. DABM from -D rats did not promote osteoinduction as effectively as DABM from +D rats. Resorption of implant matrix from -D rats was diminished compared with resorption of matrix from +D rats (P less than 0.01), and the decrease was attributed to a corresponding decrease in the number of osteoclasts in the implants (P less than 0.02). Bone formation (P less than 0.01) and total implant mineralization (P less than 0.001) were significantly reduced in implants from -D rats, and the reductions corresponded with a decline in the number of osteoblasts (P less than 0.05). Mitogenic activity in DABM from +D rats was only slightly decreased as compared with activity in ABM, but DABM from -D rats contained significantly less activity (P less than 0.001). No mitogenic activity was identified in implants of DABM from either +D or -D rats 3 wk after implantation. Serum osteocalcin was significantly higher in -D as compared with +D animals. In contrast, the concentrations of osteocalcin in DABM from the two groups of animals were not significantly different from each other. These findings indicate that the diminished osteoinductive activity of DABM from -D rats results from deficiency of one or more mitogenic factors that are essential for inducing the proliferation and differentiation of bone cells at the implant site and that osteocalcin does not play a role in this regard.

摘要

骨诱导是在植入脱矿异体骨基质(DABM)后异位骨的形成,并且被认为继发于骨基质中相关诱导因子的释放。为了阐明维生素D在骨诱导中的作用,我们将来自维生素D缺乏大鼠(-D大鼠)的DABM植入正常大鼠(+D大鼠)体内。因为有丝分裂原和骨钙素可能参与骨诱导,所以对它们进行了检测。利用胚胎鸡颅骨细胞单层培养的检测方法,测定了来自+D和-D大鼠的矿化异体骨基质(ABM)和DABM提取物中的有丝分裂活性。通过放射免疫分析法测定血清和DABM中的骨钙素。来自-D大鼠的DABM促进骨诱导的效果不如来自+D大鼠的DABM。与来自+D大鼠的基质吸收相比,来自-D大鼠的植入物基质吸收减少(P小于0.01),这种减少归因于植入物中破骨细胞数量的相应减少(P小于0.02)。来自-D大鼠的植入物中的骨形成(P小于0.01)和植入物总矿化(P小于0.001)显著降低,并且这些降低与成骨细胞数量的下降相对应(P小于0.05)。与ABM中的活性相比,来自+D大鼠的DABM中的有丝分裂活性仅略有下降,但来自-D大鼠的DABM中的活性显著较低(P小于0.001)。植入后3周,来自+D或-D大鼠的DABM植入物中均未发现有丝分裂活性。与+D动物相比,-D动物的血清骨钙素显著更高。相比之下,两组动物的DABM中骨钙素的浓度彼此之间没有显著差异。这些发现表明,来自-D大鼠的DABM骨诱导活性降低是由于一种或多种有丝分裂因子的缺乏,这些因子对于诱导植入部位骨细胞的增殖和分化至关重要,并且骨钙素在这方面不起作用。

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