Literature DB >> 20165689

Targeting p53 for Novel Anticancer Therapy.

Zhen Wang1, Yi Sun.   

Abstract

Carcinogenesis is a multistage process, involving oncogene activation and tumor suppressor gene inactivation as well as complex interactions between tumor and host tissues, leading ultimately to an aggressive metastatic phenotype. Among many genetic lesions, mutational inactivation of p53 tumor suppressor, the "guardian of the genome," is the most frequent event found in 50% of human cancers. p53 plays a critical role in tumor suppression mainly by inducing growth arrest, apoptosis, and senescence, as well as by blocking angiogenesis. In addition, p53 generally confers the cancer cell sensitivity to chemoradiation. Thus, p53 becomes the most appealing target for mechanism-driven anticancer drug discovery. This review will focus on the approaches currently undertaken to target p53 and its regulators with an overall goal either to activate p53 in cancer cells for killing or to inactivate p53 temporarily in normal cells for chemoradiation protection. The compounds that activate wild type (wt) p53 would have an application for the treatment of wt p53-containing human cancer. Likewise, the compounds that change p53 conformation from mutant to wt p53 (p53 reactivation) or that kill the cancer cells with mutant p53 using a synthetic lethal mechanism can be used to selectively treat human cancer harboring a mutant p53. The inhibitors of wt p53 can be used on a temporary basis to reduce the normal cell toxicity derived from p53 activation. Thus, successful development of these three classes of p53 modulators, to be used alone or in combination with chemoradiation, will revolutionize current anticancer therapies and benefit cancer patients.

Entities:  

Year:  2010        PMID: 20165689      PMCID: PMC2822448          DOI: 10.1593/tlo.09250

Source DB:  PubMed          Journal:  Transl Oncol        ISSN: 1936-5233            Impact factor:   4.243


  183 in total

1.  T antigen is bound to a host protein in SV40-transformed cells.

Authors:  D P Lane; L V Crawford
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2.  NMR indicates that the small molecule RITA does not block p53-MDM2 binding in vitro.

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Journal:  Nat Med       Date:  2005-11       Impact factor: 53.440

3.  Benzodiazepinedione inhibitors of the Hdm2:p53 complex suppress human tumor cell proliferation in vitro and sensitize tumors to doxorubicin in vivo.

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Journal:  Mol Cancer Ther       Date:  2006-01       Impact factor: 6.261

Review 4.  Therapeutic prospects for p73 and p63: rising from the shadow of p53.

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Review 6.  Functions of the MDM2 oncoprotein.

Authors:  D A Freedman; L Wu; A J Levine
Journal:  Cell Mol Life Sci       Date:  1999-01       Impact factor: 9.261

7.  p53 status and the efficacy of cancer therapy in vivo.

Authors:  S W Lowe; S Bodis; A McClatchey; L Remington; H E Ruley; D E Fisher; D E Housman; T Jacks
Journal:  Science       Date:  1994-11-04       Impact factor: 47.728

8.  p53: The Janus of autophagy?

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Journal:  Nat Cell Biol       Date:  2008-06       Impact factor: 28.824

Review 9.  Dangerous habits of a security guard: the two faces of p53 as a drug target.

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Journal:  Hum Mol Genet       Date:  2007-04-15       Impact factor: 6.150

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  86 in total

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Journal:  Proc Natl Acad Sci U S A       Date:  2011-11-07       Impact factor: 11.205

2.  New Phage Display-Isolated Heptapeptide Recognizing the Regulatory Carboxy-Terminal Domain of Human Tumour Protein p53.

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Journal:  Bioorg Med Chem Lett       Date:  2017-05-27       Impact factor: 2.823

4.  Cancer Cells Employ Nuclear Caspase-8 to Overcome the p53-Dependent G2/M Checkpoint through Cleavage of USP28.

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Journal:  Mol Cell       Date:  2020-01-22       Impact factor: 17.970

5.  Demonstration of Tightly Radiation-Controlled Molecular Switch Based on CArG Repeats by In Vivo Molecular Imaging.

Authors:  Ya-Ju Hsieh; Luen Hwu; Chien-Chih Ke; Ai-Lin Huang; Fu-Du Chen; Shyh-Jong Wu; Sharon Chia-Ju Chen; Yong-Hua Zhao; Ren-Shyan Liu
Journal:  Mol Imaging Biol       Date:  2015-12       Impact factor: 3.488

Review 6.  Targeted polymeric nanoparticles for cancer gene therapy.

Authors:  Jayoung Kim; David R Wilson; Camila G Zamboni; Jordan J Green
Journal:  J Drug Target       Date:  2015-06-10       Impact factor: 5.121

7.  High Expression of PhospholipaseD2 Induced by Hypoxia Promotes Proliferation of Colon Cancer Cells through Activating NF- κ Bp65 Signaling Pathway.

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Journal:  Pathol Oncol Res       Date:  2018-08-08       Impact factor: 3.201

8.  Discovery and preclinical evaluation of 7-benzyl-N-(substituted)-pyrrolo[3,2-d]pyrimidin-4-amines as single agents with microtubule targeting effects along with triple-acting angiokinase inhibition as antitumor agents.

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Journal:  Bioorg Med Chem       Date:  2016-11-15       Impact factor: 3.641

9.  Epidermal FABP Prevents Chemical-Induced Skin Tumorigenesis by Regulation of TPA-Induced IFN/p53/SOX2 Pathway in Keratinocytes.

Authors:  Yuwen Zhang; Jiaqing Hao; Jun Zeng; Qiang Li; Enyu Rao; Yanwen Sun; Lianliang Liu; Anita Mandal; V Douglas Landers; Rebecca J Morris; Margot P Cleary; Jill Suttles; Bing Li
Journal:  J Invest Dermatol       Date:  2018-03-17       Impact factor: 8.551

10.  A Chinese Decoction, Kuan-Sin-Yin, Improves Autonomic Function and Cancer-Related Symptoms of Metastatic Colon Cancer.

Authors:  Tsai-Ju Chien; Chia-Yu Liu; Pin-Hao Ko; Chung-Hua Hsu
Journal:  Integr Cancer Ther       Date:  2015-11-25       Impact factor: 3.279

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