Gray R, Peto R, Brantom P, Grasso P
Nuffield Department of Clinical Medicine, Radcliffe Infirmary, Oxford, United Kingdom.
Cancer Res. 1991 Dec 1;51(23 Pt 2):6470-91.
In parallel with a larger experiment on 4080 rats fed 16 different concentrations of N-nitrosodiethylamine (NDEA) or N-nitrosodimethylamine (NDMA) from 6 weeks of age, a variety of smaller experiments on a total of 1040 rodents were undertaken and are the subject of the present report. Three separate subjects were addressed. Studies of 16 different concentrations of N-nitrosopyrrolidine and N-nitrosopiperidine given from age 6 weeks onwards to small groups of rats yielded dose-response relationships for the effects of N-nitrosopyrrolidine on liver tumors and for those of N-nitrosopiperidine on tumors of the liver and upper gastrointestinal tract that resembled those seen for NDMA and NDEA, respectively, except that N-nitrosopyrrolidine and N-nitrosopiperidine were less potent [the respective dose rates needed to halve the proportion of tumorless survivors after 2 years of treatment being approximately 0.4 (males) and 0.6 (females) mg/kg adult body weight/day for each agent]. Alternatively, it was estimated that the risks to rats from lifelong exposure to 1 microgram/kg adult body weight/day of each agent might be about 0.1%, and that the risks to rats from lower doses would be proportionately less. Studies of 16 different concentrations of NDEA on small groups of female mice and female hamsters yielded the types of dose response that would be expected for upper gastrointestinal tumors, liver cell tumors, and Kupffer cell tumors in mice (no other types of liver tumor being produced, in contrast with previous reports) and for tracheal and liver cell tumors in hamsters (no clear effect on upper gastrointestinal tumors being apparent in hamsters). The dose rates needed to halve the proportion of tumorless survivors after 2 years of treatment were approximately 0.3 mg/kg adult body weight/day, i.e., 5 times that for the same agent in rats. In part, however, this may be because treatment started at an older age in these species. Studies were undertaken of the effects on esophageal and liver tumorigenesis of starting the treatment of rats with NDEA at 3 or at 20 weeks of age instead of at 6 weeks of age (as in the main experiment). Earlier treatment resulted in slightly greater dosage rates, if dosage was measured in mg/kg/day, and hence in a correspondingly more rapid yield of esophageal tumors, but the effect was not large. By contrast, an earlier start to treatment resulted, after a fixed duration of treatment, in animals having a 3-fold higher incidence rate of liver tumors, while a later start resulted in a 2-fold decrease.(ABSTRACT TRUNCATED AT 400 WORDS)
在一项针对4080只大鼠的规模更大的实验中,从6周龄起给它们喂食16种不同浓度的N-亚硝基二乙胺(NDEA)或N-亚硝基二甲胺(NDMA),与此同时,还开展了一系列针对总共1040只啮齿动物的规模较小的实验,这些实验是本报告的主题。涉及三个不同的主题。对6周龄起的小群大鼠给予16种不同浓度的N-亚硝基吡咯烷和N-亚硝基哌啶进行研究,得出了N-亚硝基吡咯烷对肝肿瘤影响以及N-亚硝基哌啶对肝和上消化道肿瘤影响的剂量反应关系,这两种关系分别类似于NDMA和NDEA的剂量反应关系,只是N-亚硝基吡咯烷和N-亚硝基哌啶的效力较低[两种物质在治疗2年后使无肿瘤存活者比例减半所需的各自剂量率,成年体重每千克每天约为0.4毫克(雄性)和0.6毫克(雌性)]。或者据估计,大鼠终生每天每千克成年体重暴露于1微克该物质的风险约为0.1%,较低剂量的风险相应更低。对小群雌性小鼠和雌性仓鼠给予16种不同浓度的NDEA进行研究,得出了小鼠上消化道肿瘤、肝细胞肿瘤和库普弗细胞肿瘤(与之前报告不同,未产生其他类型的肝肿瘤)以及仓鼠气管和肝细胞肿瘤(对仓鼠上消化道肿瘤无明显影响)预期的剂量反应类型。治疗2年后使无肿瘤存活者比例减半所需的剂量率约为成年体重每千克每天0.3毫克,即该物质对大鼠所需剂量率的5倍。然而,部分原因可能是这些物种开始治疗的年龄较大。开展了研究,观察在3周龄或20周龄而非6周龄(如在主要实验中)开始用NDEA治疗大鼠对食管和肝肿瘤发生的影响。如果以毫克/千克/天来衡量剂量,更早开始治疗会导致剂量率略高,因此食管肿瘤的产生相应更快,但影响不大。相比之下,在固定治疗期后,更早开始治疗会使动物肝肿瘤发病率高出3倍,而更晚开始治疗则会使发病率降低2倍。(摘要截取自400字)
