نتایج جستجو برای: smad 3

تعداد نتایج: 1814691  

Journal: :The Journal of clinical investigation 2013
Ichiaki Ito Tsuyoshi Waku Masato Aoki Rumi Abe Yu Nagai Tatsuya Watanabe Yuka Nakajima Ichiro Ohkido Keitaro Yokoyama Hiroyuki Miyachi Toshiyuki Shimizu Akiko Murayama Hiroyuki Kishimoto Kazuo Nagasawa Junn Yanagisawa

The TGF-β superfamily comprises pleiotropic cytokines that regulate SMAD and non-SMAD signaling. TGF-β-SMAD signal transduction is known to be involved in tissue fibrosis, including renal fibrosis. Here, we found that 1,25-dihydroxyvitamin D3-bound [1,25(OH)2D3-bound] vitamin D receptor (VDR) specifically inhibits TGF-β-SMAD signal transduction through direct interaction with SMAD3. In mouse mo...

Journal: :Cell 2006
Wei He David C. Dorn Hediye Erdjument-Bromage Paul Tempst Malcolm A.S. Moore Joan Massagué

Tissue homeostasis in mammals relies on powerful cytostatic and differentiation signals delivered by the cytokine TGFb and relayed within the cell via the activation of Smad transcription factors. Formation of transcription regulatory complexes by the association of Smad4 with receptor-phosphorylated Smads 2 and 3 is a central event in the canonical TGFb pathway. Here we provide evidence for a ...

Journal: :Biochemical and biophysical research communications 2008
Bei Wang Hiroyuki Suzuki Mitsuyasu Kato

TGF-beta activates receptor-regulated Smad (R-Smad) through phosphorylation by type I receptors. Activated R-Smad binds to Smad4 and the complex translocates into the nucleus and stimulates the transcription of target genes through association with co-activators including p300. It is not clear, however, how activated Smad complexes are removed from target genes. In this study, we show that TGF-...

Journal: :Journal of the Royal Society, Interface 2015
Tian Hong Ernest S Fung Lei Zhang Grace Huynh Edwin S Monuki Qing Nie

Temporal dynamics of morphogen-driven signalling events are critical for proper embryonic development. During development, cells translate extracellular bone morphogenetic protein (BMP) gradients, often subject to noise, into graded intracellular tail-phosphorylated SMAD (TP-SMAD) levels. Using modelling and experimental approaches, we found that BMPs induce TP-SMAD responses in neural precurso...

2017
Karin Walldén Tomas Nyman B. Martin Hällberg

TGF-β signaling regulates cellular processes such as proliferation, differentiation and apoptosis through activation of SMAD transcription factors that are in turn modulated by members of the Ski-SnoN family. In this process, Ski has been shown to negatively modulate TGF-β signaling by disrupting active R-SMAD/Co-SMAD heteromers. Here, we show that the related regulator SnoN forms a stable comp...

2017
Seiyu Sugiyama Kenji Yamamoto Tetsuya Matsuda Seiyu Imoto Kenji Sugiyama Tetsuya Yamamoto Tadashi Matsuda

Bone morphogenetic proteins (BMPs) play central roles in differentiation, development, and physiologic tissue remodeling. Recently, we have demonstrated that a protein inhibitor of activated STAT, PIASy suppresses TGF-b signaling by interacting with Sma and MADrelated protein 3 (Smad3). In this study, we examined a PIASy dependent inhibitory effect on BMP signaling. PIASy expression was induced...

Journal: :American journal of physiology. Endocrinology and metabolism 2007
Laura L Burger Daniel J Haisenleder Gordon M Wotton Kevin W Aylor Alan C Dalkin John C Marshall

Recent reports suggest that androgens increase FSHbeta transcription directly via the androgen receptor and by modulating activin signaling. Estrogens may also regulate FSHbeta transcription in part through the activin system. Activin signaling can be regulated extracellularly via activin, inhibin, or follistatin (FS) or intracellularly via the Smad proteins. We determined the effects of androg...

Journal: :The Journal of biological chemistry 2001
J W Wu R Fairman J Penry Y Shi

Smad proteins mediate transforming growth factor beta signaling from the cell membrane to the nucleus. Upon phosphorylation by the activated receptor kinases, the receptor-regulated Smad, such as Smad2, forms a heterocomplex with the co-mediator Smad, Smad4. This heterocomplex is then translocated into the nucleus, where it associates with other transcription factors and regulates expression of...

2016
Maria Gomes Fernandes Ruben Dries Matthias S. Roost Stefan Semrau Ana de Melo Bernardo Richard P. Davis Ramprasad Ramakrishnan Karoly Szuhai Elke Maas Lieve Umans Vanesa Abon Escalona Daniela Salvatori Dieter Deforce Wim Van Criekinge Danny Huylebroeck Christine Mummery An Zwijsen Susana M. Chuva de Sousa Lopes

Naive mouse embryonic stem cells (mESCs) are in a metastable state and fluctuate between inner cell mass- and epiblast-like phenotypes. Here, we show transient activation of the BMP-SMAD signaling pathway in mESCs containing a BMP-SMAD responsive reporter transgene. Activation of the BMP-SMAD reporter transgene in naive mESCs correlated with lower levels of genomic DNA methylation, high express...

Journal: :Development 2005
Norma T Takaesu Eric Herbig David Zhitomersky Michael B O'Connor Stuart J Newfeld

Mutations in SMAD tumor suppressor genes are involved in approximately 140,000 new cancers in the USA each year. At this time, how the absence of a functional SMAD protein leads to a tumor is unknown. However, clinical and biochemical studies suggest that all SMAD mutations are loss-of-function mutations. One prediction of this hypothesis is that all SMAD mutations cause tumors via a single mec...

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