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氧化锌颗粒物质需要与细胞接触才能对人结肠癌细胞产生毒性。

ZnO particulate matter requires cell contact for toxicity in human colon cancer cells.

机构信息

Department of Pharmacology and Toxicology, University of Utah, L. S. Skaggs Pharmacy, Room 201, 30 S 2000 East, Salt Lake City, Utah 84112, USA.

出版信息

Chem Res Toxicol. 2010 Apr 19;23(4):733-9. doi: 10.1021/tx900203v.

Abstract

There is ongoing concern regarding the toxicity of nanoparticles with sizes less than 100 nm as compared to larger particles of the same nominal substance. Two commercial ZnO types, one sold as a 8-10 nm powder and the other described as -325 mesh (<44 mum) powder, were evaluated in human colon-derived RKO cells. The powders had a volume-to-surface area ratio equivalent to 40 and 330 nm spheres, respectively. Both materials formed micrometer-sized agglomerates in cell culture media. The nanosized ZnO was more cytotoxic than the micrometer-sized ZnO with LC(50) values of 15 +/- 1 and 29 +/- 4 mug/cm(2), respectively. Transfer of Zn from the solid phase to the cell culture media in the presence of RKO cells was time- and concentration-dependent. However, direct particle-cell contact was required for RKO cell cytotoxicity, and the toxicity of particles was independent of the amount of soluble Zn in the cell culture media. The mechanism of cell death includes the disruption of mitochondrial function. Robust markers of apoptosis, Annexin V staining, loss of mitochondrial potential, and increased generation of superoxide were observed when cells were treated with ZnO particulate matter but not when treated with comparable concentration of a soluble Zn salt. Both ZnO samples induced similar mechanisms of toxicity, but there was a statistically significant increase in potency per unit mass with the smaller particles.

摘要

人们一直关注小于 100nm 的纳米颗粒的毒性,认为其毒性要大于相同名义物质的较大颗粒。两种商业 ZnO 类型,一种以 8-10nm 粉末形式出售,另一种被描述为-325 目(<44μm)粉末,在人结肠衍生的 RKO 细胞中进行了评估。这些粉末的体积-表面积比分别相当于 40nm 和 330nm 球体。两种材料在细胞培养基中均形成了微米级的聚集体。纳米 ZnO 比微米 ZnO 的细胞毒性更大,LC(50)值分别为 15±1 和 29±4μg/cm(2)。在 RKO 细胞存在的情况下,Zn 从固相向细胞培养基中的转移是时间和浓度依赖性的。然而,RKO 细胞的细胞毒性需要直接的颗粒-细胞接触,并且颗粒的毒性与细胞培养基中可溶性 Zn 的量无关。细胞死亡的机制包括线粒体功能的破坏。当用 ZnO 颗粒处理细胞时,观察到 Annexin V 染色、线粒体电位丧失和超氧生成增加等凋亡的明显标志,但当用可溶性 Zn 盐处理时则没有观察到这些标志。两种 ZnO 样品诱导了相似的毒性机制,但小颗粒的单位质量毒性效力有统计学意义的增加。

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