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Multi-walled carbon nanotube physicochemical properties predict pulmonary inflammation and genotoxicity

机译:多壁碳纳米管的理化性质预测肺部炎症和遗传毒性

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摘要

Lung deposition of multi-walled carbon nanotubes (MWCNT) induces pulmonary toxicity. Commercial MWCNT vary greatly in physicochemical properties and consequently in biological effects. To identify determinants of MWCNT-induced toxicity, we analyzed the effects of pulmonary exposure to 10 commercial MWCNT (supplied in three groups of different dimensions, with one pristine and two/three surface modified in each group). We characterized morphology, chemical composition, surface area and functionalization levels. MWCNT were deposited in lungs of female C57BL/6J mice by intratracheal instillation of 0, 6, 18 or 54 μg/mouse. Pulmonary inflammation (neutrophil influx in bronchoalveolar lavage (BAL)) and genotoxicity were determined on day 1, 28 or 92. Histopathology of the lungs was performed on day 28 and 92. All MWCNT induced similar histological changes. Lymphocytic aggregates were detected for all MWCNT on day 28 and 92. Using adjusted, multiple regression analyses, inflammation and genotoxicity were related to dose, time and physicochemical properties. The specific surface area (BET) was identified as a positive predictor of pulmonary inflammation on all post-exposure days. In addition, length significantly predicted pulmonary inflammation, whereas surface oxidation (–OH and –COOH) was predictor of lowered inflammation on day 28. BET surface area, and therefore diameter, significantly predicted genotoxicity in BAL fluid cells and lung tissue such that lower BET surface area or correspondingly larger diameter was associated with increased genotoxicity. This study provides information on possible toxicity-driving physicochemical properties of MWCNT. The results may contribute to safe-by-design manufacturing of MWCNT, thereby minimizing adverse effects.
机译:多壁碳纳米管(MWCNT)的肺部沉积会引起肺毒性。商业MWCNT的理化性质和生物学效应差异很大。为了确定决定因素的多壁碳纳米管诱导的毒性,我们分析了肺部暴露于10种商业多壁碳纳米管的影响(分为三组,每组不同尺寸,每组分别有一个原始表面和两个/三个表面修饰)。我们表征了形态,化学组成,表面积和功能化水平。通过气管内滴入0、6、18或54μg/小鼠,将MWCNT沉积在雌性C57BL / 6J小鼠的肺中。在第1、28或92天测定肺部炎症(中性粒细胞流入支气管肺泡灌洗液(BAL))和遗传毒性。在第28和92天进行肺的组织病理学检查。所有MWCNT诱导的组织学变化均相似。在第28天和第92天检测到所有MWCNT的淋巴细胞聚集体。使用调整后的多元回归分析,炎症和基因毒性与剂量,时间和理化特性有关。比表面积(BET)被确定为所有暴露后天肺炎症的阳性预测指标。此外,长度显着预测了肺部炎症,而表面氧化(-OH和-COOH)则是炎症在28天降低的预测因子。BET表面积和直径显着预测了BAL液细胞和肺组织的遗传毒性,因此BET降低表面积或相应更大的直径与遗传毒性增加有关。这项研究提供了有关MWCNT可能的毒性驱动理化特性的信息。结果可能有助于设计安全地制造MWCNT,从而最大程度地减少不利影响。

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