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基于生物信息学的体外生物材料测试模型细胞类型选择。

Bioinformatics-based selection of a model cell type for in vitro biomaterial testing.

机构信息

Department of Tissue Regeneration, MIRA Institute for Biomedical Technology and Technical Medicine, University of Twente, Drienerlolaan 5, Enschede 7500 AE, The Netherlands.

出版信息

Biomaterials. 2013 Jul;34(22):5552-61. doi: 10.1016/j.biomaterials.2013.04.001. Epub 2013 Apr 28.

Abstract

Biomaterial properties can be tailored for specific applications via systematic and high-throughput screening of biomaterial-cell interactions. However, progress in material development is often hampered by the lack of adequate in vitro testing methods, frequently due to incomplete understanding of involved in vivo mechanisms. In line with drug discovery in pharmacology, a crucial step in assay development for biomaterial screening is the identification of a target to direct the screen against. Herein, the cell type to be used for screening is of essential importance and has to be carefully chosen. So far, few attention has been put on selecting a cell type specifically suitable for in vitro testing of materials for predefined applications. In this manuscript, we describe an approach to define a suitable cell type for screening assays, for which biomaterials for bone regeneration served as example. Using a bioinformatics methodology, different cell lines are compared on three well-characterized model materials. The transcriptional profiles of MG63, iMSC, SV-HFO, hPPCT, hBPCT and SW480 cells are assessed on 3 calcium phosphate-based materials to evaluate their potential application in a screening assay. We show that MG63 is the most suitable cell line to evaluate biomaterials for bone regeneration applications, evidenced by their robust gene expression differences between the 3 model materials. The gene expression differences between the cell lines were assessed based on the overall gene expression profiles and specific subsets of genes and pathways related to osteogenesis and bone homeostasis in response to the 3 materials tested. In the next phase, this cell line will be used to identify a target correlating with in vivo biomaterial performance and henceforth to develop an in vitro screening system.

摘要

生物材料特性可通过对生物材料-细胞相互作用进行系统的高通量筛选来进行定制。然而,材料开发的进展往往受到缺乏充分的体外测试方法的阻碍,这通常是由于对涉及的体内机制缺乏了解。与药理学中的药物发现一致,生物材料筛选测定开发的关键步骤是确定一个目标来进行筛选。在此,用于筛选的细胞类型至关重要,必须仔细选择。到目前为止,很少有人关注选择一种特别适合针对预定应用的材料进行体外测试的细胞类型。在本文中,我们描述了一种定义适合筛选测定的细胞类型的方法,以骨再生用生物材料为例。使用生物信息学方法,在三种特性良好的模型材料上比较了不同的细胞系。通过对 3 种基于钙磷的材料评估 MG63、iMSC、SV-HFO、hPPCT、hBPCT 和 SW480 细胞的转录谱,评估它们在筛选测定中的潜在应用。我们表明,MG63 是评估骨再生应用生物材料的最合适的细胞系,这一点可以从它们在 3 种模型材料之间的稳健基因表达差异中得到证明。细胞系之间的基因表达差异是基于整体基因表达谱以及与成骨和骨稳态相关的特定基因和途径亚群进行评估的,这些基因和途径亚群对 3 种测试材料的反应。在下一阶段,将使用该细胞系来鉴定与体内生物材料性能相关的靶标,并开发体外筛选系统。

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