Toxicological analysis of chronic exposure to polymeric nanocapsules with different coatings in Drosophila melanogaster

IF 3.9 3区 环境科学与生态学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY Comparative Biochemistry and Physiology C-toxicology & Pharmacology Pub Date : 2024-05-07 DOI:10.1016/j.cbpc.2024.109939
Franciéle Romero Machado , Vandreza Cardoso Bortolotto , Stífani Machado Araujo , Mustafa Munir Mustafa Dahleh , Eliana Jardim Fernandes , Elize Aparecida Santos Musachio , Ana Cláudia Funguetto-Ribeiro , Sandra Elisa Haas , Gustavo Petri Guerra , Marina Prigol , Silvana Peterini Boeira
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Abstract

Nanotechnology involves the utilization of nanomaterials, including polymeric nanocapsules (NCs) that are drug carriers. For modify drug release and stability, nanoformulations can feature different types of polymers as surface coatings: Polysorbate 80 (P80), Polyethylene glycol (PEG), Chitosan (CS) and Eudragit (EUD). Although nanoencapsulation aims to reduce side effects, these polymers can interact with living organisms, inducing events in the antioxidant system. Thus far, little has been described about the impacts of chronic exposure, with Drosophila melanogaster being an in vivo model for characterizing the toxicology of these polymers. This study analyzes the effects of chronic exposure to polymeric NCs with different coatings. Flies were exposed to 10, 50, 100, and 500 μL of NCP80, NCPEG, NCCS, or EUD. The survival rate, locomotor changes, oxidative stress markers, cell viability, and Nrf2 expression were evaluated. Between the coatings, NCPEG had minimal effects, as only 500 μL affected the levels of reactive species (RS) and the enzymatic activities of catalase (CAT) and glutathione S-transferase (GST) without reducing Nrf2 expression. However, NCEUD significantly impacted the total flies killed, RS, CAT, and Superoxide dismutase from 100 μL. In part, the toxicity mechanisms of these coatings can be explained by the imbalance of the antioxidant system. This research provided initial evidence on the chronic toxicology of these nanomaterials in D. melanogaster to clarify the nanosafety profile of these polymers in future nanoformulations. Further investigations are essential to characterize possible biochemical pathways involved in the toxicity of these polymeric coatings.

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黑腹果蝇长期接触不同涂层的聚合物纳米胶囊的毒理学分析。
纳米技术涉及纳米材料的利用,包括作为药物载体的聚合物纳米胶囊(NC)。为了改变药物的释放和稳定性,纳米制剂可以采用不同类型的聚合物作为表面涂层:聚山梨醇酯 80 (P80)、聚乙二醇 (PEG)、壳聚糖 (CS) 和 Eudragit (EUD)。虽然纳米封装的目的是减少副作用,但这些聚合物会与生物体相互作用,诱导抗氧化系统发生变化。黑腹果蝇是表征这些聚合物毒理学的活体模型,但迄今为止,有关长期接触这些聚合物的影响的描述很少。本研究分析了长期接触具有不同涂层的聚合物 NC 的影响。蝇类分别暴露于 10、50、100 和 500 μL 的 NCP80、NCPEG、NCCS 或 EUD。对苍蝇的存活率、运动变化、氧化应激标记、细胞活力和 Nrf2 表达进行了评估。在不同的涂层中,NCPEG 的影响最小,因为只有 500 μL 会影响活性物质(RS)的水平以及过氧化氢酶(CAT)和谷胱甘肽 S 转移酶(GST)的酶活性,而不会降低 Nrf2 的表达。然而,NCEUD 会明显影响 100 μL 中被杀死的苍蝇总数、RS、CAT 和超氧化物歧化酶。在一定程度上,这些涂层的毒性机制可以用抗氧化系统失衡来解释。这项研究为这些纳米材料在黑腹蝇蛆体内的慢性毒理学提供了初步证据,从而明确了这些聚合物在未来纳米制剂中的纳米安全性。进一步的研究对于确定这些聚合物涂层毒性可能涉及的生化途径至关重要。
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来源期刊
CiteScore
7.50
自引率
5.10%
发文量
206
审稿时长
30 days
期刊介绍: Part C: Toxicology and Pharmacology. This journal is concerned with chemical and drug action at different levels of organization, biotransformation of xenobiotics, mechanisms of toxicity, including reactive oxygen species and carcinogenesis, endocrine disruptors, natural products chemistry, and signal transduction with a molecular approach to these fields.
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