论文信息 - The role of p53 in cancer drug resistance and targeted chemotherapy

The role of p53 in cancer drug resistance and targeted chemotherapy

Cancer has long been a grievous disease complicated by innumerable players aggravating its cure. Many clinical studies demonstrated the prognostic relevance of the tumor suppressor protein p53 for many human tumor types. Overexpression of mutated p53 with reduced or abolished function is often connected to resistance to standard medications, including cisplatin, alkylating agents (temozolomide), anthracyclines, (doxorubicin), antimetabolites (gemcitabine), antiestrogenes (tamoxifen) and EGFR-inhibitors (cetuximab). Such mutations in the TP53 gene are often accompanied by changes in the conformation of the p53 protein. Small molecules that restore the wild-type conformation of p53 and, consequently, rebuild its proper function have been identified. These promising agents include PRIMA-1, MIRA-1, and several derivatives of the thiosemicarbazone family. In addition to mutations in p53 itself, p53 activity may be also be impaired due to alterations in p53s regulating proteins such as MDM2. MDM2 functions as primary cellular p53 inhibitor and deregulation of the MDM2/p53-balance has serious consequences. MDM2 alterations often result in its overexpression and therefore promote inhibition of p53 activity. To deal with this problem, a judicious approach is to employ MDM2 inhibitors. Several promising MDM2 inhibitors have been described such as nutlins, benzodiazepinediones or spiro-oxindoles as well as novel compound classes such as xanthone derivatives and trisubstituted aminothiophenes. Furthermore, even naturally derived inhibitor compounds such as a-mangostin, gambogic acid and siladenoserinols have been discovered. In this review, we discuss in detail such small molecules that play a pertinent role in affecting the p53-MDM2 signaling axis and analyze their potential as cancer chemotherapeutics.

[1] J. Piette,et al. Mdm2: keeping p53 under control , 1997, Oncogene.

[2] David Lane,et al. p53 Research: the past thirty years and the next thirty years. , 2010, Cold Spring Harbor perspectives in biology.

[3] Maxwell D Cummings,et al. Substituted 1,4‐Benzodiazepine‐2,5‐diones as α‐Helix Mimetic Antagonists of the HDM2‐p53 Protein–Protein Interaction , 2006, Chemical biology & drug design.

[4] Galina Selivanova,et al. Restoration of the tumor suppressor function to mutant p53 by a low-molecular-weight compound , 2002, Nature Medicine.

[5] Weisi Wang,et al. Design, synthesis and biological evaluation of novel 3,4,5-trisubstituted aminothiophenes as inhibitors of p53-MDM2 interaction. Part 1. , 2013, Bioorganic & medicinal chemistry.

[6] K. Vousden,et al. Stress Signals Utilize Multiple Pathways To Stabilize p53 , 2000, Molecular and Cellular Biology.

[7] X Chen,et al. The p53-estrogen receptor loop in cancer. , 2013, Current molecular medicine.

[8] B. Katzenellenbogen,et al. Antiestrogens: Mechanisms of action and resistance in breast cancer , 1997, Breast Cancer Research and Treatment.

[9] T. Aas,et al. Influence of TP53 gene alterations and c-erbB-2 expression on the response to treatment with doxorubicin in locally advanced breast cancer. , 2001, Cancer research.

[10] I. Arisi,et al. Targeting the MDM2/MDM4 interaction interface as a promising approach for p53 reactivation therapy. , 2015, Cancer research.

[11] Kareem Khoury,et al. P53 mdm2 inhibitors. , 2012, Current pharmaceutical design.

[12] A. Rajasekaran,et al. Estrogen receptor-alpha binds p53 tumor suppressor protein directly and represses its function. , 2006, The Journal of biological chemistry.

[13] Manuel Serrano,et al. p53: Guardian of the Genome and Policeman of the Oncogenes , 2007, Cell cycle.

[14] R. Mohammad,et al. HDM2 antagonist MI-219 (spiro-oxindole), but not Nutlin-3 (cis-imidazoline), regulates p53 through enhanced HDM2 autoubiquitination and degradation in human malignant B-cell lymphomas , 2012, Journal of Hematology & Oncology.

