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非黑色素瘤皮肤癌的小鼠模型

Mouse models of nonmelanoma skin cancer.

作者信息

Amberg Nicole, Holcmann Martin, Glitzner Elisabeth, Novoszel Philipp, Stulnig Gabriel, Sibilia Maria

机构信息

Department of Medicine I, Institute of Cancer Research, Comprehensive Cancer Center, Medical University of Vienna, Borschkegasse 8a, A-1090, Vienna, Austria.

出版信息

Methods Mol Biol. 2015;1267:217-50. doi: 10.1007/978-1-4939-2297-0_10.

DOI:10.1007/978-1-4939-2297-0_10
PMID:25636471
Abstract

The skin is the largest organ of the mammalian body, made up of multiple layers, which include the epidermis, dermis, and subcutis (Alam and Ratner, N Engl J Med 344(13):975-983, 2001). The human interfollicular epidermis can be subdivided into five different layers: (1) stratum basale, (2) stratum spinosum, (3) stratum granulosum, (4) stratum lucidum, and (5) stratum corneum, all originating from basal keratinocytes by differentiation (Hameetman et al., BMC cancer 13:58, 2013; Ramirez et al., Differentiation 58(1):53-64, 1994). The epidermis is also able to generate different appendages: hair follicles (HF) and their associated sebaceous glands (Sibilia et al., Cell 102(2):211-220, 2000) as well as sweat glands (Luetteke et al., Genes Dev 8(4):399-413, 1994). The skin has important functions in several biological processes like environmental barrier, tissue regeneration, hair cycling, and wound repair. During these processes, stem cells from the interfollicular epidermis and from the hair follicle bulge are activated to renew the epidermis or hair. The epidermis and hair undergo continuous homeostatic regeneration and mutations, upon mutations which disturb the balance of homeostatic regeneration of epidermis and hair and lead to enhanced proliferation of keratinocytes, development of skin cancer is developed. Tumors that arise in the skin are mainly of three types: malignant melanoma, arising from melanocytes, basal cell carcinoma (BCC), and squamous cell carcinoma (SCC), the latter two both arising from keratinocytes or hair follicle cells. In this chapter, we will describe some genetically engineered mouse models (GEMM) that aim at modeling human BCC and SCC and their respective precancerous lesions. We will describe the experimental approaches used in our laboratory to analyze tumor-bearing mice focusing on methods necessary for the induction of tumor growth as well as for the molecular and histological analysis of tumor tissue.

摘要

皮肤是哺乳动物身体最大的器官,由多层组成,包括表皮、真皮和皮下组织(阿拉姆和拉特纳,《新英格兰医学杂志》344(13):975 - 983,2001年)。人类非毛囊表皮可细分为五层:(1)基底层,(2)棘层,(3)颗粒层,(4)透明层,和(5)角质层,所有这些都起源于基底角质形成细胞的分化(哈梅特曼等人,《BMC癌症》13:58,2013年;拉米雷斯等人,《分化》58(1):53 - 64,1994年)。表皮还能够产生不同的附属器:毛囊(HF)及其相关的皮脂腺(西比利亚等人,《细胞》102(2):211 - 220,2000年)以及汗腺(吕特克等人,《基因与发育》8(4):399 - 413,1994年)。皮肤在几个生物学过程中具有重要功能,如环境屏障、组织再生、毛发周期和伤口修复。在这些过程中,来自非毛囊表皮和毛囊隆突的干细胞被激活以更新表皮或毛发。表皮和毛发经历持续的稳态再生和突变,当突变扰乱表皮和毛发稳态再生的平衡并导致角质形成细胞增殖增强时,就会发生皮肤癌。皮肤中出现的肿瘤主要有三种类型:源自黑素细胞的恶性黑色素瘤、基底细胞癌(BCC)和鳞状细胞癌(SCC),后两种均源自角质形成细胞或毛囊细胞。在本章中,我们将描述一些旨在模拟人类BCC和SCC及其各自癌前病变的基因工程小鼠模型(GEMM)。我们将描述我们实验室用于分析荷瘤小鼠的实验方法,重点是诱导肿瘤生长以及肿瘤组织分子和组织学分析所需的方法。

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Mouse models of nonmelanoma skin cancer.非黑色素瘤皮肤癌的小鼠模型
Methods Mol Biol. 2015;1267:217-50. doi: 10.1007/978-1-4939-2297-0_10.
2
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Early epidermal destruction with subsequent epidermal hyperplasia is a unique feature of the papilloma-independent squamous cell carcinoma phenotype in PKCepsilon overexpressing transgenic mice.早期表皮破坏并随后出现表皮增生是蛋白激酶Cε过表达转基因小鼠中不依赖乳头瘤的鳞状细胞癌表型的独特特征。
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Expression of the TGF-beta coreceptor endoglin in epidermal keratinocytes and its dual role in multistage mouse skin carcinogenesis.转化生长因子-β共受体内皮糖蛋白在表皮角质形成细胞中的表达及其在小鼠皮肤多阶段致癌过程中的双重作用。
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Evidence that initiated keratinocytes clonally expand into multiple existing hair follicles during papilloma histogenesis in SENCAR mouse skin.在SENCAR小鼠皮肤乳头瘤组织发生过程中,起始角质形成细胞克隆性扩增至多个现存毛囊的证据。
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Altered expression of interleukin-1 receptor antagonist in different stages of mouse skin carcinogenesis.白细胞介素-1受体拮抗剂在小鼠皮肤癌发生不同阶段的表达变化
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Expression of the hair stem cell-specific marker nestin in epidermal and follicular tumors.毛发干细胞特异性标志物巢蛋白在表皮和毛囊肿瘤中的表达。
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Human keratin-1.bcl-2 transgenic mice aberrantly express keratin 6, exhibit reduced sensitivity to keratinocyte cell death induction, and are susceptible to skin tumor formation.人角蛋白-1.bcl-2转基因小鼠异常表达角蛋白6,对角质形成细胞死亡诱导的敏感性降低,且易发生皮肤肿瘤。
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