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β-连环蛋白信号过度激活导致小鼠睾丸支持细胞瘤的发生。

Overactive beta-catenin signaling causes testicular sertoli cell tumor development in the mouse.

作者信息

Chang Hao, Guillou Florian, Taketo Makoto M, Behringer Richard R

机构信息

Program in Genes and Development, The University of Texas Graduate School of Biomedical Sciences at Houston, Houston, Texas, USA.

出版信息

Biol Reprod. 2009 Nov;81(5):842-9. doi: 10.1095/biolreprod.109.077446. Epub 2009 Jun 24.

Abstract

Overactive WNT/beta-catenin signaling has been found in many forms of cancer in human patients. Mouse models with mutations in different components of the WNT/beta-catenin signaling pathway have been generated to mimic tumorigenesis in humans. Mice with mutations that result in overactive WNT/beta-catenin signaling developed tumors in some tissues, such as digestive tract, skin, and ovary, but they failed to develop tumors in other tissues, such as mammary gland, liver, kidney, and primordial germ cells. To investigate whether overactive beta-catenin signaling is capable of inducing Sertoli cell tumorigenesis in testes, we generated Ctnnb1(tm1Mmt/+);Tg(AMH-cre)1Flor male mice that express a constitutively active form of beta-catenin specifically in Sertoli cells. No tumors were observed at 4 mo of age, but 70% of the mutant males developed Sertoli cell tumors at 8 mo of age. At 1 yr of age, more than 90% of the mutant males developed tumors. No instances of extratesticular spread of the tumors were found in the mutant mice. These studies show a causal link between overactive WNT/beta-catenin signaling and Sertoli cell tumor development and provide a novel mouse model for the study of Sertoli cell tumor biology.

摘要

在人类患者的多种癌症中都发现了WNT/β-连环蛋白信号通路过度活跃的情况。人们构建了WNT/β-连环蛋白信号通路不同组分发生突变的小鼠模型,以模拟人类的肿瘤发生过程。WNT/β-连环蛋白信号通路过度活跃的突变小鼠在某些组织中会发生肿瘤,比如消化道、皮肤和卵巢,但在其他组织中却不会发生肿瘤,如乳腺、肝脏、肾脏和原始生殖细胞。为了研究过度活跃的β-连环蛋白信号是否能够诱导睾丸支持细胞瘤的发生,我们构建了Ctnnb1(tm1Mmt/+);Tg(AMH-cre)1Flor雄性小鼠,其在支持细胞中特异性表达持续激活形式的β-连环蛋白。在4月龄时未观察到肿瘤,但70%的突变雄性小鼠在8月龄时发生了支持细胞瘤。在1岁时,超过90%的突变雄性小鼠发生了肿瘤。在突变小鼠中未发现肿瘤发生睾丸外扩散的情况。这些研究表明WNT/β-连环蛋白信号过度活跃与支持细胞瘤发生之间存在因果关系,并为支持细胞瘤生物学研究提供了一种新的小鼠模型。

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