Toxicological evaluation of therapeutically active zinc oxide nanoflowers in pre-clinical mouse model

IF 4.7 3区 环境科学与生态学 Q2 ENVIRONMENTAL SCIENCES NanoImpact Pub Date : 2023-07-01 DOI:10.1016/j.impact.2023.100479
Ayan Kumar Barui , Vishnu Sravan Bollu , Swapnali Londhe , Shruti S. Deshpande , Sourav Das , Susheel Kumar Nethi , Muntadher Mazin Abdulkareem Alabbasi , Madhusudana Kuncha , Jerald Mahesh Kumar , Ramakrishna Sistla , Sunil Misra , Chitta Ranjan Patra
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Abstract

Our earlier reports established that zinc oxide nanoflowers (ZONF) show significant pro-angiogenic properties, where reactive oxygen species, nitric oxide and MAPK-AKT-eNOS cell signaling axis play an essential task. Considering the significance of angiogenesis in healthcare, our research group has recently demonstrated the in vivo therapeutic application of ZONF (10 mg/kg b.w.) for treating peripheral artery disease. Moreover, based on the angio-neural crosstalk between vascular and neuronal systems, we have further demonstrated the neuritogenic and neuroprotective characteristics of pro-angiogenic nanoflowers (10 mg/kg b.w.) for the treatment of cerebral ischemia. However, it is crucial for a therapeutic material to be non-toxic for its practical clinical applications and therefore assessment of its in vivo toxicity and adverse effect is highly important. Herein, for the first time, we investigate a detailed nanotoxicology of therapeutically active ZONF in Swiss albino mice to evaluate their safety profile and comprehend their aspects for future clinical applications. The maximum tolerated dose (MTD) of ZONF was found to be 512.5 mg/kg b.w. which was employed for acute exposure (2 weeks), showing slight toxicity. However, sub-chronic (4 weeks) and long term chronic (8–12 weeks) studies of nanoflowers exhibited their non-toxic nature particularly at lower therapeutic doses (1–10 mg/kg b.w.). Additionally, in depth genotoxicity study revealed that lower therapeutic dose of ZONF (10 mg/kg b.w.) did not exhibit significant toxicity even in genetic level. Overall, the present nanotoxicology of ZONF suggests their high biocompatible nature at therapeutic dose, offering the basis of their future clinical applications in ischemic and other vascular diseases.

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临床前小鼠模型中治疗活性氧化锌纳米花的毒理学评价。
我们早期的报告证实,氧化锌纳米花(ZONF)显示出显著的促血管生成特性,其中活性氧、一氧化氮和MAPK-AKT-eNOS细胞信号轴发挥着重要作用。考虑到血管生成在医疗保健中的重要性,我们的研究小组最近证明了ZONF(10 mg/kg b.w.)在体内治疗外周动脉疾病的应用。此外,基于血管和神经元系统之间的血管-神经串扰,我们进一步证明了促血管生成纳米花(10mg/kg b.w.)治疗脑缺血的神经炎和神经保护特性。然而,治疗材料的无毒性对其实际临床应用至关重要,因此评估其体内毒性和不良反应非常重要。在此,我们首次在瑞士白化病小鼠中研究了治疗活性ZONF的详细纳米毒理学,以评估其安全性,并了解其在未来临床应用中的作用。ZONF的最大耐受剂量(MTD)为512.5 mg/kg体重,用于急性暴露(2周),显示轻微毒性。然而,纳米花的亚慢性(4周)和长期慢性(8-12周)研究显示出其无毒性,特别是在较低的治疗剂量(1-10 mg/kg b.w.)下。此外,深入的遗传毒性研究表明,较低的ZONF治疗剂量(10 mg/kg b.w..)即使在遗传水平上也没有表现出显著的毒性。总的来说,目前ZONF的纳米毒理学表明,在治疗剂量下,ZONF具有高度的生物相容性,为其未来在缺血性和其他血管疾病中的临床应用奠定了基础。
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来源期刊
NanoImpact
NanoImpact Social Sciences-Safety Research
CiteScore
11.00
自引率
6.10%
发文量
69
审稿时长
23 days
期刊介绍: NanoImpact is a multidisciplinary journal that focuses on nanosafety research and areas related to the impacts of manufactured nanomaterials on human and environmental systems and the behavior of nanomaterials in these systems.
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