M/P Biomedical Consultants LLC, 402 Live Oak Drive, Mill Valley, CA 94941, USA.
Inflammopharmacology. 2011 Aug;19(4):227-33. doi: 10.1007/s10787-010-0049-1. Epub 2010 Jun 22.
An extract of the seed from celery (Apium graviolens) (CSE), and fractions thereof, have been found to possess anti-inflammatory activity, gastro-protective activity, and anti-Helicobacter pylori activity. In view of the potential for employing these extracts for therapeutic use, toxicological investigations were undertaken with an alcoholic extract (A-CSE) which has previously been shown to have the above pharmacological activities.
A 28-day toxicity study was performed in rats according to Good Laboratory Practice (GLP) conditions. Eighteen adult male and 18 adult female rats were randomly assigned to 3 treatment groups of 6 rats/sex/group and were dosed orally with A-CSE of 0, 150 or 5,000 mg/kg per day. Daily observations of vital signs and body weights were recorded and ophthalmological investigations were performed. At autopsy, the principal organs were weighed and sections collected for histological analysis. Serum and urine samples were collected at termination for routine clinical chemistry. Under non-GLP conditions alpha-2-μ-globulin immunohistochemistry was performed on kidney tissues and hepatic cytochrome P450 protein was determined, as well as, the enzymatic activities of the principal isoforms.
All animals survived treatments with no visible or behavioral signs of toxicity being observed during the study. There were no statistically significant differences in body weight gains, body weight gains per day or cumulative absolute body weight gains, for either sex, in any treatment groups when compared with controls. Slightly increased liver weight and liver to body and brain weight ratios were observed in female rats and in liver to body weight ratios in male rats given high dose A-CSE which was a test article effect, but the absence of any microscopic correlates for the liver weight increases suggests that these were not toxicologically significant. Treatment related macroscopic changes were not observed at necropsy and microscopic findings were limited to minimal increases in gastric eosinophils in several male and female rats in the 5,000 mg/kg per day treatment groups. Minimal focal degeneration of renal tubules was observed sporadically in both sexes assigned to all treatment groups including control and was consistent with early spontaneous nephropathy of laboratory rats and thus was not considered to represent a pathologic change associated with the test article. Increased serum globulin and phosphorus levels were observed in male rats given 5,000 mg/kg per day A-CSE and decreased serum triglycerides levels in female animals given 150 or 5,000 mg/kg per day A-CSE. The increase in serum globulin and phosphorus in male animals was small in magnitude and not considered toxicologically significant. The mechanism for the decrease in serum triglycerides in female rats was not apparent. Changes in urinalysis parameters were limited to small decreases in urine pH in female animals in the 150 and 5,000 mg/kg per day groups and were not deemed toxicologically significant. Alpha-2-μ-globulin immunohistochemistry was performed on kidney tissues from all animals and found to be within normal physiologic limits. Minor corneal mineralization occurred in some animals from all treatment groups. Cataracts were observed in one in the control and one in an animal that had 5,000 mg/kg per day but since the cataracts occurred in the metabolically inactive region of the lens, these were not considered indicative of test article related lesions. There were no changes in total hepatic microsomal protein or in total cytochrome P450 protein. Although male rats appeared to have to higher levels of total microsomal protein than female rats, there appeared to be no treatment effect in either male or female animals. As regards the activity of the various isoforms tested (CYP2B1/2, CYP1A1/2, CYP3A1/2), with the large range of activities detected for each P450 isoform, no clear change in activity or protein were observed, however, these data were not statistically analyzed.
These results suggest that there are no toxicologically significant sub-chronic effects of oral A-CSE in rats. The no adverse effect level for systemic toxicity would appear to be 5,000 mg/kg per day.
芹菜(Apium graveolens)种子提取物(CSE)及其部分成分已被发现具有抗炎、胃保护和抗幽门螺杆菌活性。鉴于这些提取物有用于治疗的潜力,因此对先前显示出上述药理学活性的酒精提取物(A-CSE)进行了毒理学研究。
根据良好实验室规范(GLP)条件进行了为期 28 天的毒性研究。18 只成年雄性和 18 只成年雌性大鼠随机分为 3 个治疗组,每组 6 只大鼠/性别/组,经口给予 A-CSE 剂量为 0、150 或 5,000mg/kg/天。记录每日生命体征和体重变化,并进行眼科检查。解剖时称重主要器官,并采集组织学分析的切片。在试验结束时收集血清和尿液样本,用于常规临床化学检测。在非 GLP 条件下,对肾脏组织进行α-2-μ-球蛋白免疫组织化学检测,并测定肝细胞色素 P450 蛋白以及主要同工酶的酶活性。
所有动物均耐受治疗,在研究过程中未观察到任何可见或行为毒性迹象。与对照组相比,任何治疗组的雄性或雌性动物的体重增加、体重增加率或累积绝对体重增加均无统计学差异。在接受高剂量 A-CSE 的雌性大鼠中,肝脏重量略有增加,以及雄性大鼠的肝体比和脑体比增加,这是一种受试物效应,但肝脏重量增加没有任何微观相关性,表明这不是毒理学上的显著变化。在尸检时未观察到与治疗相关的大体变化,显微镜下发现仅在一些接受 5,000mg/kg/天 A-CSE 治疗的雄性和雌性大鼠中胃嗜酸性粒细胞有轻微增加。所有治疗组(包括对照组)的雄性和雌性大鼠均可见散在的肾脏小管局灶性变性,这与实验室大鼠的早期自发性肾病一致,因此不认为这与受试物有关。接受 5,000mg/kg/天 A-CSE 的雄性大鼠血清球蛋白和磷水平升高,接受 150 或 5,000mg/kg/天 A-CSE 的雌性动物血清甘油三酯水平降低。雄性动物血清球蛋白和磷水平的升高幅度较小,不认为具有毒理学意义。雌性大鼠血清甘油三酯水平降低的机制尚不清楚。尿液分析参数的变化仅限于雌性动物尿液 pH 值略有降低,在 150 和 5,000mg/kg/天组中,不认为具有毒理学意义。对所有动物的肾脏组织进行了α-2-μ-球蛋白免疫组织化学检测,结果均在正常生理范围内。一些动物的角膜有轻微的矿化。在一只对照动物和一只接受 5,000mg/kg/天 A-CSE 的动物中观察到白内障,但由于白内障发生在晶状体的代谢不活跃区域,因此不认为这与受试物有关的病变。总肝微粒体蛋白或总细胞色素 P450 蛋白没有变化。虽然雄性大鼠的总肝微粒体蛋白似乎比雌性大鼠高,但在雄性或雌性动物中均未观察到治疗作用。关于测试的各种同工酶的活性(CYP2B1/2、CYP1A1/2、CYP3A1/2),由于每个 P450 同工酶的活性范围很大,因此未观察到活性或蛋白的明显变化,但这些数据未进行统计学分析。
这些结果表明,A-CSE 口服给药在大鼠中没有毒理学上显著的亚慢性作用。全身毒性的无不良影响水平似乎为 5,000mg/kg/天。
