In vitro toxicity of biomaterials determined with cell density, total protein, cell cycle distribution and adenine nucleotides.

A P Wieslander, M K Nordin, B Hansson, B Baldetorp, P T Kjellstrand
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引用次数: 8

Abstract

Inhibition of cell growth is the most commonly used endpoint for in vitro toxicity of biomaterials. The use of several different endpoints might however generate more information concerning the nature of the toxicity. Thus, we examined the toxicity of two biomaterials, Polyvinylchloride (PVC) and Polyoximethene (POM), with different selected endpoints. The influence of cell growth on these endpoints was also investigated. Water extracts from the polymeric materials were tested on the continuous cell line L-929. Cell density, total protein, total protein per cell, fraction of cells in G0/G1- or S-phase, the concentration of ATP, ADP and AMP were used as endpoints. The PVC material did not significantly influence any of these endpoints until after 72 hours of exposure and the main part of the toxicity at 72 hours was related to higher proliferation rate in control cultures. After the cells had been incubated for 8 hour with POM the main toxic effect was on the energy parameters. In conclusion the PVC material was less toxic than the POM material. Our results also implies that the choice of endpoint will influence the evaluation of cytotoxicity.

用细胞密度、总蛋白、细胞周期分布和腺嘌呤核苷酸测定生物材料的体外毒性。
抑制细胞生长是生物材料体外毒性研究中最常用的终点。然而,使用几个不同的终点可能会产生更多关于毒性性质的信息。因此,我们研究了两种生物材料的毒性,聚氯乙烯(PVC)和聚氧甲烷(POM),选择了不同的终点。还研究了细胞生长对这些终点的影响。在L-929连续细胞系上测试了聚合物材料的水提取物。以细胞密度、总蛋白、每细胞总蛋白、G0/G1期或s期细胞比例、ATP、ADP和AMP浓度为终点。PVC材料直到暴露72小时后才对这些终点产生显著影响,72小时毒性的主要部分与对照培养物中较高的增殖率有关。经POM孵育8小时后,细胞的毒性主要表现在能量参数上。综上所述,PVC材料的毒性低于POM材料。我们的结果还表明,终点的选择将影响细胞毒性的评价。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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