论文信息 - miR-629 Targets TRIM33 to Promote TGFβ/Smad Signaling and Metastatic Phenotypes in ccRCC - 字舞流文

miR-629 Targets TRIM33 to Promote TGFβ/Smad Signaling and Metastatic Phenotypes in ccRCC

Renal cell carcinoma (RCC) is the most common neoplasm of the adult kidney, and clear cell RCC (ccRCC) represents its most common histological subtype. To identify a therapeutic target for ccRCC, miRNA expression signatures from ccRCC clinical specimens were analyzed. miRNA microarray and real-time PCR analyses revealed that miR-629 expression was significantly upregulated in human ccRCC compared with adjacent noncancerous renal tissue. Functional inhibition of miR-629 by a hairpin miRNA inhibitor suppressed ccRCC cell motility and invasion. Mechanistically, miR-629 directly targeted tripartite motif-containing 33 (TRIM33), which inhibits the TGFβ/Smad signaling pathway. In clinical ccRCC specimens, downregulation of TRIM33 was observed with the association of both pathologic stages and grades. The miR-629 inhibitor significantly suppressed TGFβ-induced Smad activation by upregulating TRIM33 expression and subsequently inhibited the association of Smad2/3 and Smad4. Moreover, a miR-629 mimic enhanced the effect of TGFβ on the expression of epithelial–mesenchymal transition–related factors as well as on the motility and invasion in ccRCC cells. These findings identify miR-629 as a potent regulator of the TGFβ/Smad signaling pathway via TRIM33 in ccRCC. Implications: This study suggests that miR-629 has biomarker potential through its ability to regulate TGFβ/Smad signaling and accelerate ccRCC cell motility and invasion. Mol Cancer Res; 13(3); 565–74. ©2014 AACR.

Hiroshi Egawa | Kazutoshi Fujita | Yuko Ueda | K. Tsujikawa | N. Nonomura | K. Fujita | M. Uemura | H. Egawa | Kentaro Jingushi | Yuko Ueda | K. Kitae | W. Nakata | Norio Nonomura | Kentaro Jingushi | Yuri Kashiwagi | Kaori Kitae | Hiroaki Hase | Wataru Nakata | Motohide Uemura | Kazutake Tsujikawa | Ikumi Ohshio | Ryoji Kawakami | Yohei Tsukada | Takumi Kobayashi | Takumi Kobayashi | H. Hase | I. Ohshio | Ryoji Kawakami | Yuri Kashiwagi | Yohei Tsukada | K. Fujita

[1] A. Czarnecka,et al. Resistance to tyrosine kinase inhibitors in clear cell renal cell carcinoma: from the patient's bed to molecular mechanisms. , 2014, Biochimica et biophysica acta.

[2] W. Schiemann,et al. Transforming growth factor-β and the hallmarks of cancer. , 2011, Cellular signalling.

[3] M. Nakao,et al. Loss of expression of type IV collagen alpha5 and alpha6 chains in colorectal cancer associated with the hypermethylation of their promoter region. , 2006, The American journal of pathology.

[4] Samy Lamouille,et al. TGF-&bgr; signaling and epithelial–mesenchymal transition in cancer progression , 2013, Current opinion in oncology.

[5] N. Gerry,et al. Previously unidentified changes in renal cell carcinoma gene expression identified by parametric analysis of microarray data , 2003, BMC Cancer.

[6] G. Ryffel,et al. Human renal cell carcinogenesis is accompanied by a coordinate loss of the tissue specific transcription factors HNF4α and HNF1α , 1996 .

[7] K. Alitalo,et al. Loss of Neural Cell Adhesion Molecule Induces Tumor Metastasis by Up-regulating Lymphangiogenesis , 2004, Cancer Research.

[8] L. Hunyady,et al. Crosstalk between TGF-β signaling and the microRNA machinery. , 2012, Trends in pharmacological sciences.

[9] The Cancer Genome Atlas Research Network. COMPREHENSIVE MOLECULAR CHARACTERIZATION OF CLEAR CELL RENAL CELL CARCINOMA , 2013, Nature.

[10] D. Lindgren,et al. Effects of TGF-β signaling in clear cell renal cell carcinoma cells. , 2013, Biochemical and biophysical research communications.

