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Changes in biochemical and physiological indices in animals produced by the combined effect of benz a pyrene and phenol.

机译：苯并a and和苯酚的共同作用产生的动物生化和生理指标变化。

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摘要

Early energy changes in lungs, liver, and kidneys during the introduction of a benz a pyrene and phenol (as the possible carcinogen activator) were studied. It was observed that 10 days after a single instance introduction of 5 mg benz a pyrene per 0.9% NaCl (60 rats), oxidative phosphorylation in the lungs and livers is disturbed in the test rats, accompanied by a reduction of adenine nucleotides in these tissues. It is assumed that at this stage, the detoxication of benz a pyrene is intensified by free oxidation systems and by the respiratory chain of mitochondria. A chronic 3-month exposure to benz a pyrene and phenol (150 rats, each 5 mg of benz a pyrene per month intratracheally and 0.4 mg/m3 of phenol round-the-clock) results in greater disturbances of the energy exchange in the lungs, liver and kidneys. Benz a pyrene and phenol, individually and in combination, inhibit oxidative phosphorylation in the lungs. This significantly decreases the content of adenine nucleotides in this tissue. Activation of anaerobic glycolysis (twofold) and of aerobic glycolysis (eightfold) does not make up for the energy insufficiency in the tissue. The effect of benz a pyrene and phenol in the liver also results in suppressing oxidative phosphorylation and in the activation of glycolysis (anaerobic 2.5 times, the aerobic 3.7 times). Changes in the bioenergy of the kidneys are not as great. Phenol in its combined effect with benz[a]pyrene intensifies the effect of the latter, as shown primarily to the greater activation of anaerobic and aerobic glycolysis in the lungs and livers of test rats. The observed disturbances as concern the weight dynamics of the animals (weight loss in test rats), vitamin metabolism (their decrease in the organs in in urine) and hemopoiesis of red blood cells (erythropenia) attest to the toxic effect of benz a pyrene phenol on the organism, which is greater in the case of the combined action of the studied agents. No changes were discerned in the morphology of white blood cells.

机译：研究了在引入苯，pyr和苯酚（可能的致癌物质活化剂）期间，肺，肝和肾的早期能量变化。观察到，在每例中每0.9％NaCl引入5 mg苯a后60天（60只大鼠），受试大鼠的肺和肝中的氧化磷酸化受到干扰，同时这些组织中的腺嘌呤核苷酸减少。假定在此阶段，苯氧化a的脱毒作用通过自由氧化系统和线粒体的呼吸链而加剧。长期暴露于苯a和苯酚的3个月中（150只大鼠，气管内每月每只苯并a 5毫克，且全天候苯酚0.4 mg / m3每天暴露）会严重影响肺部能量交换，肝脏和肾脏。苯a和苯酚分别或联合抑制肺中的氧化磷酸化。这显着降低了该组织中腺嘌呤核苷酸的含量。厌氧糖酵解（两倍）和有氧糖酵解（八倍）的激活不能弥补组织中的能量不足。苯，a和苯酚在肝脏中的作用还导致抑制氧化磷酸化并激活糖酵解（无氧2.5倍，有氧3.7倍）。肾脏生物能的变化并不那么大。苯酚与苯并[a] combined的联合作用增强了苯并[a] re的作用，主要表现为试验大鼠的肺和肝中厌氧和有氧糖酵解的活化更大。观察到的紊乱涉及动物的体重动态（测试大鼠体重减轻），维生素代谢（尿中器官的减少）和红细胞的造血作用（红血球减少），证明苯并a具有毒性。在生物体上的作用更大，在被研究药物的联合作用下更大。白细胞的形态没有变化。

