نتایج جستجو برای: tumor suppressor protein p53

تعداد نتایج: 1594311  

Journal: :Molecular cancer research : MCR 2017
Kyrie Pappas Jia Xu Sakellarios Zairis Lois Resnick-Silverman Francesco Abate Nicole Steinbach Sait Ozturk Lao H Saal Tao Su Pamela Cheung Hank Schmidt Stuart Aaronson Hanina Hibshoosh James Manfredi Raul Rabadan Ramon Parsons

TP53 is the most commonly mutated tumor suppressor gene and its mutation drives tumorigenesis. Using ChIP-seq for p53 in the absence of acute cell stress, we found that wild-type but not mutant p53 binds and activates numerous tumor suppressor genes, including PTEN, STK11(LKB1), miR-34a, KDM6A(UTX), FOXO1, PHLDA3, and TNFRSF10B through consensus binding sites in enhancers and promoters. Depleti...

Journal: :The Journal of biological chemistry 2008
Hongjie Yao Pingxin Li Bryan J Venters Suting Zheng Paul R Thompson B Franklin Pugh Yanming Wang

Protein Arg methyltransferases function as coactivators of the tumor suppressor p53 to regulate gene expression. Peptidylarginine deiminase 4 (PAD4/PADI4) counteracts the functions of protein Arg methyltransferases in gene regulation by deimination and demethylimination. Here we show that the expression of a tumor suppressor gene, OKL38, is activated by the inhibition of PAD4 or the activation ...

Journal: :Cell 2003
Michelangelo Cordenonsi Sirio Dupont Silvia Maretto Alessandra Insinga Carol Imbriano Stefano Piccolo

The p53 tumor suppressor belongs to a family of proteins that sense multiple cellular inputs to regulate cell proliferation, apoptosis, and differentiation. Whether and how these functions of p53 intersect with the activity of extracellular growth factors is not understood. Here, we report that key cellular responses to TGF-beta signals rely on p53 family members. During Xenopus embryonic devel...

2015
Dawid Walerych Kamil Lisek Giannino Del Sal

Encoded by the mutated variants of the TP53 tumor suppressor gene, mutant p53 proteins are getting an increased experimental support as active oncoproteins promoting tumor growth and metastasis. p53 missense mutant proteins are losing their wild-type tumor suppressor activity and acquire oncogenic potential, possessing diverse transforming abilities in cell and mouse models. Whether various mut...

Journal: :Methods in molecular biology 2003
Timothy K MacLachlan Wafik S El-Deiry

PART I. UNDERSTANDING THE FUNCTION AND REGULATION OF TUMOR SUPPRESSOR GENES 1 Utilizing NMR to Study the Structure of Growth-Inhibitory Proteins Francesca M. Marassi ........................................................................................ 3 2 Generation and Application of Phospho-Specific Antibodies for p53 and pRB Yoichi Taya, Kiichiro Nakajima, Kumiko Yoshizawa-Kumagaye, and K...

2016
Jiangbo Liu Wei Li Miao Deng Dechun Liu Qingyong Ma Xiaoshan Feng

BACKGROUND Whether increased expression of the tumor suppressor protein p53 indicates a p53 gene mutation in hepatocellular carcinoma (HCC) remains unclear. We conducted a meta-analysis to determine whether p53 protein overexpression detected by immunohistochemistry (IHC) offers a diagnostic prediction for p53 gene mutations in HCC patients. METHODS Systematic literature searches were conduct...

Journal: :Diabetologie Und Stoffwechsel 2023

Background Beta cell dysfunction and death are critical steps in the development of both type 1 2 diabetes (T1D T2D), but underlying mechanisms incompletely understood. Activation essential tumor suppressor transcription factor P53 was linked to beta vitro has been reported several mouse models cells humans with T2D. Therefore, we investigated specific role dysfunction, vivo.

Journal: :Cell growth & differentiation : the molecular biology journal of the American Association for Cancer Research 1999
M H Kubbutat R L Ludwig A J Levine K H Vousden

Degradation of the p53 tumor suppressor protein has been shown to be regulated by Mdm2. In this study, we identify regions of Mdm2 that are not required for p53 binding but are essential for degradation. Mdm2 mutants lacking these regions function in a dominant negative fashion, stabilizing endogenous p53 in cells by interfering with the degradative function of the endogenous Mdm2. p53 protein ...

Journal: :The Journal of clinical investigation 2011
Wenyi Wei William G Kaelin

The evolutionarily conserved protein COP1 has been shown to operate as an E3 ubiquitin ligase complex, and a number of putative substrates have been identified, including the c-JUN oncoprotein and p53 tumor suppressor protein. New work by Migliorini and colleagues described in the current issue of JCI demonstrates that COP1 acts as a tumor suppressor in vivo and does so, at least in part, by pr...

Journal: :Journal of Cancer Prevention & Current Research 2015

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