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苯并[a]芘对F-344大鼠的急性和亚慢性经口毒性

Acute and subchronic oral toxicities of benzo[a]pyrene in F-344 rats.

作者信息

Knuckles M E, Inyang F, Ramesh A

机构信息

District of Columbia Department of Health, Public Health Laboratory, Washington, DC 0001, USA.

出版信息

Toxicol Sci. 2001 Jun;61(2):382-8. doi: 10.1093/toxsci/61.2.382.

Abstract

We have studied the acute and subchronic oral toxicities of benzo[a]pyrene (BaP) in male and female F-344 rats. Single acute BaP doses of 0, 100, 600, and 1000 mg /kg dissolved in peanut oil were administered by oral gavage. Subchronic doses of 0, 5, 50, and 100 mg/kg/day were administered for 90 days in the animal diet. The major toxicological endpoints examined included animal body weight, selected tissue weights, and histopathological examinations (liver, kidney, stomach, prostate, testes, and ovaries). In addition, we examined blood elements: red blood cells (RBC), white blood cells (WBC), hemoglobin (Hgb), hematocrit (Hct), mean cell volume (MCV), mean cell hematocrit (MCH), and mean cell hemoglobin concentration (MCHC), blood chemistry (ALT, AST, and BUN), and urine chemistry (glucose, bilirubin, specific gravity, pH, protein, urobilinogen, nitrite, occult blood, and leucocytes). In the acute study, WBC were significantly decreased and mean cell-hemoglobin concentration was significantly increased, both in males only. The liver:body weight ratio was significantly increased in males and females (up to 30%). None of the blood chemistry or urine parameters were significantly affected. In the subchronic study, mean body weight was significantly decreased in males only (13%), and the liver:body weight ratio in males was significantly increased. Several of the blood elements were significantly decreased in males and females after 90 days; RBCs (up to 10%), Hct (up to 12%), and Hgb (up to 12%). For blood chemistry parameters (AST, ALT, BUN), only BUN in males was significantly increased in the high dose group (100 mg/kg) at the 90 day time point. The histopathological examination of selected tissues showed significant abnormalities (tubular casts) only in the male kidney, at the 2 highest doses, after 90 days. These studies indicate that the acute and subchronic toxicities of BaP are relatively low, BaP affects specific blood elements and organs, and BaP has a greater effect on males than females. The induction of non-carcinogenic kidney abnormalities in males only may be indicative of renal dysfunction and further substantiates an apparent sex difference in tolerance to BAP:

摘要

我们研究了苯并[a]芘(BaP)对雄性和雌性F-344大鼠的急性和亚慢性经口毒性。将0、100、600和1000mg/kg的单次急性BaP剂量溶解于花生油中,通过灌胃给药。亚慢性剂量为0、5、50和100mg/kg/天,在动物饲料中给药90天。所检测的主要毒理学终点包括动物体重、选定组织重量以及组织病理学检查(肝脏、肾脏、胃、前列腺、睾丸和卵巢)。此外,我们还检测了血液成分:红细胞(RBC)、白细胞(WBC)、血红蛋白(Hgb)、血细胞比容(Hct)、平均红细胞体积(MCV)、平均红细胞血红蛋白含量(MCH)和平均红细胞血红蛋白浓度(MCHC),血液生化指标(谷丙转氨酶、谷草转氨酶和尿素氮)以及尿液生化指标(葡萄糖、胆红素、比重、pH值、蛋白质、尿胆原、亚硝酸盐、隐血和白细胞)。在急性研究中,仅雄性大鼠的白细胞显著减少,平均红细胞血红蛋白浓度显著升高。雄性和雌性大鼠的肝脏与体重之比均显著增加(高达30%)。血液生化指标或尿液参数均未受到显著影响。在亚慢性研究中,仅雄性大鼠的平均体重显著下降(13%),雄性大鼠的肝脏与体重之比显著增加。90天后,雄性和雌性大鼠的几种血液成分均显著减少;红细胞(高达10%)、血细胞比容(高达12%)和血红蛋白(高达12%)。对于血液生化参数(谷草转氨酶、谷丙转氨酶、尿素氮),在90天时间点,仅高剂量组(100mg/kg)雄性大鼠的尿素氮显著升高。选定组织的组织病理学检查显示,仅在90天后,最高的两个剂量组雄性大鼠的肾脏出现显著异常(肾小管管型)。这些研究表明,BaP的急性和亚慢性毒性相对较低,BaP影响特定的血液成分和器官,并且BaP对雄性的影响大于雌性。仅在雄性大鼠中诱导出非致癌性肾脏异常可能表明肾功能障碍,并进一步证实了对BaP耐受性存在明显的性别差异:

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