[3'-甲基-4-二甲氨基偶氮苯(3'-MeDAB)处理大鼠肝癌发生过程中血清和肝组织胸苷激酶活性的变化]。

Nihon Gan Chiryo Gakkai shi Pub Date : 1990-12-20
S Sakamoto, K Kuwa, Y Kawachi, H Kudo, N Kasahara, T Kato, R Okamoto, H Taga, H Hirai, T Sunaga
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引用次数: 0

摘要

已知3'-甲基-4-二甲氨基偶氮苯(3'-MeDAB)可诱导大鼠肝脏高发病率的肝细胞癌。在本研究中,我们检测了3′-MeDAB处理大鼠肝脏中血清甲胎蛋白(AFP)、胸苷激酶(TK)、救助途径dna合成酶水平以及组织TK及其同工酶活性。3′-MeDAB治疗开始后,血清TK活性突然升高,1周后达到峰值,随后逐渐下降。3周时,血清TK虽有所下降,但血清AFP和组织TK开始升高,肝脏出现卵形细胞。5周时,血清TK虽降至最低点,但血清AFP和组织TK均出现短暂峰值,椭圆形细胞占肝小叶的主要部分,伴增厚结节。此后,血清TK继续升高,血清AFP和组织TK在短暂下降后又再次升高;20周时,各指标均处于较高水平,可见混合型肝癌。采用deae -纤维素柱层析法将肝脏TK同工酶分为3种类型。3'-MeDAB在5周和20周时诱导肝脏非肿瘤区细胞质和胎儿型同工酶活性显著增加。这些结果表明,3'- medab处理大鼠肝脏的生化变化可能为肝癌发生的两步过程提供了有价值的见解。
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[Thymidine kinase activities in sera and liver tissues during hepatocarcinogenesis in rats treated with 3'-methyl-4-dimethylaminoazobenzene (3'-MeDAB)].

It is known that a high incidence of hepatocellular carcinoma in rat liver can be induced with 3'-methyl-4-dimethylaminoazobenzene (3'-MeDAB). In the present study, we investigated serum levels of alpha-fetoprotein (AFP) and thymidine kinase (TK), DNA-synthesizing enzyme in the salvage pathway, and tissue TK and its isozyme activities in the liver of rats treated with 3'-MeDAB. Serum TK activities rose abruptly right after the onset of 3'-MeDAB treatment, peaking after one week and then gradually decreasing. At 3 weeks, though serum TK was decreasing, serum AFP and tissue TK began to increase, and oval cells appeared in the liver. At 5 weeks, though serum TK reached a nadir, serum AFP and tissue TK formed transient peaks, and oval cells occupied a major part of the hepatic lobules with hyperplastic nodules. Thereafter, serum TK continued to increase, and serum AFP and tissue TK, after transiently decreasing, re-increased; at 20 weeks, each value was at high level, and mixed type hepatocarcinoma was observed. The liver TK isozymes were separated into 3 types by DEAE-cellulose column chromatography. A 3'-MeDAB induced a remarkable increase in activity of cytosolic and fetal type isozyme in non-tumorous regions of livers at 5 weeks and tumorous regions at 20 weeks. These results indicate that biochemical changes in 3'-MeDAB-treated rat liver may provide a valuable insight into two step process in hepatocarcinogenesis.

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