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新型斑马鱼多囊肾病模型揭示 Hippo 通路在肾脏囊肿发生中的作用。

Novel zebrafish polycystic kidney disease models reveal functions of the Hippo pathway in renal cystogenesis.

机构信息

Department of Biomedical Sciences and Centre of Reproduction, Development and Aging (CRDA), Faculty of Health Sciences, University of Macau, Taipa, Macau 999078, China.

出版信息

Dis Model Mech. 2021 Nov 1;14(11). doi: 10.1242/dmm.049027. Epub 2021 Nov 9.

Abstract

The Hippo signaling pathway is a kinase cascade that plays an important role in organ size control. As the main effectors of the Hippo pathway, transcription coactivators Yap1/Wwtr1 are regulated by the upstream kinase Stk3. Recent studies in mammals have implicated the Hippo pathway in kidney development and kidney diseases. To further illustrate its roles in vertebrate kidney, we generated a series of zebrafish mutants targeting stk3, yap1 and wwtr1 genes. The stk3-/- mutant exhibited edema, formation of glomerular cysts and pronephric tubule dilation during the larval stage. Interestingly, disruption of wwtr1, but not yap1, significantly alleviated the renal phenotypes of the stk3-/- mutant, and overexpression of Wwtr1 with the CMV promoter also induced pronephric phenotypes, similar to those of the stk3-/- mutant, during larval stage. Notably, adult fish with Wwtr1 overexpression developed phenotypes similar to those of human polycystic kidney disease (PKD). Overall, our analyses revealed roles of Stk3 and Wwtr1 in renal cyst formation. Using a pharmacological approach, we further demonstrated that Stk3-deficient zebrafish could serve as a PKD model for drug development.

摘要

Hippo 信号通路是一个激酶级联反应,在器官大小控制中发挥重要作用。作为 Hippo 通路的主要效应物,转录共激活因子 yap1/Wwtr1 受上游激酶 Stk3 的调节。最近在哺乳动物中的研究表明 Hippo 通路参与了肾脏发育和肾脏疾病。为了进一步阐明其在脊椎动物肾脏中的作用,我们针对 stk3、yap1 和 wwtr1 基因生成了一系列斑马鱼突变体。stk3-/- 突变体在幼虫期表现出水肿、肾小球囊肿形成和前肾管扩张。有趣的是,wwtr1 的破坏,而不是 yap1 的破坏,显著缓解了 stk3-/- 突变体的肾脏表型,并且用 CMV 启动子过表达 Wwtr1 也在前肾管期诱导了类似于 stk3-/- 突变体的表型。值得注意的是,过表达 Wwtr1 的成年鱼表现出类似于人类多囊肾病 (PKD) 的表型。总体而言,我们的分析揭示了 Stk3 和 Wwtr1 在肾脏囊肿形成中的作用。使用药理学方法,我们进一步证明 Stk3 缺陷型斑马鱼可以作为 PKD 药物开发的模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/785f/8592019/fe69c488b157/dmm-14-049027-g1.jpg

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