نتایج جستجو برای: tumor suppressor protein p53

تعداد نتایج: 1594311  

2011
Yuhui Jiang Xiaoduo Xie Zhigang Li Zheng Wang Yixuan Zhang Zhiqiang Ling Yi Pan Zhenzhen Wang Yan Chen

Raf kinase trapping to Golgi (RKTG) is a potential tumor suppressor gene due to its negative roles in regulating Ras/Raf/MEK/ERK (extracellular signal–regulated kinase) pathway and GPCR (G protein–coupled receptor) Gbg subunit signaling. Interestingly, RKTG-deficient mice are free of tumors, although they are prone to form skin cancer on carcinogen administration. On the other hand, p53 is a we...

Journal: :Proceedings of the National Academy of Sciences of the United States of America 2000
R Lev Bar-Or R Maya L A Segel U Alon A J Levine M Oren

The intracellular activity of the p53 tumor suppressor protein is regulated through a feedback loop involving its transcriptional target, mdm2. We present a simple mathematical model suggesting that, under certain circumstances, oscillations in p53 and Mdm2 protein levels can emerge in response to a stress signal. A delay in p53-dependent induction of Mdm2 is predicted to be required, albeit no...

2017
Sanam Sane Khosrow Rezvani

The ubiquitination pathway and proteasomal degradation machinery dominantly regulate p53 tumor suppressor protein stability, localization, and functions in both normal and cancerous cells. Selective E3 ubiquitin ligases dominantly regulate protein levels and activities of p53 in a large range of physiological conditions and in response to cellular changes induced by exogenous and endogenous str...

Journal: :Proceedings of the National Academy of Sciences of the United States of America 2002
Paraskevi Giannakakou Michel Nakano Kyriacos C Nicolaou Aurora O'Brate Jian Yu Mikhail V Blagosklonny Urs F Greber Tito Fojo

The tumor suppressor protein p53 localizes to microtubules (MT) and, in response to DNA damage, is transported to the nucleus via the MT minus-end-directed motor protein dynein. Dynein is also responsible for MT-mediated nuclear targeting of adenovirus type 2 (Ad2). Here we show that treatment with low concentrations of MT-targeting compounds (MTCs) that do not disrupt the MT network but are kn...

Journal: :The Journal of clinical investigation 1998
E Conseiller L Debussche D Landais C Venot M Maratrat V Sierra B Tocque L Bracco

The clinical potential of the p53 tumor suppressor gene is being evaluated currently for gene therapy of cancer. We have built a variant of wild-type p53, chimeric tumor suppressor 1 (CTS1), in which we have replaced the domains that mediate its inactivation. CTS1 presents some very interesting properties: (a) enhanced transcriptional activity; (b) resistance to the inactivation by oncogenic fo...

2012
Cheol-Hee Yoon Seung Bae Rho Seong-Tae Kim Seongho Kho Junsoo Park Ik-Soon Jang Seonock Woo Sung Soon Kim Je-Ho Lee Seung-Hoon Lee

The p53 tumor suppressor function can be compromised in many tumors by the cellular antagonist HDM2 and human papillomavirus oncogene E6 that induce p53 degradation. Restoration of p53 activity has strong therapeutic potential. Here, we identified TSC-22 as a novel p53-interacting protein and show its novel function as a positive regulator of p53. We found that TSC-22 level was significantly do...

Journal: :Cancer research 2011
Yuhui Jiang Xiaoduo Xie Zhigang Li Zheng Wang Yixuan Zhang Zhi-Qiang Ling Yi Pan Zhenzhen Wang Yan Chen

Raf kinase trapping to Golgi (RKTG) is a potential tumor suppressor gene due to its negative roles in regulating Ras/Raf/MEK/ERK (extracellular signal-regulated kinase) pathway and GPCR (G protein-coupled receptor) Gβγ subunit signaling. Interestingly, RKTG-deficient mice are free of tumors, although they are prone to form skin cancer on carcinogen administration. On the other hand, p53 is a we...

M.A Damghani M.R Bazrafshani T,R Mirshekari

Background &Aims: Laryngeal cancer is the second common cancer of respiratory tract, following the lung cancer. Carcinogenesis is a complex multistage process; molecular genetics has provided the evidence that activation of proto-oncogene and loss or inactivation of tumor suppressor genes (TSG) are involved in a large number of malignancies. One of the earliest significant tumor suppressor gene...

Journal: :Chinese Physics 2023

<sec>P53 is well recognized to be a tumor suppressor protein. In response the external stress or environmental perturbation, p53 can promote transcription of various target genes downstream, thus regulating cell cycle, apoptosis, DNA repair, and angiogenesis. However, activation further activated by another protein, MDM2, which negatively regulates level inverse reduces p53. This phenomen...

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