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期刊名称 Environmental Health Perspectives
作者
N N Skvortsova; I V Vysochina;
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年(卷),期 1976(13),-1
年度 1976
页码 101–106
总页数 6
原文格式 PDF
正文语种
中图分类公共卫生工程 ;
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1. Mutagenic activation and detoxification of benzo(a)pyrene in vitro by hepatic cytochrome P450 1A1 and phase II enzymes in three meat-producing animals [J] . W. Darwish, Y. Ikenaka, E. Eldaly, Food and Chemical Toxicology: An International Journal Published for the British Industrial Biological Research . 2010 ,第8a9期

机译：肝细胞色素P450 1A1和II期酶在三只肉类动物体内体外诱变激活苯并（a）re
2. Combined effects of seawater acidification and benzo(a)pyrene on the physiological performance of the marine bloom-forming diatom Skeletonema costatum [J] . Li Futian, Jiang Lele, Zhang Tianzhi, Marine Environmental Research . 2021 ,第Jula期

机译：海水酸化和苯并（A）芘对海洋绽放成型硅藻骨架骨架的生理性能的综合影响
3. Understanding the linked kinetics of benzo(a)pyrene and 3-hydroxybenzo(a)pyrene biomarker of exposure using physiologically-based pharmacokinetic modelling in rats [J] . Heredia-OrtizR., BouchardM. Journal of pharmacokinetics and pharmacodynamics . 2013 ,第6期

机译：使用基于生理的药代动力学模型在大鼠中了解苯并（a）re和3-羟基苯并（a）bio生物标志物的联系动力学
4. Monitoring benzo(a)pyrene exposure using laser-excited Shpol'skii spectroscopy of benzo(a)pyrene metabolites [C] . Freek Ariese, S.J. Kok, M.Verkaik Free Univ. of Amsterdam Amsterdam Netherlands, International conference on monitorning of toxic chemicals and biomarkers . 1993

机译：使用激光激发的Shpol'skii光谱法监测苯并（a）芘暴露的苯并（a）芘代谢物
5. Benzo(a)pyrene and benzo(a)pyrene-induced protein adducts in hair as biomarkers of toxic benzo(a)pyrene exposures. [D] . Campbell, Sarah Colleen. 2011

机译：苯并（a）and和苯并（a）-诱导的头发蛋白质加合物是有毒苯并（a）exposure暴露的生物标志物。
6. Enzymatic conversion of benzo(a)pyrene leading predominantly to the diol-epoxide r-7t-8-dihydroxy-t-910-oxy-78910-tetrahydrobenzo(a)pyrene through a single enantiomer of r-7 t-8-dihydroxy-78-dihydrobenzo(a)pyrene. [O] . S K Yang, D W McCourt, P P Roller, 1976

机译：通过单一对映异构体将苯并（a）py主要转化为二醇-环氧化物r-7t-8-二羟基-t-910-氧基-78910-四氢苯并（a）py r-7t-8-二羟基-78-二氢苯并（a）py的合成。
7. Changes in biochemical and physiological indices in animals produced by the combined effect of benz [a] pyrene and phenol. [O] . Skvortsova, N N, Vysochina, I V 1976

机译：苯并[a] and和苯酚的共同作用产生的动物生化和生理指标变化。
8. Exposure and Risk Assessment for Benzo(a)pyrene and Other Polycyclic Aromatic Hydrocarbons. Volume 4. Benzo(a)pyrene, Acenaphthylene, Benz(a)anthracene, Chrysene, Dibenz(a,h)anthracene, Benzo(b)fluoranthene, Benzo(k)fluoranthene, Benzo(g,h,i)perylene, Indeno(1,2,3-c,d)pyrene [R] . Perwak, J. , Byrne, M. , Coons, S. , 1982

机译：苯并（a）芘和其他多环芳烃的暴露和风险评估。第4卷。苯并（a）芘，a烯，苯并（a）蒽，Chrysene，Dibenz（a，h）蒽，苯并（b）荧蒽，苯并（k）荧蒽，苯并（g，h，i）per，Indeno （1,2,3-C，d）芘

Changes in biochemical and physiological indices in animals produced by the combined effect of benz a pyrene and phenol.

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