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由突变型H-ras转基因表达诱导的皮肤肿瘤的恶性能力取决于所靶向的细胞类型。

The malignant capacity of skin tumours induced by expression of a mutant H-ras transgene depends on the cell type targeted.

作者信息

Brown K, Strathdee D, Bryson S, Lambie W, Balmain A

机构信息

CRC Beatson Laboratories Department of Medical Oncology Alexander Stone Building University of Glasgow Garscube Estate, Switchback Road, Bearsden, Glasgow, G61 1BD, UK.

出版信息

Curr Biol. 1998 Apr 23;8(9):516-24. doi: 10.1016/s0960-9822(98)70203-9.

DOI:10.1016/s0960-9822(98)70203-9
PMID:9560338
Abstract

BACKGROUND

. Pinpointing the cells from which tumours arise is a major challenge n tumour biology. Previous work has shown that the targeted expression of a mutant ras gene within the interfollicular cell compartment of mouse skin induces the formation of benign papillomas, but these do not spontaneously progress to malignancy. We have investigated the carcinogenic effects of expressing the same oncogene in a different population of epidermal cells.

RESULTS

Expression of mutant ras from a truncated keratin 5 gene promoter, which directs expression to the follicular and interfollicular cells of newborn mice and the hair follicle cells of adults, stimulated the development of acanthotic areas in newborn mice. Within one week of birth, the acanthotic skin developed areas of carcinoma in situ and adult mice developed papillomas and keratoacanthomas, the latter having a high frequency of spontaneous malignant transformation to squamous and occasionally spindle carcinomas. The benign tumours that arose had several hallmarks of tumours at a high risk of malignant progression, including suprabasal cell proliferation and heterogeneous expression of keratin 13. In contrast to tumours induced by expressing mutant ras under the control of the keratin 10 or keratin 1 gene promoters, the formation of these lesions was not dependent on wounding or a tumour promoter.

CONCLUSIONS

Benign tumours that are at a risk of malignant conversion are primarily derived from cells located within the hair follicle, and the nature of the cell in which tumour initiation occurs is a major determinant of malignant potential.

摘要

背景

确定肿瘤起源的细胞是肿瘤生物学中的一项重大挑战。先前的研究表明,在小鼠皮肤的滤泡间细胞区室中靶向表达突变型ras基因可诱导良性乳头状瘤的形成,但这些乳头状瘤不会自发进展为恶性肿瘤。我们研究了在不同表皮细胞群体中表达相同癌基因的致癌作用。

结果

从截短的角蛋白5基因启动子表达突变型ras,该启动子将表达导向新生小鼠的滤泡和滤泡间细胞以及成年小鼠的毛囊细胞,刺激了新生小鼠棘皮化区域的发展。出生后一周内,棘皮化皮肤出现原位癌区域,成年小鼠出现乳头状瘤和角化棘皮瘤,后者有很高频率自发恶性转化为鳞状癌,偶尔也会转化为梭形癌。所产生的良性肿瘤具有恶性进展高风险肿瘤的几个特征,包括基底上层细胞增殖和角蛋白13的异质性表达。与在角蛋白10或角蛋白1基因启动子控制下表达突变型ras诱导的肿瘤不同,这些病变的形成不依赖于创伤或肿瘤启动子。

结论

有恶性转化风险的良性肿瘤主要来源于毛囊内的细胞,肿瘤起始细胞的性质是恶性潜能的主要决定因素。

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