Tumor persistence and regression in skin carcinogenesis. An experimental study.

F Stenbäck
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引用次数: 3

Abstract

A lifetime study in Swiss mice showed that a single 300microgram application of 7, 12-dimethylbenzanthracene (DMBA) once, or 300 or 30microgram DMBA once followed by 3.2 microgram phorbolester for 15 weeks induced a high number of skin tumors many of which regressed spontaneously. The regression occurred mostly early in the experiment, the number of appearing and regressing tumors following a cynical pattern. The incidence of regressions was only to a limited extent associated with tumor size, tumor duration and total number of tumors. Repeated DMBA treatment, 5 microgram twice a week induced the same types of tumors in larger numbers: with a smaller incidence of regressions and only if they were transient in nature, i.e., lasting less than 3 weeks. These occurred in animals which showed a large number of persisting tumors simultaneously, but which rarely displayed multiple regressions. The results indicate the occurrence of multiple steps of neoplastic transformation from hyperplastic lesions, benign regressing tumors, presistent tumors and frankly malignant ones, the incidence as well as biological behavior depending upon inducing treatment.

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皮肤癌变中肿瘤的持续与消退。一项实验性研究。
一项对瑞士小鼠的终身研究表明,单次300微克的7,12 -二甲基苯并蒽(DMBA)一次,或300或30微克的DMBA一次,然后是3.2微克的磷酯,持续15周,诱发了大量的皮肤肿瘤,其中许多自发消退。这种退化大多发生在实验的早期,出现和退化的肿瘤数量遵循一种令人怀疑的模式。回归的发生率仅在有限程度上与肿瘤大小、肿瘤持续时间和肿瘤总数相关。重复DMBA治疗,5微克,每周两次,诱导相同类型的肿瘤,数量更多,退化发生率更小,只有当它们是短暂的性质,即持续时间少于3周。这些发生在同时显示大量持续肿瘤的动物中,但很少显示多重退化。结果表明:肿瘤发生由增生性病变、良性退行性肿瘤、持续性肿瘤和明显恶性肿瘤的多个阶段,其发生率和生物学行为取决于诱导治疗。
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