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钛表面的高性能支架:通过细胞自主的 BMP 信号促进球蛋白层纤维蛋白原促进成骨细胞分化和矿化。

High-performance scaffolds on titanium surfaces: osteoblast differentiation and mineralization promoted by a globular fibrinogen layer through cell-autonomous BMP signaling.

机构信息

Department of Dental Materials, Matsumoto Dental University, 1780 Hiro-oka Gobara, Shiojiri, Nagano 399-0781, Japan.

Institute for Oral Science, Matsumoto Dental University, 1780 Hiro-oka Gobara, Shiojiri, Nagano 399-0781, Japan.

出版信息

Mater Sci Eng C Mater Biol Appl. 2015 Jan;46:86-96. doi: 10.1016/j.msec.2014.10.025. Epub 2014 Oct 13.

Abstract

Titanium has been widely used as a dental implant material. However, it takes several months for the implant body to bind with the jawbone. To develop new bioactive modification on titanium surfaces to achieve full osseointegration expeditiously, we used fibrinogen and fibronectin as bioactive scaffolds on the titanium plate, which are common extracellular matrix (ECM) proteins. We analyzed the features of the surface of ECM-modified titanium plates by atomic force microscopy and Fourier transform infrared spectrophotometry. We also evaluated the effect of ECM modification on promoting the differentiation and mineralization of osteoblasts on these surfaces. Fibrinogen had excellent adsorption on titanium surfaces even at low concentrations, due to the binding ability of fibrinogen via its RGD motif. The surface was composed of a fibrinogen monolayer, in which the ratio of β-sheets was decreased. Osteoblast proliferation on ECM-modified titanium surface was significantly promoted compared with titanium alone. Calcification on the modified surface was also accelerated. These ECM-promoting effects correlated with increased expression of bone morphogenetic proteins (BMPs) by the osteoblasts themselves and were inhibited by Noggin, a BMP inhibitor. These results suggest that the fibrinogen monolayer-modified titanium surface is recognized as bioactive scaffolds and promotes bone formation, resulting in the acceleration of osseointegration.

摘要

钛已被广泛用作牙科植入物材料。然而,植入体与颌骨结合需要数月的时间。为了在钛表面开发新的生物活性改性以迅速实现完全骨整合,我们将纤维蛋白原和纤维连接蛋白用作钛板上的生物活性支架,它们是常见的细胞外基质 (ECM) 蛋白。我们通过原子力显微镜和傅里叶变换红外光谱法分析了 ECM 改性钛板表面的特征。我们还评估了 ECM 改性对促进成骨细胞在这些表面上的分化和矿化的影响。纤维蛋白原通过其 RGD 基序具有出色的与钛表面的结合能力,即使在低浓度下也能极好地吸附在钛表面上。表面由纤维蛋白原单层组成,其中β-折叠的比例降低。与单独的钛相比,成骨细胞在 ECM 改性钛表面上的增殖明显增加。改性表面上的钙化也得到了加速。这些 ECM 促进作用与成骨细胞自身表达的骨形态发生蛋白 (BMPs) 增加有关,并且被 BMP 抑制剂 Noggin 抑制。这些结果表明纤维蛋白原单层改性钛表面被认为是生物活性支架,并促进骨形成,从而加速骨整合。

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