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细胞增殖对多氯联苯纯品及混合物在抗药肝细胞体内致癌性试验中启动活性的影响。

Influence of cell proliferation on initiating activity of pure polychlorinated biphenyls and complex mixtures in resistant hepatocyte in vivo assays for carcinogenicity.

作者信息

Hayes M A, Safe S H, Armstrong D, Cameron R G

出版信息

J Natl Cancer Inst. 1985 May;74(5):1037-41.

PMID:2860266
Abstract

The abilities of various pure polychlorinated biphenyls (PCB) and complex mixtures to generate resistant gamma-glutamyltransferase (GGT)-positive hepatocellular nodules was evaluated in F344 rats in which hepatocytes were proliferating. The PCB examined were 2,2',4,4',5,5'-hexachlorobiphenyl (CAS: 35065-27-1), 2,2',4,4'-tetrachlorobiphenyl, 2,2',5,5'-tetrachlorobiphenyl, Aroclor 1254 (CAS: 11097-69-1), and a prepared mixture of pure PCB isomers and congeners similar to those found in human breast milk. The PCB were administered either to male and female suckling rats (weekly for 3 wk) during liver growth or to adult male rats (150-160 g body wt) previously subjected to two-thirds partial hepatectomy (PH). Rats were subsequently given a selection regimen consisting of 3 daily doses (20 mg/kg) of 2-acetylamino-fluorene (2-FAA; CAS: 53-96-3) followed by either PH or necrotizing carbon tetrachloride (CAS: 56-23-5) in adult rats that previously underwent PH. None of the PCB exposures generated GGT-positive nodules after selection, whereas known initiators such as diethylnitrosamine (CAS: 55-18-5), 3-methylcholanthrene (CAS: 56-49-5), benzo[a]pyrene (CAS: 50-32-8), and 2-FAA were active initiators of nodules in suckling or hepatectomized rats. These findings indicate that short-term exposures to these PCB during liver cell proliferation do not show initiating action in an in vivo assay that detects both hepatic and nonhepatic initiating carcinogens.

摘要

在肝细胞正在增殖的F344大鼠中,评估了各种纯多氯联苯(PCB)和复杂混合物产生抗γ-谷氨酰转移酶(GGT)阳性肝细胞结节的能力。所检测的PCB包括2,2',4,4',5,5'-六氯联苯(CAS:35065-27-1)、2,2',4,4'-四氯联苯、2,2',5,5'-四氯联苯、氯丹1254(CAS:11097-69-1),以及一种类似于人母乳中发现的纯PCB异构体和同系物的制备混合物。PCB在肝脏生长期间给予雄性和雌性乳鼠(每周一次,共3周),或给予先前接受过三分之二部分肝切除术(PH)的成年雄性大鼠(体重150 - 160 g)。随后,给大鼠进行一个选择方案,包括每日3次剂量(20 mg/kg)的2-乙酰氨基芴(2-FAA;CAS:53-96-3),然后在先前接受过PH的成年大鼠中进行PH或坏死性四氯化碳(CAS:56-23-5)处理。在选择后,没有一种PCB暴露产生GGT阳性结节,而已知的引发剂如二乙基亚硝胺(CAS:55-18-5)、3-甲基胆蒽(CAS:56-49-5)、苯并[a]芘(CAS:50-32-8)和2-FAA在乳鼠或肝切除大鼠中是结节的活性引发剂。这些发现表明,在肝细胞增殖期间短期暴露于这些PCB,在检测肝脏和非肝脏引发致癌物的体内试验中未显示出引发作用。

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