[11] M. Doucet,et al. TGF‐β Promotes the Establishment of Renal Cell Carcinoma Bone Metastasis , 2006 .

[12] M. Rugge,et al. Germ-Layer Specification and Control of Cell Growth by Ectodermin, a Smad4 Ubiquitin Ligase , 2005, Cell.

[13] P. Chambon,et al. TIF1γ, a novel member of the transcriptional intermediary factor 1 family , 1999, Oncogene.

[14] R. Losson,et al. Transcription cofactors TRIM24, TRIM28, and TRIM33 associate to form regulatory complexes that suppress murine hepatocellular carcinoma , 2011, Proceedings of the National Academy of Sciences.

[15] Kai-ping Yan,et al. Transcription intermediary factor 1γ is a tumor suppressor in mouse and human chronic myelomonocytic leukemia. , 2011, The Journal of clinical investigation.

[16] Kevin Struhl,et al. An HNF4α-miRNA Inflammatory Feedback Circuit Regulates Hepatocellular Oncogenesis , 2011, Cell.

[17] P. A. Futreal,et al. State of the Science: An Update on Renal Cell Carcinoma , 2012, Molecular Cancer Research.

[18] Steven J. M. Jones,et al. Comprehensive molecular characterization of clear cell renal cell carcinoma , 2013, Nature.

[19] S. Dupont,et al. Recruitment of TIF1γ to chromatin via its PHD finger-bromodomain activates its ubiquitin ligase and transcriptional repressor activities. , 2011, Molecular cell.

[20] M. Nakao,et al. Loss of expression of type IV collagen α5 and α6 chains in colorectal cancer associated with the hypermethylation of their promoter region , 2006 .

[21] L. Zon,et al. TIF1γ Controls Erythroid Cell Fate by Regulating Transcription Elongation , 2010, Cell.

[22] Daniel B. Martin,et al. Circulating microRNAs as stable blood-based markers for cancer detection , 2008, Proceedings of the National Academy of Sciences.

[23] Stefan Holdenrieder,et al. MicroRNAs in Renal Cell Carcinoma: Diagnostic Implications of Serum miR-1233 Levels , 2011, PloS one.

[24] Marta Di Nicola,et al. microRNAs Derived from Circulating Exosomes as Noninvasive Biomarkers for Screening and Diagnosing Lung Cancer , 2013, Journal of thoracic oncology : official publication of the International Association for the Study of Lung Cancer.

[25] Leonardo Morsut,et al. FAM/USP9x, a Deubiquitinating Enzyme Essential for TGFβ Signaling, Controls Smad4 Monoubiquitination , 2009, Cell.

[26] A. Freywald,et al. The EphB6 receptor cooperates with c-Cbl to regulate the behavior of breast cancer cells. , 2010, Cancer research.

[27] I. Anastasiou,et al. Expression of transforming growth factor β in renal cell carcinoma and matched non-involved renal tissue , 2004, Urological Research.

[28] M. Lerman,et al. Mesenchymal‐epithelial transition in the developing metanephric kidney: Gene expression study by differential display , 2000, Genesis.

[29] H. Sugimura,et al. Loss of Expression of EphB1 Protein in Gastric Carcinoma Associated with Invasion and Metastasis , 2008, Oncology.

[30] Y. Hata,et al. The RASSF6 Tumor Suppressor Protein Regulates Apoptosis and the Cell Cycle via MDM2 Protein and p53 Protein* , 2013, The Journal of Biological Chemistry.

[31] M. Walker,et al. Repression of Androgen Receptor Activity by HEYL, a Third Member of the Hairy/Enhancer-of-split-related Family of Notch Effectors* , 2011, The Journal of Biological Chemistry.

[32] Samy Lamouille,et al. TGF-β-induced epithelial to mesenchymal transition , 2009, Cell Research.

[33] Wei He,et al. Hematopoiesis Controlled by Distinct TIF1γ and Smad4 Branches of the TGFβ Pathway , 2006, Cell.

[34] Thomas Schaffner,et al. Calpain-mediated cleavage of Atg5 switches autophagy to apoptosis , 2006, Nature Cell Biology.