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单壁碳纳米管皮肤毒性中的氧化应激与炎症反应

Oxidative stress and inflammatory response in dermal toxicity of single-walled carbon nanotubes.

作者信息

Murray A R, Kisin E, Leonard S S, Young S H, Kommineni C, Kagan V E, Castranova V, Shvedova A A

机构信息

Health Effects Laboratory Division, Pathology and Physiology Research Branch, NIOSH, M/L 2015, 1095 Willowdale Road, Morgantown, WV 26505, United States.

出版信息

Toxicology. 2009 Mar 29;257(3):161-71. doi: 10.1016/j.tox.2008.12.023. Epub 2008 Dec 30.

Abstract

Single-walled carbon nanotubes (SWCNT) represent a novel material with unique electronic and mechanical properties. The extremely small size ( approximately 1 nm diameter) renders their chemical and physical properties unique. A variety of different techniques are available for the production of SWCNT; however, the most common is via the disproportionation of gaseous carbon molecules supported on catalytic iron particles (high-pressure CO conversion, HiPCO). The physical nature of SWCNT may lead to dermal penetration following deposition on exposed skin. This dermal deposition provides a route of exposure which is important to consider when evaluating SWCNT toxicity. The dermal effects of SWCNT are largely unknown. We hypothesize that SWCNT may be toxic to the skin. We further hypothesize that SWCNT toxicity may be dependent upon the metal (particularly iron) content of SWCNT via the metal's ability to interact with the skin, initiate oxidative stress, and induce redox-sensitive transcription factors thereby affecting/leading to inflammation. To test this hypothesis, the effects of SWCNT were assessed both in vitro and in vivo using EpiDerm FT engineered skin, murine epidermal cells (JB6 P+), and immune-competent hairless SKH-1 mice. Engineered skin exposed to SWCNT showed increased epidermal thickness and accumulation and activation of dermal fibroblasts which resulted in increased collagen as well as release of pro-inflammatory cytokines. Exposure of JB6 P+ cells to unpurified SWCNT (30% iron) resulted in the production of ESR detectable hydroxyl radicals and caused a significant dose-dependent activation of AP-1. No significant changes in AP-1 activation were detected when partially purified SWCNT (0.23% iron) were introduced to the cells. However, NFkappaB was activated in a dose-dependent fashion by exposure to both unpurified and partially purified SWCNT. Topical exposure of SKH-1 mice (5 days, with daily doses of 40 microg/mouse, 80 microg/mouse, or 160 microug/mouse) to unpurified SWCNT caused oxidative stress, depletion of glutathione, oxidation of protein thiols and carbonyls, elevated myeloperoxidase activity, an increase of dermal cell numbers, and skin thickening resulting from the accumulation of polymorphonuclear leukocytes (PMNs) and mast cells. Altogether, these data indicated that topical exposure to unpurified SWCNT, induced free radical generation, oxidative stress, and inflammation, thus causing dermal toxicity.

摘要

单壁碳纳米管(SWCNT)是一种具有独特电子和机械性能的新型材料。其极小的尺寸(直径约1纳米)使其化学和物理性质独特。有多种不同技术可用于生产单壁碳纳米管;然而,最常见的是通过负载在催化铁颗粒上的气态碳分子的歧化反应(高压一氧化碳转化法,HiPCO)。单壁碳纳米管的物理性质可能导致其沉积在暴露皮肤后穿透皮肤。这种皮肤沉积提供了一种暴露途径,在评估单壁碳纳米管毒性时是一个需要考虑的重要因素。单壁碳纳米管对皮肤的影响在很大程度上尚不清楚。我们假设单壁碳纳米管可能对皮肤有毒性。我们进一步假设,单壁碳纳米管的毒性可能取决于其金属(特别是铁)含量,这是因为金属有能力与皮肤相互作用、引发氧化应激并诱导对氧化还原敏感的转录因子,从而影响/导致炎症。为了验证这一假设,使用EpiDerm FT工程皮肤、小鼠表皮细胞(JB6 P+)和具有免疫能力的无毛SKH-1小鼠,在体外和体内评估了单壁碳纳米管的影响。暴露于单壁碳纳米管的工程皮肤显示表皮厚度增加,真皮成纤维细胞积累并活化,导致胶原蛋白增加以及促炎细胞因子释放。将JB6 P+细胞暴露于未纯化的单壁碳纳米管(含铁30%)会产生可检测到的电子自旋共振(ESR)羟基自由基,并导致AP-1显著的剂量依赖性活化。当将部分纯化的单壁碳纳米管(含铁0.23%)引入细胞时,未检测到AP-1活化有显著变化。然而,通过暴露于未纯化和部分纯化的单壁碳纳米管,核因子κB(NFkappaB)均以剂量依赖性方式被激活。对SKH-1小鼠进行局部暴露(5天,每日剂量为40微克/小鼠、80微克/小鼠或160微克/小鼠)于未纯化的单壁碳纳米管,会引起氧化应激、谷胱甘肽消耗、蛋白质硫醇和羰基氧化、髓过氧化物酶活性升高、真皮细胞数量增加以及由于多形核白细胞(PMN)和肥大细胞积累导致的皮肤增厚。总之,这些数据表明,局部暴露于未纯化的单壁碳纳米管会诱导自由基生成、氧化应激和炎症,从而导致皮肤毒性。

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