Correlation of systemic and biochemical effects of PBB with behavioral effects.

Neurobehavioral toxicology Pub Date : 1979-01-01

E M Gause, D H Ross, M G Hamilton, B Z Leal, J Seifter, I Geller

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Abstract

Rats were given PBB orally at 1, 3, and 6 mg/kg (or vehicle as control) daily for 20 days. Some animals were sacrificed immediately while the food intake of remaining animals was limited to attain and maintain 80% of normal body weight. No effect of PBB upon body weight was observed for any of the dose levels employed. Immediately after dosing, liver/body weight ratios were 110% of controls for the 1 mg/kg group and 152% for the 3 and 6 mg/kg groups; after weight reduction for 2-6 months liver/body weight ratios for all 3 dose groups were 160-170% of controls. In the absence of body fat, most tissues exhibited dose-dependent retention of PBB 2-6 months after dosing with highest levels in liver followed by kidney. In 6 mg/kg rats weight-reduced for 6 months, liver AHH activity was 613% of controls; in rats sacrificed immediately after dosing, liver AHH activity was dose-related but appeared to reach maximal value at the 3 mg/kg dose. Both calcium binding to synaptic plasma membranes and calcium uptake by intact synaptosomes was significantly reduced in the brains of 1 mg/kg PBB rats, but not affected in preparations from 3 and 6 mg/kg animals.

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PBB的全身生化效应与行为效应的相关性。

大鼠每天口服1、3、6 mg/kg(或对照)PBB，连续20天。部分动物立即处死，其余动物限制摄取量，以达到并维持正常体重的80%。在任何剂量水平下，均未观察到多溴联苯对体重的影响。给药后，1 mg/kg组的肝脏/体重比为对照组的110%，3和6 mg/kg组为对照组的152%;体重减轻2-6个月后，所有3个剂量组的肝脏/体重比均为对照组的160-170%。在没有体脂的情况下，大多数组织在给药后2-6个月表现出剂量依赖性的PBB滞留，肝脏最高，其次是肾脏。6 mg/kg大鼠减重6个月后，肝脏AHH活性为对照组的613%;在给药后立即处死的大鼠中，肝脏AHH活性与剂量相关，但似乎在3 mg/kg剂量时达到最大值。1 mg/kg PBB大鼠脑内突触质膜钙结合和完整突触体钙摄取均显著降低，3和6 mg/kg PBB大鼠脑内钙结合和完整突触体钙摄取均不受影响。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Neurobehavioral toxicology

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