Peraino C, Carnes B A, Stevens F J, Staffeldt E F, Russell J J, Prapuolenis A, Blomquist J A, Vesselinovitch S D, Maronpot R R
Biological, Environmental, and Medical Research Division, Argonne National Laboratory, Illinois 60439.
Cancer Res. 1988 Aug 1;48(15):4171-8.
Previous investigations in this laboratory have provided evidence that histochemically detectable altered hepatocyte foci and hepatic tumors appearing in rats given a single neonatal treatment with a low dose of carcinogen followed by chronic dietary phenobarbital administration are developmentally independent. The present investigation further evaluates developmental relationships among these lesions. Altered hepatocyte foci were divided into two subclasses consisting of foci that were detectable by histochemical as well as by hematoxylin-eosin staining [designated hist(+)/morph(+) foci] and those foci that were detectable solely by histochemical staining [designated hist(+)/morph(-) foci]. The developmental and phenotypic properties of the hist(+)/morph(-) foci, hist(+)/morph(+) foci, and hepatic tumors were compared in rats initiated once neonatally with different doses of diethylnitrosamine and promoted with dietary phenobarbital from weaning. The morph(+) and morph(-) lesion subclasses were distinguishable on the basis of several developmental characteristics. Hist(+)/morph(+) foci were present at low frequency until at least 150 days after initiation. Although the development of hist(+)/morph(-) foci was essentially complete at that point, the rate of appearance of hist(+)/morph(+) increased significantly. The diethylnitrosamine dose response of the hist(+)/morph(+) foci followed the histochemical marker patterns of the tumor lesion class more closely than that of the hist(+)/morph(-) group. The rates of expression of the hist(+)/morph(+) foci increased with the increasing level of histochemical complexity, whereas the rates of expression of the hist(+)/morph(-) foci groups were inversely correlated to their complexity level. Although the average focus size or diameter in the hist(+)/morph(+) groups was greater than that of the hist(+)/morph(-) foci, the focus growth rates of morph(+) and morph(-) subsets matched for histochemical phenotype were comparable. The complexity level and individual marker distribution patterns of the hist(+)/morph(+) focus class were more similar to tumor patterns than to the distribution patterns of the hist(+)/morph(-) lesion class. The results suggest the following. (a) The development of lesion classes with successively greater deviation from normalcy does not occur via lineal progression from less to more deviated forms within a given lesion class. The three lesion classes appear to develop independently, with the developmental characteristics of each lesion class determined at the time of initiation.(ABSTRACT TRUNCATED AT 400 WORDS)
本实验室之前的研究已提供证据表明,在新生大鼠接受低剂量致癌物单次处理后,再给予慢性饮食苯巴比妥,所出现的组织化学可检测到的肝细胞灶改变和肝肿瘤在发育上是独立的。本研究进一步评估了这些病变之间的发育关系。改变的肝细胞灶被分为两个亚类,一类是通过组织化学以及苏木精 - 伊红染色均可检测到的灶[称为组织化学(+)/形态学(+)灶],另一类是仅通过组织化学染色可检测到的灶[称为组织化学(+)/形态学(-)灶]。在新生大鼠一次性给予不同剂量的二乙基亚硝胺并从断奶起用饮食苯巴比妥促进的大鼠中,比较了组织化学(+)/形态学(-)灶、组织化学(+)/形态学(+)灶和肝肿瘤的发育及表型特性。形态学(+)和形态学(-)病变亚类在几个发育特征的基础上是可区分的。组织化学(+)/形态学(+)灶在启动后至少150天内出现频率较低。虽然此时组织化学(+)/形态学(-)灶的发育基本完成,但组织化学(+)/形态学(+)灶的出现率显著增加。组织化学(+)/形态学(+)灶的二乙基亚硝胺剂量反应比组织化学(+)/形态学(-)组更紧密地遵循肿瘤病变类别的组织化学标记模式。组织化学(+)/形态学(+)灶的表达率随着组织化学复杂性水平的增加而增加,而组织化学(+)/形态学(-)灶组的表达率与其复杂性水平呈负相关。虽然组织化学(+)/形态学(+)组中平均灶大小或直径大于组织化学(+)/形态学(-)灶,但形态学(+)和形态学(-)亚组中与组织化学表型匹配的灶生长率相当。组织化学(+)/形态学(+)灶类别的复杂性水平和个体标记分布模式与肿瘤模式比与组织化学(+)/形态学(-)病变类别的分布模式更相似。结果表明如下。(a)与正常状态偏差越来越大的病变类别的发展并非通过给定病变类别内从偏差较小的形式向偏差较大的形式的线性进展发生。这三类病变似乎是独立发展的,每个病变类别的发育特征在启动时就已确定。(摘要截短于400字)
