Department of Biochemistry, Roberto Alcantara Gomes Institute of Biology, State University of Rio de Janeiro, Rio de Janeiro, Brazil.
Laboratory of Immunophysiology, Department of Biology, Center for Biological Sciences and Health, Federal University of Maranhão, São Luís, Maranhão, Brazil.
J Ethnopharmacol. 2024 Mar 1;321:117476. doi: 10.1016/j.jep.2023.117476. Epub 2023 Nov 25.
Echinodorus macrophyllus (Kunth.) Micheli (Alismataceae), known as chapéu-de-couro in Brazil, is popularly used to treat inflammatory diseases. We have previously demonstrated a significant reduction in the acute inflammation for the aqueous extract of E. macrophyllus (AEEm) and its ethanolic fraction (Fr20) and described that hydroxycinnamoyl derivatives present in SF1 (Fr20 subfraction) showed higher anti-inflammatory properties by mechanisms that include a reduction of TNF-α, IL-1β, CKCL1/KC, LTB4, and PGE2 levels in exudate.
This work describes the acute toxicological effect of SF1 subfraction on SW mice treated orally for five days in the air pouch model by evaluating the hematological and biochemical determinations on the blood samples; the relative organ weight and its histopathological analysis; the liver genotoxicity assessment and the activity of liver enzymes from xenobiotic metabolism.
Fr20 was earlier fractionated on the Sephadex LH-20 column, yielding mainly four subfractions, including SF1. The SF1 toxicity was evaluated in mice challenged with carrageenan on the air pouch inflammation model and orally treated for five days. The body weight was monitored daily, and the organs were weighed after the euthanasia. Hematological and biochemical determinations were carried out using specific commercial kits and following the protocols provided by the manufacturers. The organs were fixed, sectioned, processed for hematoxylin and eosin staining, and analyzed by light microscopy. Genotoxicity assessment was performed by the alkaline single-cell gel electrophoresis. Livers were processed for ethoxyresorufin-O-deethylase (EROD) and Glutathione S-transferase (GST) assays.
SF1 exhibited low toxicity, as no significant discrepancy was observed in the relative weight of the body organs of mice. Moreover, the daily treatment with SF1 did not alter the number and percentage of red blood cells or hemoglobin concentration in the blood. The treatment with SF1 did not affect the creatinine concentration, but the 25 mg/kg dose reduced the plasma urea level and uric acid, suggesting its use in treating acute renal failure. The parameters analyzed did not present biochemical alterations indicative of liver disease. Regarding serum triglyceride and cholesterol levels, a significant decrease was detected in both parameters in mice treated with SF1. In addition, the histopathological analysis showed that inflammatory focus in the livers seemed more relevant in the control groups than in those treated. There were no significant changes in the renal or splenic tissues of animals treated with SF1. Treatment with SF1 also does not have a genotoxic effect on liver cells.
Treatment with SF1 showed no toxicity in mice at doses equivalent to those recommended for humans, which provides evidence of the safety of the therapeutic use of this subfraction.
Echinodorus macrophyllus(Kunth.)Micheli(泽泻科),在巴西被称为 chapéu-de-couro,民间用于治疗炎症性疾病。我们之前已经证明,Echinodorus macrophyllus 的水提物(AEEm)及其乙醇级分(Fr20)显著减少了急性炎症,并且描述了 SF1(Fr20 亚级分)中存在的羟基肉桂酰衍生物通过包括降低 TNF-α、IL-1β、CKCL1/KC、LTB4 和 PGE2 水平在内的机制表现出更高的抗炎特性渗出液。
本工作描述了 SF1 亚级分在气囊炎模型中通过口服给予 SW 小鼠 5 天的急性毒理学效应,通过评估血液样本中的血液学和生化测定、相对器官重量及其组织病理学分析、肝遗传毒性评估和外源性代谢的肝酶活性来评价。
Fr20 先前在 Sephadex LH-20 柱上进行了分级,主要得到四个亚级分,包括 SF1。SF1 毒性在气囊炎炎症模型中用角叉菜胶挑战的小鼠中进行评估,并口服给予 5 天。每天监测体重,安乐死后称重器官。使用特定的商业试剂盒进行血液学和生化测定,并按照制造商提供的方案进行。将器官固定、切片、用苏木精和曙红染色、并通过光镜进行分析。遗传毒性评估通过碱性单细胞凝胶电泳进行。处理肝脏以进行乙氧基Resorufin-O-脱乙基酶(EROD)和谷胱甘肽 S-转移酶(GST)测定。
SF1 表现出低毒性,因为小鼠体器官的相对重量没有明显差异。此外,SF1 的每日治疗不会改变血液中红细胞的数量和百分比或血红蛋白浓度。SF1 治疗不会影响肌酐浓度,但 25mg/kg 剂量会降低血浆尿素水平和尿酸,提示其可用于治疗急性肾衰竭。分析的参数未显示出表明肝脏疾病的生化改变。关于血清甘油三酯和胆固醇水平,SF1 治疗的小鼠这两种参数均显著降低。此外,组织病理学分析表明,在对照组中,肝脏中的炎症焦点似乎比在治疗组中更为相关。SF1 处理的动物的肾脏或脾脏组织没有明显变化。SF1 对肝细胞也没有遗传毒性作用。
SF1 在相当于推荐用于人类的剂量下对小鼠没有毒性,这为该亚级分的治疗用途的安全性提供了证据。