[15] L. Gianni,et al. Anthracyclines: Molecular Advances and Pharmacologic Developments in Antitumor Activity and Cardiotoxicity , 2004, Pharmacological Reviews.

[16] K. Wiman,et al. Mutant p53 reactivation by small molecules makes its way to the clinic , 2014, FEBS letters.

[17] C. Auffray,et al. Drug specific resistance to oxaliplatin is associated with apoptosis defect in a cellular model of colon carcinoma , 2002, FEBS letters.

[18] C. Maki,et al. Acquisition of p53 mutations in response to the non-genotoxic p53 activator Nutlin-3 , 2011, Oncogene.

[19] C. Deng. SIRT1, Is It a Tumor Promoter or Tumor Suppressor? , 2009, International journal of biological sciences.

[20] Mark R Player,et al. Small-molecule inhibitors of the p53-HDM2 interaction for the treatment of cancer. , 2008, Expert opinion on investigational drugs.

[21] V. Rotter,et al. Oncogenic mutations of the p53 tumor suppressor: the demons of the guardian of the genome. , 2000, Cancer research.

[22] J. V. van Meerbeeck,et al. The MDM2-inhibitor Nutlin-3 synergizes with cisplatin to induce p53 dependent tumor cell apoptosis in non-small cell lung cancer , 2015, Oncotarget.

[23] D. Parks,et al. Benzodiazepinedione inhibitors of the Hdm2:p53 complex suppress human tumor cell proliferation in vitro and sensitize tumors to doxorubicin in vivo , 2006, Molecular Cancer Therapeutics.

[24] Maxwell D Cummings,et al. Structure-based design, synthesis, and biological evaluation of novel 1,4-diazepines as HDM2 antagonists. , 2005, Bioorganic & medicinal chemistry letters.

[25] Galina Selivanova,et al. Therapeutic targeting of p53 by small molecules. , 2010, Seminars in cancer biology.

[26] Liu Liu,et al. A potent small-molecule inhibitor of the MDM2-p53 interaction (MI-888) achieved complete and durable tumor regression in mice. , 2013, Journal of medicinal chemistry.

[27] J Milner,et al. A structural role for metal ions in the "wild-type" conformation of the tumor suppressor protein p53. , 1993, Cancer research.

[28] Jürgen Geisler,et al. TP53 gene mutations predict the response to neoadjuvant treatment with 5-fluorouracil and mitomycin in locally advanced breast cancer. , 2003, Clinical cancer research : an official journal of the American Association for Cancer Research.

[29] C. Harris,et al. p53: 25 years after its discovery. , 2004, Trends in pharmacological sciences.

[30] G. Blandino,et al. Mutant p53 stimulates chemoresistance of pancreatic adenocarcinoma cells to gemcitabine. , 2015, Biochimica et biophysica acta.

[31] M. Saha,et al. Small molecule MIRA-1 induces in vitro and in vivo anti-myeloma activity and synergizes with current anti-myeloma agents , 2014, British Journal of Cancer.

[32] L. Vassilev,et al. In Vivo Activation of the p53 Pathway by Small-Molecule Antagonists of MDM2 , 2004, Science.

[33] O. Myklebost,et al. Small-molecule MDM2 antagonists reveal aberrant p53 signaling in cancer: implications for therapy. , 2006, Proceedings of the National Academy of Sciences of the United States of America.

[34] John Nguyen,et al. Formation of disulfide bond in p53 correlates with inhibition of DNA binding and tetramerization. , 2003, Antioxidants & redox signaling.

[35] M. Olivier,et al. Impact of mutant p53 functional properties on TP53 mutation patterns and tumor phenotype: lessons from recent developments in the IARC TP53 database , 2007, Human mutation.

[36] J. Manfredi,et al. Multiple roles of the tumor suppressor p53 , 2002, Current opinion in oncology.

