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钛表面协同作用:锶的掺入和可控无序纳米形貌优化成骨诱导。

Titanium Surface Synergy: Strontium Incorporation and Controlled Disorder Nanotopography Optimize Osteoinduction.

机构信息

Centre for the Cellular Microenvironment, School of Molecular Biosciences, College of Medical, Veterinary and Life Sciences, The Advanced Research Centre, 11 Chapel Lane, Glasgow G11 6EW, Scotland, U.K.

Department of Trauma and Orthopaedics, University Hospital Ayr, Ayr, KA6 6DX, Scotland, U.K.

出版信息

ACS Appl Mater Interfaces. 2024 Nov 20;16(46):63129-63141. doi: 10.1021/acsami.4c04117. Epub 2024 Nov 7.

DOI:10.1021/acsami.4c04117
PMID:39509174
Abstract

Osteoporotic fractures and arthritis represent a major socioeconomic health burden. Fragility fracture fixation and joint replacement are often undertaken using titanium (Ti) or Ti alloy implants. Ideally these should induce bone formation and reduce osteoclast formation. Nanoscale topographies are potent inducers of osteogenesis, and strontium (Sr) has both osteogenic and antiosteoclastic effects. We incorporated strontium into a titanium surface with an osteogenic disordered nanoscale topography. The surface comprises 120 nm diameter, 100 nm deep pits in a near-square order with deliberate offset from the center pit position up to ±50 nm, providing a pattern with an average center-center pit spacing of 300 nm (called near-square 50, NSQ50). Several surfaces were assessed, including NSQ50 alone, strontium incorporated alone, and combined, compared with control surfaces. We assessed the surfaces using a human bone marrow stromal cell (BMSC)/ bone marrow hematopoietic cell (BHSC) coculture capable of osteogenesis and osteoclastogenesis. The samples eluted Sr over long-term culture, and uptake of Sr was better with eluted Sr than with Sr added to the culture media. The NSQ50 pattern in Ti was osteogenic, and addition of Sr elution increased osteogenesis further for both flat and NSQ50 samples. Interestingly, BMSCs on all Ti samples did not secrete the receptor activator of nuclear factor kappa-Β ligand (RANKL) or macrophage colony-stimulating factor (M-CSF) while secreting osteoprotegrin (OPG) at high levels. This meant that no osteoclast formation was observed on any Ti surface. Therefore, using Sr-incorporated nanotopographical imprinting, we generated highly osteogenic Ti surfaces that inhibited osteoclast formation.

摘要

骨质疏松性骨折和关节炎是一个主要的社会经济健康负担。脆性骨折固定和关节置换通常使用钛(Ti)或 Ti 合金植入物进行。理想情况下,这些植入物应能诱导骨形成并减少破骨细胞形成。纳米级形貌是成骨的有效诱导剂,锶(Sr)具有成骨和抗破骨作用。我们将锶掺入具有成骨无序纳米形貌的钛表面。该表面由直径为 120nm、深度为 100nm 的近正方形排列的凹坑组成,凹坑中心位置故意偏移至±50nm,从而形成平均中心-中心凹坑间距为 300nm 的图案(称为近正方形 50,NSQ50)。评估了几种表面,包括单独的 NSQ50、单独掺入锶以及与对照表面相比的组合。我们使用能够成骨和破骨的人骨髓基质细胞(BMSC)/骨髓造血细胞(BHSC)共培养物评估了这些表面。样品在长期培养过程中洗脱 Sr,并且洗脱 Sr 的 Sr 摄取量优于添加到培养基中的 Sr。Ti 中的 NSQ50 图案具有成骨作用,添加 Sr 洗脱进一步增加了平板和 NSQ50 样品的成骨作用。有趣的是,所有 Ti 样品上的 BMSCs 都没有分泌核因子 kappa-B 配体(RANKL)或巨噬细胞集落刺激因子(M-CSF)受体激活剂,同时高水平分泌护骨素(OPG)。这意味着在任何 Ti 表面都没有观察到破骨细胞形成。因此,通过使用掺入 Sr 的纳米形貌印迹,我们生成了高度成骨的 Ti 表面,抑制了破骨细胞形成。

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