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在表达A2a腺苷受体基因和人乳头瘤病毒16型E7癌基因的转基因小鼠中转移性分化型甲状腺癌的早期发生。

Early occurrence of metastatic differentiated thyroid carcinomas in transgenic mice expressing the A2a adenosine receptor gene and the human papillomavirus type 16 E7 oncogene.

作者信息

Coppée F, Gérard A C, Denef J F, Ledent C, Vassart G, Dumont J E, Parmentier M

机构信息

IRIBHN, Université Libre de Bruxelles, Campus Erasme, Belgium.

出版信息

Oncogene. 1996 Oct 3;13(7):1471-82.

PMID:8875985
Abstract

We report here the characterization of a transgenic mouse model (Tg-A2aR/Tg-E7) resulting from the coexpression of two oncogenic transgenes in the thyroid. The two transgenes (Tg-A2aR and Tg-E7) were placed under control of the thyroid specific thyroglobulin gene promoter, and directed the expression of either the A2a adenosine receptor that constitutively activates the cAMP pathway, or the E7 protein of the human papillomavirus type 16, that binds and inactivates the retinoblastoma susceptibility gene product (Rb1). Transgenic mice expressing both transgenes were generated by interbreeding the Tg-A2aR and Tg-E7 transgenic lines, generated and characterized previously (Ledent et al., 1992, 1995). These mice develop a larger goiter than that of the two parental lines, and a severe hyperthyroidism comparable to that observed in the Tg-A2aR parental line. The main feature of the Tg-A2aR/Tg-E7 mice is the rapid occurrence of malignant lesions, and the dissemination of malignant thyroid tissue through the blood stream, generating multiple differentiated and functional metastases in the lung. These metastases appeared as early as 2 months after birth and their frequency increased to 75% over 3 months. They were associated with the presence of large vascular lakes in the thyroid. Electron microscopy of the malignant cells revealed nuclear features similar to those of human thyroid papillary carcinoma. These mice, in which two oncogenes are co-expressed in the thyroid, represent the first genetic animal model developing metastatic differentiated carcinomas of the thyroid with a high frequency.

摘要

我们在此报告一种转基因小鼠模型(Tg-A2aR/Tg-E7)的特征,该模型由甲状腺中两个致癌转基因的共表达产生。这两个转基因(Tg-A2aR和Tg-E7)置于甲状腺特异性甲状腺球蛋白基因启动子的控制之下,分别指导组成性激活cAMP途径的A2a腺苷受体或人乳头瘤病毒16型的E7蛋白的表达,后者可结合并使视网膜母细胞瘤易感基因产物(Rb1)失活。通过将先前已构建并鉴定的Tg-A2aR和Tg-E7转基因品系进行杂交,培育出同时表达这两个转基因的转基因小鼠(Ledent等人,1992年,1995年)。这些小鼠形成的甲状腺肿比两个亲本品系更大,且出现了与Tg-A2aR亲本品系中观察到的严重程度相当的甲状腺功能亢进。Tg-A2aR/Tg-E7小鼠的主要特征是恶性病变迅速发生,恶性甲状腺组织通过血流扩散,在肺部产生多个分化且有功能的转移灶。这些转移灶在出生后2个月就已出现,3个月内其发生率增至75%。它们与甲状腺中存在大的血管湖有关。恶性细胞的电子显微镜检查显示出与人类甲状腺乳头状癌相似的核特征。在这些小鼠中,两个癌基因在甲状腺中共表达,它们代表了首个高频发生转移性分化型甲状腺癌的遗传动物模型。

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