[37] P. Lønning,et al. Low expression levels of ATM may substitute for CHEK2 /TP53 mutations predicting resistance towards anthracycline and mitomycin chemotherapy in breast cancer , 2012, Breast Cancer Research.

[38] D. Schuppan,et al. EGFR blockade by cetuximab alone or as combination therapy for growth control of hepatocellular cancer. , 2005, Biochemical pharmacology.

[39] Jing Zhang,et al. Discovery of RG7388, a potent and selective p53-MDM2 inhibitor in clinical development. , 2013, Journal of medicinal chemistry.

[40] Marina Konopleva,et al. Mdm2 inhibitor Nutlin-3a induces p53-mediated apoptosis by transcription-dependent and transcription-independent mechanisms and may overcome Atm-mediated resistance to fludarabine in chronic lymphocytic leukemia. , 2006, Blood.

[41] Moshe Oren,et al. The p53 and Mdm2 families in cancer. , 2002, Current opinion in genetics & development.

[42] S. Narod,et al. Triple-Negative Breast Cancer: Clinical Features and Patterns of Recurrence , 2007, Clinical Cancer Research.

[43] B. Gusterson,et al. p53 polymorphism influences response in cancer chemotherapy via modulation of p73-dependent apoptosis. , 2003, Cancer cell.

[44] S. Chaney,et al. Efficient nucleotide excision repair of cisplatin, oxaliplatin, and Bis-aceto-ammine-dichloro-cyclohexylamine-platinum(IV) (JM216) platinum intrastrand DNA diadducts. , 1999, Cancer research.

[45] J. Li,et al. Anti-tumorigenicity of dietary α-mangostin in an HT-29 colon cell xenograft model and the tissue distribution of xanthones and their phase II metabolites. , 2013, Molecular nutrition & food research.

[46] J. Perez,et al. Cisplatin biochemical mechanism of action: from cytotoxicity to induction of cell death through interconnections between apoptotic and necrotic pathways. , 2003, Current medicinal chemistry.

[47] Hui Zhao,et al. MDM2 inhibitor Nutlin-3a suppresses proliferation and promotes apoptosis in osteosarcoma cells. , 2012, Acta biochimica et biophysica Sinica.

[48] J. Marin,et al. Overview of the molecular bases of resistance to chemotherapy in liver and gastrointestinal tumours. , 2009, Current molecular medicine.

[49] E. White,et al. Nutlin-3 Protects Kidney Cells during Cisplatin Therapy by Suppressing Bax/Bak Activation* , 2007, Journal of Biological Chemistry.

[50] L. Mayo,et al. Nutlin3 blocks vascular endothelial growth factor induction by preventing the interaction between hypoxia inducible factor 1alpha and Hdm2. , 2007, Cancer research.

[51] C. Prives,et al. p53: puzzle and paradigm. , 1996, Genes & development.

[52] Gabriel Pons,et al. MDM2 antagonists activate p53 and synergize with genotoxic drugs in B-cell chronic lymphocytic leukemia cells. , 2006, Blood.

[53] Jayne M. Silver,et al. Potentiation of Carboplatin-Mediated DNA Damage by the Mdm2 Modulator Nutlin-3a in a Humanized Orthotopic Breast-to-Lung Metastatic Model , 2015, Molecular Cancer Therapeutics.

[54] T. Aas,et al. Specific P53 mutations are associated with de novo resistance to doxorubicin in breast cancer patients , 1996, Nature Medicine.

[55] E. Dmitrovsky,et al. Aberrant p53 expression predicts clinical resistance to cisplatin-based chemotherapy in locally advanced non-small cell lung cancer. , 1995, Cancer research.

[56] Jean-Yves Blay,et al. Effect of the MDM2 antagonist RG7112 on the P53 pathway in patients with MDM2-amplified, well-differentiated or dedifferentiated liposarcoma: an exploratory proof-of-mechanism study. , 2012, The Lancet. Oncology.

[57] M. Oren,et al. RITA can induce cell death in p53-defective cells independently of p53 function via activation of JNK/SAPK and p38 , 2014, Cell Death and Disease.

