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围生期小鼠组织的肿瘤反应及其在化学致癌作用中的意义。

Neoplastic response of mouse tissues during perinatal age periods and its significance in chemical carcinogenesis.

作者信息

Vesselinovitch S D, Rao K V, Mihailovich N

出版信息

Natl Cancer Inst Monogr. 1979 May(51):239-50.

PMID:384263
Abstract

A series of studies pertaining to perinatal carcinogenesis have been reviewed. Their main objective was development and definition of a sensitivity biologic model for carcinogenicity screening. Data were summarized on factors modifying the carcinogenic response of various tissues following transplacental, neonatal-infant, or adult exposure of (B57BL/6J X C3HeB/FeJ)F1 mice to a single administration of ENU. In addition, tumor response of mice treated during specific perinatal age periods with DEN, BP, aflatoxin B1, benzidine . 2HCl, DDT, dieldrin, and safrole were analyzed. The results revealed that the age of the animals at the time of carcinogenic exposure has been the most effective modulator of carcinogenesis in liver, lung, stomach, ovary, and lymphoreticular tissues. Infancy proved to be the most susceptible period to carcinogenesis as demonstrated by a great variety of tissues that responded to treatment and the incidence of tumors which developed. Depending on the nature of carcinogen, variation in organ sites undergoing carcinogenesis was considerable, apparently due to difference in their enzymatic competence to activate and metabolize the agent. Thus a single treatment with ENU, a spontaneously activated type of procarcinogen, induced 59 primary types of tumors in 22 tissues. In contrast, treatment of infants by procarcinogens requiring enzymatic activation led to development of tumors only at a limited number of tissue sites. However, regardless of the type of carcinogen used, the liver consistently responded with development of tumors. Detailed morphologic and biologic evaluations of the induced liver tumors demonstrated in addition to the benign neoplastic variety, the presence of the frank malignant tumors. The character of tumors was dependent not only on carcinogenicity of the agent used but also on the age of mice at the time of carcinogenic treatment. Perinatally induced primary liver tumors showed greater tendency to metastasize and were more readily transplantable into an isogeneic host than those induced at later age periods. Data showed the advantage of prenatal and/or postnatal treatment in combination of life-long exposures to test agents as a more sensitive bioassay system in comparison with solely postweaning treatment. Because the early age period is the most sensitivity life phase to carcinogenesis, it appears to be a good model for prescreening various potential carcinogens, especially when only small amounts of test substances are available. The importance of the proper relationship of such bioassay to the other test systems regarding assessment of potential human risk has been emphasized.

摘要

对一系列有关围产期致癌作用的研究进行了综述。其主要目标是开发并定义一种用于致癌性筛查的敏感性生物学模型。总结了关于(B57BL/6J×C3HeB/FeJ)F1小鼠经胎盘、新生儿期或成年期暴露于单次给予ENU后,影响各种组织致癌反应的因素的数据。此外,还分析了在特定围产期年龄段用二乙基亚硝胺(DEN)、苯并芘(BP)、黄曲霉毒素B1、联苯胺二盐酸盐、滴滴涕(DDT)、狄氏剂和黄樟素处理的小鼠的肿瘤反应。结果表明,致癌暴露时动物的年龄是肝脏、肺、胃、卵巢和淋巴网状组织中致癌作用最有效的调节因素。婴儿期被证明是对致癌作用最敏感的时期,这体现在多种对治疗有反应的组织以及所发生肿瘤的发生率上。根据致癌物的性质,发生致癌作用的器官部位差异很大,这显然是由于它们激活和代谢该物质的酶活性不同所致。因此,单次给予ENU(一种自发激活型的前致癌物)可在22种组织中诱发59种原发性肿瘤类型。相比之下,用需要酶激活的前致癌物处理婴儿仅导致在有限数量的组织部位发生肿瘤。然而,无论使用何种类型的致癌物,肝脏始终会出现肿瘤。对诱发的肝脏肿瘤进行的详细形态学和生物学评估表明,除了良性肿瘤类型外,还存在明显的恶性肿瘤。肿瘤的特征不仅取决于所用致癌物的致癌性,还取决于致癌处理时小鼠的年龄。围产期诱发的原发性肝脏肿瘤比后期诱发的肿瘤更易发生转移,并且更容易移植到同基因宿主中。数据显示,与仅在断奶后处理相比,产前和/或产后处理结合终生暴露于受试物作为一种更敏感的生物测定系统具有优势。由于早期是对致癌作用最敏感的生命阶段,它似乎是预筛各种潜在致癌物的良好模型,尤其是当只有少量受试物质可用时。强调了这种生物测定与其他测试系统在评估潜在人类风险方面保持适当关系的重要性。

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