Literature DB >> 24072042

Tissue-specific differences in the regulation of KIBRA gene expression involve transcription factor TCF7L2 and a complex alternative promoter system.

Katrin Guske1, Boris Schmitz, Michael Schelleckes, Kerstin Duning, Joachim Kremerskothen, Hermann J Pavenstädt, Stefan-Martin Brand, Eva Brand.   

Abstract

UNLABELLED: KIBRA has been described as a key regulator of the Hippo signaling pathway, regulating organ size control, cell contact inhibition, cell growth, as well as tumorigenesis and cystogenesis. Since there is scarce information on KIBRA gene expression regulation, we analyzed the molecular basis of tissue-specific KIBRA expression in human kidney epithelial (IHKE, HPCT) and neuroblastoma (SH-SY5Y, SK-SN-SH) cells. We detected four novel and differentially used transcription start sites, two of which positioned in the first intron, generating two novel alternative exons. We identified one constitutively active core promoter (P1a) and three alternative promoters (P1b, P2, and P3), which were exclusively active in kidney cells. Transcription factor 7-like 2 (TCF7L2) selectively activated KIBRA at P1a, P2, and P3 in kidney cells. The two genetic variants -580C>T (p < 0.05) and -1691C>T (p < 0.01) significantly affected the transcriptional activity of the KIBRA core promoter. We propose a novel functional structure of the KIBRA gene and provide detailed insight into molecular cell type-specific KIBRA transcriptional regulation by TCF7L2, the Yes-associated protein 1 and TEA domain family member. Our findings provide a potential basis for future studies on malfunctioning KIBRA regulation in pathophysiological conditions such as cancer development. KEY MESSAGE: KIBRA expression is regulated by three independent, cell type-specific promoters Two novel TSS were located within intron one resulting in two alternative exons TSS utilization is cell type-specific TCF7L2, YAP1, and TEAD are involved in the differential KIBRA expression regulation.

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Year:  2013        PMID: 24072042     DOI: 10.1007/s00109-013-1089-y

Source DB:  PubMed          Journal:  J Mol Med (Berl)        ISSN: 0946-2716            Impact factor:   4.599


  62 in total

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2.  Characterization of KIBRA, a novel WW domain-containing protein.

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Journal:  Biochem Biophys Res Commun       Date:  2003-01-24       Impact factor: 3.575

Review 3.  The Hippo pathway regulates stem cell proliferation, self-renewal, and differentiation.

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Journal:  Protein Cell       Date:  2012-05-02       Impact factor: 14.870

4.  Association of common KIBRA variants with episodic memory and AD risk.

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Journal:  Neurobiol Aging       Date:  2010-12-24       Impact factor: 4.673

5.  KIBRA exhibits MST-independent functional regulation of the Hippo signaling pathway in mammals.

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Journal:  Oncogene       Date:  2012-05-21       Impact factor: 9.867

6.  KIBRA modulates directional migration of podocytes.

Authors:  Kerstin Duning; Eva-Maria Schurek; Marc Schlüter; Michael Bayer; Hans-Christian Reinhardt; Albrecht Schwab; Liliana Schaefer; Thomas Benzing; Bernhard Schermer; Moin A Saleem; Tobias B Huber; Sebastian Bachmann; Joachim Kremerskothen; Thomas Weide; Hermann Pavenstädt
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7.  beta-catenin regulates the expression of the matrix metalloproteinase-7 in human colorectal cancer.

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8.  Identification of c-MYC as a target of the APC pathway.

Authors:  T C He; A B Sparks; C Rago; H Hermeking; L Zawel; L T da Costa; P J Morin; B Vogelstein; K W Kinzler
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9.  KIBRA: A New Gateway to Learning and Memory?

Authors:  Armin Schneider; Matthew J Huentelman; Joachim Kremerskothen; Kerstin Duning; Robert Spoelgen; Karoly Nikolich
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10.  KIBRA genetic polymorphism influences episodic memory in later life, but does not increase the risk of mild cognitive impairment.

Authors:  O P Almeida; S G Schwab; N T Lautenschlager; B Morar; K R Greenop; L Flicker; D Wildenauer
Journal:  J Cell Mol Med       Date:  2008-01-11       Impact factor: 5.310

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  7 in total

1.  KIBRA: In the brain and beyond.

Authors:  Lin Zhang; Shuping Yang; Dirk Oliver Wennmann; Yuanhong Chen; Joachim Kremerskothen; Jixin Dong
Journal:  Cell Signal       Date:  2014-03-15       Impact factor: 4.315

Review 2.  The Regulatory Role of KIBRA and PTPN14 in Hippo Signaling and Beyond.

Authors:  Kayla E Wilson; Nuo Yang; Ashley L Mussell; Jianmin Zhang
Journal:  Genes (Basel)       Date:  2016-05-27       Impact factor: 4.096

3.  ZFP226 is a novel artificial transcription factor for selective activation of tumor suppressor KIBRA.

Authors:  Katrin Schelleckes; Boris Schmitz; Malte Lenders; Mirja Mewes; Stefan-Martin Brand; Eva Brand
Journal:  Sci Rep       Date:  2018-03-09       Impact factor: 4.379

Review 4.  Alternative Splicing in the Hippo Pathway-Implications for Disease and Potential Therapeutic Targets.

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Journal:  Genes (Basel)       Date:  2018-03-13       Impact factor: 4.096

5.  Promoter methylation inhibits expression of tumor suppressor KIBRA in human clear cell renal cell carcinoma.

Authors:  Katrin Schelleckes; Boris Schmitz; Giuliano Ciarimboli; Malte Lenders; Hermann J Pavenstädt; Edwin Herrmann; Stefan-Martin Brand; Eva Brand
Journal:  Clin Epigenetics       Date:  2017-10-06       Impact factor: 6.551

6.  A 5-Methylcytosine Site of Growth Differentiation Factor 9 (GDF9) Gene Affects Its Tissue-Specific Expression in Sheep.

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Journal:  Animals (Basel)       Date:  2018-11-07       Impact factor: 2.752

Review 7.  Analysis of the role of the Hippo pathway in cancer.

Authors:  Yanyan Han
Journal:  J Transl Med       Date:  2019-04-08       Impact factor: 5.531

  7 in total

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