DMBA-induced Mammary Carcinogenesis, in Relaton to Rebound Increase of Serum Prolactin after Suppression with Bromocryptine in Pubescent Virgin Rats

F. Hara
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Abstract

Twenty six, 31 and 53 young female Sprague-Dawley rats in Groups A, C and E, respectively, were administered 10 mg/Kg Bromocryptine daily by intubation for 3 weeks from 31 to 51 days of age. Twenty five rats each in Groups B and D served as the controls. Tail blood was collected for radioimmunoassay of prolactin from only metaand di-estrus rats in Groups A, B and E around 10 am at the age of 51-58 days, and the sampling was not repeated in any animal. A rebound increase of serum prolactin level occurred within 3 days after the termination of Bromocryptine treatment. A single dose of 5mg/rat DMBA in Groups A and B and 2.5mg/rat in Groups C and D was given orally around 11 am at the age of 52 days, and the carcinogenesis with DMBA was evaluated 22 weeks after the single administration of carcinogen. Mammary adenocarcinoma developed in some animals, but no other tumors could be found. When a single weaker dose of DMBA was administered orally on the day after the cessation of the 3 week treatment with Bromocryptine, the chemical induction of mammary carcinogenesis was enhanced distinctly.
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dmba诱导的乳腺癌发生与溴隐碱抑制后血清泌乳素反弹升高有关
取A、C、E组26、31、53只年轻雌性Sprague-Dawley大鼠,从31 ~ 51日龄,每日插管给药10 mg/Kg溴隐亭,连续3周。B、D组各25只大鼠作为对照组。51 ~ 58日龄A、B、E组大鼠仅于上午10时左右采尾血进行催乳素放射免疫测定,不重复采样。停用溴隐亭后3天内血清催乳素水平出现反弹性升高。A、B组小鼠于52日龄时上午11时左右口服单剂量DMBA 5mg/只,C、D组小鼠口服2.5mg/只,在单次给药22周后评价DMBA的致癌性。一些动物出现乳腺腺癌,但未发现其他肿瘤。在停止溴隐碱治疗3周后的第二天口服单次较弱剂量的DMBA,其对乳腺癌的化学诱导作用明显增强。
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