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小鼠表皮黄嘌呤氧化酶活性:与肿瘤启动子诱导的增生程度的相关性。

Murine epidermal xanthine oxidase activity: correlation with degree of hyperplasia induced by tumor promoters.

作者信息

Pence B C, Reiners J J

机构信息

University of Texas System Cancer Center, Science Park--Research Division, Smithville 78957.

出版信息

Cancer Res. 1987 Dec 1;47(23):6388-92.

PMID:3677084
Abstract

Topical application of the tumor promoter 12-O-tetradecanoylphorbol-13-acetate (TPA) to SENCAR mouse skin results within 48 h in a 3-fold elevation of xanthine oxidase (XO) activity, an enzyme capable of generating the reactive oxygen species superoxide and hydrogen peroxide. The antiinflammatory steroid fluocinolone acetonide, an inhibitor of TPA-induced hyperplasia, as well as the multiple stages of tumor promotion as defined in SENCAR mice (Stages I and II), inhibited the TPA-dependent elevation of epidermal XO activity. Neither tosylphenylalanyl chloromethyl ketone nor retinoic acid, inhibitors of promotion Stages I and II, respectively, had significant effects on TPA-induced hyperplasia or elevated XO activity. The nonpromoting but hyperplasiogenic agents ethyl phenylpropiolate and acetic acid significantly elevated XO activity within 48 h of topical application. The non-phorbol ester tumor promoter benzoyl peroxide also elevated XO activity consistent with the degree of induced hyperplasia. Multiple treatments with TPA or ethyl phenylpropiolate resulted in a sustained elevation of XO activity which peaked at five treatments and then declined. Sustained inhibition of XO activity by p.o. administration of allopurinol did not inhibit the TPA-induced hyperplasia as determined histologically. These results suggest that the TPA-dependent elevation of epidermal XO activity is associated with the hyperplasia induced by the agent, and is a consequence of the hyperplasia rather than the cause of it.

摘要

将肿瘤促进剂12 - O - 十四酰佛波醇 - 13 - 乙酸酯(TPA)局部应用于SENCAR小鼠皮肤,48小时内黄嘌呤氧化酶(XO)活性升高3倍,XO是一种能够产生活性氧超氧化物和过氧化氢的酶。抗炎类固醇氟轻松丙酮化物是TPA诱导增生的抑制剂,也是SENCAR小鼠中定义的肿瘤促进的多个阶段(I期和II期)的抑制剂,它抑制了TPA依赖性的表皮XO活性升高。分别作为促进I期和II期抑制剂的甲苯磺酰苯丙氨酰氯甲基酮和视黄酸,对TPA诱导的增生或XO活性升高均无显著影响。非促进但能引起增生的试剂苯丙炔酸乙酯和乙酸在局部应用48小时内显著提高了XO活性。非佛波酯类肿瘤促进剂过氧化苯甲酰也提高了XO活性,且与诱导增生的程度一致。用TPA或苯丙炔酸乙酯多次处理导致XO活性持续升高,在五次处理时达到峰值,然后下降。口服别嘌呤醇持续抑制XO活性,但组织学检查显示并未抑制TPA诱导的增生。这些结果表明,TPA依赖性的表皮XO活性升高与该试剂诱导的增生相关,是增生所致而非增生的原因。

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