Natural Remedies Research Center, Bangalore, India.
Toxicol Mech Methods. 2003;13(4):253-61. doi: 10.1080/713857188.
Allergic rhinitis (also known as hay fever) is the most commonly occurring immunological disorder, and it affects 40 million men, women, and children in the United States. Symptomatically, it is an inflammation and irritation of the mucous membranes that line the nose. Allergy is defined as a state of hypersensitivity or hyperimmunity caused by exposure to a particular antigen (allergen) that results in increased reactivity upon subsequent exposure. A novel botanical formulation, Aller-7/NR-A2, was developed for the treatment of allergic rhinitis; it is a combination of medicinal plant extracts from Phyllanthus emblica, Terminalia chebula, Terminalia bellerica, Albizia lebbeck, Piper nigrum, Zingiber officinale, and Piper longum. This novel formulation has demonstrated potent antihistaminic, anti-inflammatory, antispasmodic, antioxidant, and mast-cell-stabilization activities. All of the doses for these toxicity studies were selected according to the guidelines of the Organization for Economic Cooperation and Development, the World Health Organization, and the Environmental Protection Agency. Acute toxicity of Aller-7 was evaluated in Swiss Albino mice at doses of 125, 250, 500, 1000, and 1500 mg/kg. After 15 days of treatment, the animals were sacrificed. No histopathological changes were observed in major vital organs. A similar study was conducted in Albino Wistar rats, which were sacrificed at the end of 15 days. No histopathological changes or toxicity was observed at up to 2 g/kg body weight. Subacute toxicity was conducted in Albino Wistar rats at a dose of 90 mg/kg body weight for 3 days, then at 180 mg/kg for the next 3 days, and then at 270 mg/kg for 3 weeks. After 28 days, the animals were sacrificed and tested; no toxicity was observed. In a subchronic toxicity study, there was no observed adverse effect level at 1 g/kg body weight in rats. In a teratological assay, at doses of 3.0 g/kg (20 times the recommended dose) and 1.8 g/kg, respectively, no visceral or skeletal anomalies were observed in the fetuses. No maternal changes were observed when Aller-7 was administered during gestation and lactation. No evidence of mutagenicity was observed at doses up to 5000 mug per plate of Aller-7 in Salmonella typhimurium cells. The present study evaluated the safety of Aller-7 by conducting several in vitro and in vivo studies. Further studies of the 90-day chronic toxicity of Aller-7 are currently in progress.
变应性鼻炎(也称为花粉症)是最常见的免疫性疾病,影响美国 4000 万男性、女性和儿童。其症状为鼻腔黏膜的炎症和刺激。过敏被定义为暴露于特定抗原(过敏原)引起的超敏或过度免疫状态,导致随后暴露时反应性增加。一种新型植物制剂 Aller-7/NR-A2 被开发用于治疗变应性鼻炎;它是 Phyllanthus emblica、Terminalia chebula、Terminalia bellerica、Albizia lebbeck、Piper nigrum、Zingiber officinale 和 Piper longum 药用植物提取物的组合。这种新型配方具有强大的抗组胺、抗炎、抗痉挛、抗氧化和肥大细胞稳定作用。这些毒性研究的所有剂量均根据经济合作与发展组织、世界卫生组织和美国环境保护署的指南选择。在 125、250、500、1000 和 1500mg/kg 剂量的瑞士白化小鼠中评估了 Aller-7 的急性毒性。治疗 15 天后,处死动物。在主要生命器官中未观察到组织病理学变化。在 Albino Wistar 大鼠中进行了类似的研究,在第 15 天处死。在高达 2g/kg 体重时,未观察到组织病理学变化或毒性。在 90mg/kg 体重的 Albino Wistar 大鼠中进行了亚急性毒性试验,连续 3 天,然后连续 3 天 180mg/kg,然后连续 3 周 270mg/kg。28 天后处死并检测,未观察到毒性。在亚慢性毒性研究中,在 1g/kg 体重的大鼠中未观察到不良作用水平。在致畸试验中,在 3.0g/kg(推荐剂量的 20 倍)和 1.8g/kg 剂量下,胎儿未观察到内脏或骨骼异常。在妊娠和哺乳期给予 Aller-7 时,未观察到母体变化。在 Salmonella typhimurium 细胞中,高达 5000μg/盘的 Aller-7 剂量下未观察到致突变性。本研究通过进行几项体外和体内研究评估了 Aller-7 的安全性。目前正在进行 Aller-7 的 90 天慢性毒性的进一步研究。