[58] H. Yokosawa,et al. Siladenoserinols A-L: new sulfonated serinol derivatives from a tunicate as inhibitors of p53-Hdm2 interaction. , 2013, Organic letters.

[59] M. E. Perry,et al. mdm2 Is Critical for Inhibition of p53 during Lymphopoiesis and the Response to Ionizing Irradiation , 2003, Molecular and Cellular Biology.

[60] W. Chng,et al. p53 Abnormalities and Potential Therapeutic Targeting in Multiple Myeloma , 2014, BioMed research international.

[61] K. Vousden,et al. p53 mutations in cancer , 2013, Nature Cell Biology.

[62] M. Dobbelstein,et al. Cooperation of Nutlin-3a and a Wip1 inhibitor to induce p53 activity , 2016, Oncotarget.

[63] R. Mirimanoff,et al. MGMT gene silencing and benefit from temozolomide in glioblastoma. , 2005, The New England journal of medicine.

[64] A. Fersht,et al. Structural biology of the tumor suppressor p53. , 2008, Annual review of biochemistry.

[65] Maxwell D Cummings,et al. 1,4-Benzodiazepine-2,5-diones as small molecule antagonists of the HDM2-p53 interaction: discovery and SAR. , 2005, Bioorganic & medicinal chemistry letters.

[66] D. Richardson,et al. Thiosemicarbazones from the old to new: iron chelators that are more than just ribonucleotide reductase inhibitors. , 2009, Journal of medicinal chemistry.

[67] A. Giaccia,et al. The complexity of p53 modulation: emerging patterns from divergent signals. , 1998, Genes & development.

[68] D. Lane,et al. p53, guardian of the genome , 1992, Nature.

[69] Small molecule compounds targeting the p53 pathway: are we finally making progress? , 2014, Apoptosis.

[70] R. Mirzayans,et al. New Insights into p53 Signaling and Cancer Cell Response to DNA Damage: Implications for Cancer Therapy , 2012, Journal of biomedicine & biotechnology.

[71] A. Levine. p53, the Cellular Gatekeeper for Growth and Division , 1997, Cell.

[72] K. Schulze-Osthoff,et al. Translational approaches targeting the p53 pathway for anti‐cancer therapy , 2012, British journal of pharmacology.

[73] Ying Huang,et al. Membrane transporters and channels in chemoresistance and -sensitivity of tumor cells. , 2006, Cancer letters.

[74] S. Howell,et al. DNA mismatch repair and p53 function are major determinants of the rate of development of cisplatin resistance , 2006, Molecular Cancer Therapeutics.

[75] Uri Alon,et al. Dynamics of the p53-Mdm2 feedback loop in individual cells , 2004, Nature Genetics.

[76] J. Mackey,et al. Expression of a non‐functional p53 affects the sensitivity of cancer cells to gemcitabine , 2002, International journal of cancer.

[77] Q. Ma. Role of nrf2 in oxidative stress and toxicity. , 2013, Annual review of pharmacology and toxicology.

[78] W. A. Mardin,et al. MicroRNA Profiling Implies New Markers of Gemcitabine Chemoresistance in Mutant p53 Pancreatic Ductal Adenocarcinoma , 2015, PloS one.

[79] P. Harari,et al. p53 modulates acquired resistance to EGFR inhibitors and radiation. , 2011, Cancer research.

[80] Akira Endou,et al. Effect of Y220C Mutation on p53 and Its Rescue Mechanism: A Computer Chemistry Approach , 2013, The Protein Journal.

[81] Myles Brown,et al. Molecular Determinants for the Tissue Specificity of SERMs , 2002, Science.

[82] P. Distefano,et al. Inhibition of SIRT1 Catalytic Activity Increases p53 Acetylation but Does Not Alter Cell Survival following DNA Damage , 2006, Molecular and Cellular Biology.

[83] N. Smith,et al. The p53 tumor suppressor gene and nuclear protein: basic science review and relevance in the management of bladder cancer. , 2003, The Journal of urology.

