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乳腺中的体细胞突变:时间和发情期的影响

Somatic mutation in the mammary gland: influence of time and estrus.

作者信息

Sun B, Shima N, Heddle J A

机构信息

Department of Biology, York University, 4700 Keele Street, Toronto, Ontario, Canada.

出版信息

Mutat Res. 1999 Jun 1;427(1):11-9. doi: 10.1016/S0027-5107(99)00039-1.

Abstract

A critical factor in the quantitation of mutation induction in vivo is the time interval between treatment and sampling. In order to study mutagenesis in the mammary epithelium, the cell type in which breast cancer arises, we have measured the manifestation time, the minimum time required for the maximum mutant frequency to be achieved, in this tissue. The F1 LacZ transgenic mice (Muta MousexSWR) were treated with N-ethyl-N-nitrosourea (ENU) at 50 mg/kg for five consecutive days and then sampled at 1, 2, 4, 6, 9, or 12 weeks after the last treatment. The LacZ- mutant frequency reached a maximum at 4 weeks post-treatment and did not vary significantly thereafter. Dlb-1- mutations in the small intestine reached a maximum at 2 weeks after treatment and did not vary significantly thereafter. Since the stage of estrus cycle during carcinogen exposure influences the mammary tumor incidence and latency, it was expected that it would also affect mutation induction. To test this, F1 LacZ mice in the estrus or di-estrus stage were treated with an acute dose of 250 mg/kg ENU and sampled 10-13 weeks post-treatment. No statistical difference between the two groups was found, indicating that the effect of estrus on carcinogenesis is not due to variation in the sensitivity of the stage of the mammary gland to mutation.

摘要

体内突变诱导定量分析的一个关键因素是处理与取样之间的时间间隔。为了研究乳腺癌起源的细胞类型——乳腺上皮中的诱变作用,我们测定了该组织中的表现时间,即达到最大突变频率所需的最短时间。将F1 LacZ转基因小鼠(Muta Mouse×SWR)以50 mg/kg的剂量连续5天用N-乙基-N-亚硝基脲(ENU)处理,然后在最后一次处理后的1、2、4、6、9或12周取样。LacZ突变频率在处理后4周达到最大值,此后无显著变化。小肠中的Dlb-1突变在处理后2周达到最大值,此后无显著变化。由于致癌物暴露期间的发情周期阶段会影响乳腺肿瘤的发生率和潜伏期,因此预计它也会影响突变诱导。为了验证这一点,对处于发情期或间情期的F1 LacZ小鼠给予250 mg/kg ENU的急性剂量,并在处理后10 - 13周取样。两组之间未发现统计学差异,表明发情对致癌作用的影响并非由于乳腺腺体阶段对突变的敏感性差异。

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