Inhibition of tumour development in the partially resected, proliferating rat urinary bladder.

Acta histochemica. Supplementband Pub Date : 1990-01-01
E Kunze
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Abstract

Autoradiographic studies have shown that the urothelium of the rat urinary bladder is capable to considerably proliferate in response to a partial cystectomy (one-third resection of the bladder) as is indicated by a 190-fold increase of the 3H-thymidine labelling index above normal levels 45 h postoperatively and an enormous increase of the compartment of proliferating cells (so-called growth fraction). The stimulated urothelial proliferation can be synchronized by multiple, fractionated doses of hydroxyurea (HU), resulting in a high degree of synchrony. Based on these findings, the partial cystectomy model seemed to be a useful tool to examine whether stimulated proliferation exerts a modifying effect on initiation of urothelial carcinogenesis. Following feeding N-butyl-N-(4-hydroxybutyl)-nitrosamine by gavage in 3 fractionated doses during most pronounced proliferation 30, 45 and 70 h postoperatively, the development of bladder tumors proved to be significantly dose- and time-related inhibited. Accordingly, N-methyl-N-nitrosourea (MNU)-induced tumour formation was considerably reduced following intravesicular instillation of the carcinogen at a single dose 45 h postoperatively, when stimulated DNA synthesis reached its peak. Experiments testing a possible cell cycle specific dependence of MNU-initiated tumor development in the partially resected bladder after synchronization of the stimulated proliferation by HU revealed an inhibition of urothelial carcinogenesis in particular, when the carcinogen was administered during the early DNA synthesis phase. The mechanisms underlying the observed inhibition of tumor development in the regeneration urinary bladder are unknown. It is assumed that an increased capacity of the proliferating urothelial cells to repair carcinogen-induced DNA-damage may play an important role.

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部分切除增殖大鼠膀胱肿瘤发展的抑制作用。
放射自显像研究表明,大鼠膀胱尿路上皮在部分膀胱切除术(三分之一的膀胱切除)后能够显著增殖,如术后45小时3h -胸腺嘧啶标记指数比正常水平增加190倍,增殖细胞的隔室(所谓的生长分数)大幅增加所示。不同剂量的羟基脲(HU)可同步刺激尿路上皮的增殖,导致高度同步性。基于这些发现,部分膀胱切除术模型似乎是一种有用的工具,可以检查刺激的增殖是否对尿路上皮癌变的发生起调节作用。在术后增殖最明显的30,45和70 h,分3次灌胃n -丁基-n -(4-羟基丁基)-亚硝胺后,膀胱肿瘤的发展被证明具有显著的剂量和时间相关性。因此,术后45小时,当刺激的DNA合成达到峰值时,n -甲基-n -亚硝基脲(MNU)诱导的肿瘤形成显著减少。在HU刺激的增殖同步后,部分切除膀胱中mnu引发的肿瘤发展可能存在细胞周期特异性依赖的实验显示,当致癌物在早期DNA合成阶段给予时,对尿路上皮癌的发生有抑制作用。在再生膀胱中观察到的抑制肿瘤发展的机制尚不清楚。据推测,增殖的尿路上皮细胞修复致癌物质诱导的dna损伤的能力增加可能起重要作用。
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