Plumbagin Attenuates Ovalbumin-induced Allergic Asthma in Mice through Inhibition of Inflammatory Response

IF 0.6 4区医学 Q4 CHEMISTRY, MEDICINAL

Pharmacognosy Magazine Pub Date : 2023-11-03 DOI:10.1177/09731296231184537

Dong Yiming, Abdullah R Alzahrani, Abubucker Peer Mohideen

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Abstract

Background Asthma is a prominent non-communicable inflammatory disease that affects both children and the elderly. Younger people are more prone to asthma, and most prescribed anti-asthmatic medicines relieve symptoms but do not cure the condition completely. We investigated the ability of a phytochemical plumbagin to alleviate ovalbumin (OVA)-induced asthma in BALB/c mice. Materials and Methods The allergic asthma-induced mice were treated with two different doses of 25 and 50 mg/kg bwt plumbagin, and to compare the efficacy of plumbagin, a standard drug dexamethasone treatment was given. OVA-specific IgE and eotaxin were quantified to determine the induction of asthma and the inhibitory role of plumbagin. Total leukocyte and differential count were done to assess the effect of plumbagin on inflammatory cells. Inflammatory cytokines inducing both atopic and non-atopic asthma were quantified to examine the efficacy of plumbagin against allergic and non-allergic-induced asthma. Nitric oxide (NO) and myeloperoxidase activity were measured to investigate the anti-asthmatic potential of plumbagin. The antioxidant potency of plumbagin was assessed by quantifying the levels of antioxidants and the oxidative stress marker malondialdehyde. Lung weight index and histopathological analysis of lung tissue were done to confirm the ameliorative potency of plumbagin against OVA allergen-induced asthma. Results Plumbagin treatment significantly decreased the status of OVA-specific IgE and eotaxin, thereby prevented the eosinophilic infiltration. It also inhibited the synthesis of both atopic and non-atopic inducing inflammatory cytokines. Plumbagin treatment also increased the levels of antioxidants and prevented the lung tissue damage, which was evidenced with our histopathology study of lung tissue. Conclusion Overall, our finding confirms that plumbagin is persuasively alleviated OVA allergen-induced asthma complications in mice model and may be an alternative for currently available anti-asthmatic drugs.

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白桦素通过抑制炎症反应减轻卵清蛋白诱导的小鼠过敏性哮喘

哮喘是一种影响儿童和老年人的非传染性炎症性疾病。年轻人更容易患哮喘，大多数处方的抗哮喘药物可以缓解症状，但不能完全治愈病情。我们研究了一种植物化学物质白桦素缓解BALB/c小鼠卵清蛋白(OVA)诱导的哮喘的能力。材料与方法分别给予25、50 mg/kg bwt不同剂量的白丹素治疗过敏性哮喘小鼠，并以标准药物地塞米松治疗白丹素，比较其疗效。测定ova特异性IgE和eotaxin对哮喘的诱导作用和白桦素的抑制作用。用白细胞总数和差异计数来评估白桦素对炎症细胞的影响。对诱导特应性和非特应性哮喘的炎症细胞因子进行量化，以检验白桦素对过敏性和非过敏性哮喘的疗效。通过测定一氧化氮(NO)和髓过氧化物酶活性来研究白桦素的抗哮喘作用。通过定量测定抗氧化剂和氧化应激标志物丙二醛的水平来评估白桦素的抗氧化能力。肺重指数和肺组织病理分析证实白桦素对OVA变应原诱导哮喘的改善作用。结果白桦素可显著降低ova特异性IgE和eotaxin水平，从而抑制嗜酸性粒细胞的浸润。它还抑制了特应性和非特应性诱导炎症细胞因子的合成。我们对肺组织的组织病理学研究证明，白桦苷处理还能提高抗氧化剂水平，防止肺组织损伤。综上所述，我们的研究结果证实了白桦白素有减轻OVA过敏原诱导的小鼠哮喘并发症的作用，可能是现有抗哮喘药物的替代方案。

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