Coula edulis B.(橄榄科)茎皮乙醇提取物的急性和亚慢性毒性评估

Eric Beyegue, J. Youovop, G. R. Takuissu, Nadine Essola Ndoue, Florine Essouman Mbappe, Ferdinand Edou, B. Azantsa, J. Ngondi, J. Oben
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引用次数: 0

摘要

目的:库拉·埃利斯·贝尔。(Olacaceae)是一种非木质化的森林产品,在撒哈拉以南非洲不为人所知,但被广泛用作植物药或食品添加剂。然而,这种植物的毒性仍然未知。本研究旨在评价毛竹茎皮乙醇提取物(CEE)的安全性。研究设计:药理学研究。学习地点和时间:喀麦隆雅温得第一大学生物化学系营养与营养生物化学实验室,2018年6月至2022年7月。方法:关于急性和亚慢性毒性评估的研究是根据经济合作与发展组织(经合组织)准则423进行的。根据经合组织指南407,在28天内使用重复剂量评估了样品的亚急性毒性。结果:治疗大鼠未见死亡及临床毒性症状,提示毛竹醇提物LD50 > 2000 mg/kg bw。在亚急性毒性研究中,施用CEE也没有导致体重过程的任何变化。在最高剂量为600 mg/kg时,只观察到雌性卵巢的相对重量有显著下降。在男性和女性中,CEE不影响血脂标记物或转氨酶水平(AST, ALT)。此外,肌酸酐虽有小幅升高,但不显著(p> 0.05),未见肾功能不全。在雄性小鼠中,CEE在600 mg/kg剂量下引起平均红细胞体积数增加,同时在300 mg/kg剂量下引起平均红细胞血红蛋白浓度下降。在女性中,观察到单核细胞数量、红细胞数量和血红蛋白水平显著增加。尿素、葡萄糖和脂质标志物的水平没有差异,所研究的器官也没有组织学变化。结论:正如预期的那样,暴露于CEE并没有对治疗大鼠造成明显的毒性作用。因此,这种植物提取物可以安全地推荐用于治疗用途。
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Acute and Sub-chronic Toxicity Evaluation of the Ethanolic Extract of Coula edulis B., (Olacaceae) Stem Bark
Aims: Coula edulis Baill., (Olacaceae) is a non-lignified forest product not well known and widely used in sub-Saharan Africa as a phytomedicine or food additive. However, the toxicity of this plant remains unknown. This study aimed to assess the safety of the ethanolic extract of C. edulis stem bark (CEE). Study Design:  Pharmacological study. Place and Duration of Study: Laboratory of Nutrition and Nutritional Biochemistry, Department of Biochemistry, University of Yaounde 1 (Cameroon), between June 2018 and July 2022. Methodology: Studies on the assessment of acute and subchronic toxicity were carried out by guidelines 423 of the Organization for Economic Co-operation and Development (OECD). Subacute toxicity of the sample was assessed over 28 days using repeated doses by OECD Guideline 407. Results: No cases of death and clinical signs of toxicity were observed in the treated rats, suggesting that the LD50 of C. edulis ethanolic extract is greater than 2000 mg/kg bw. Regarding the subacute toxicity study, the administration of CEE also did not result in any changes in the course of body weight. Only a significant decrease in the relative weight of the ovaries in females at the highest dose of 600 mg/kg was observed. In males and females, CEE did not affect lipid profile markers or transaminase levels (AST, ALT). In addition, a small but non-significant (p> 0.05) increase in creatinine was observed without kidney dysfunction. In males, CEE induced an increase in mean corpuscular volume number at 600 mg/kg, while at the same time, mean corpuscular hemoglobin concentration decreased at the 300 mg/kg dose. In females, a significant increase in the number of monocytes, red blood cells, and hemoglobin level were observed. No difference in the levels of urea, glucose, and lipid markers was observed nor histological changes in the organs studied. Conclusion: As would be expected, exposure to CEE did not cause significant toxic effects in treated rats. Therefore, this plant extract can be safely recommended for therapeutic use.
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