[84] S. Cravo,et al. Dihydroxyxanthones prenylated derivatives: synthesis, structure elucidation, and growth inhibitory activity on human tumor cell lines with improvement of selectivity for MCF-7. , 2007, Bioorganic & medicinal chemistry.

[85] J. Robert,et al. Determinants of the cytotoxicity of irinotecan in two human colorectal tumor cell lines , 2002, Cancer Chemotherapy and Pharmacology.

[86] A. Palmeira,et al. Discovery of a new small-molecule inhibitor of p53-MDM2 interaction using a yeast-based approach. , 2013, Biochemical pharmacology.

[87] R. Bristow,et al. Nutlin-3 radiosensitizes hypoxic prostate cancer cells independent of p53 , 2008, Molecular Cancer Therapeutics.

[88] Shanghai Yu,et al. SAR405838: an optimized inhibitor of MDM2-p53 interaction that induces complete and durable tumor regression. , 2014, Cancer research.

[89] K. Wiman,et al. Pharmacological reactivation of mutant p53: from protein structure to the cancer patient , 2010, Oncogene.

[90] Baoying Huang,et al. Elevated MDM2 boosts the apoptotic activity of p53-MDM2 binding inhibitors by facilitating MDMX degradation , 2008, Cell cycle.

[91] X. Zhao,et al. HDM2 antagonist Nutlin-3 disrupts p73-HDM2 binding and enhances p73 function , 2008, Oncogene.

[92] J. Cairncross,et al. Effect of aberrant p53 function on temozolomide sensitivity of glioma cell lines and brain tumor initiating cells from glioblastoma , 2011, Journal of Neuro-Oncology.

[93] Shengzheng Wang,et al. Structure-activity relationship and antitumor activity of thio-benzodiazepines as p53-MDM2 protein-protein interaction inhibitors. , 2012, European journal of medicinal chemistry.

[94] J N Weinstein,et al. Characterization of the p53 tumor suppressor pathway in cell lines of the National Cancer Institute anticancer drug screen and correlations with the growth-inhibitory potency of 123 anticancer agents. , 1997, Cancer research.

[95] A. Gadducci,et al. Molecular mechanisms of apoptosis and chemosensitivity to platinum and paclitaxel in ovarian cancer: biological data and clinical implications. , 2002, European journal of gynaecological oncology.

[96] J. Yoshida,et al. A combination of IFN-β and temozolomide in human glioma xenograft models: implication of p53-mediated MGMT downregulation , 2008, Cancer Chemotherapy and Pharmacology.

[97] N. Chang,et al. Tumor Suppressor WWOX and p53 Alterations and Drug Resistance in Glioblastomas , 2013, Front. Oncol..

[98] A. Levine,et al. Surfing the p53 network , 2000, Nature.

[99] X. Lin,et al. The role of DNA mismatch repair in cisplatin mutagenicity. , 1999, Journal of inorganic biochemistry.

[100] Yanhui Liu,et al. Mutant TP53 enhances the resistance of glioblastoma cells to temozolomide by up-regulating O6-methylguanine DNA-methyltransferase , 2013, Neurological Sciences.

[101] Binh Vu,et al. MDM2 small-molecule antagonist RG7112 activates p53 signaling and regresses human tumors in preclinical cancer models. , 2013, Cancer research.

[102] Y. Akao,et al. α-Mangostin extracted from the pericarp of the mangosteen (Garcinia mangostana Linn) reduces tumor growth and lymph node metastasis in an immunocompetent xenograft model of metastatic mammary cancer carrying a p53 mutation , 2011, BMC medicine.

[103] M. Stevens,et al. Temozolomide: mechanisms of action, repair and resistance. , 2012, Current molecular pharmacology.

[104] M C Willingham,et al. Cellular localization of the multidrug-resistance gene product P-glycoprotein in normal human tissues. , 1987, Proceedings of the National Academy of Sciences of the United States of America.

[105] A. Levine,et al. Structure of the MDM2 Oncoprotein Bound to the p53 Tumor Suppressor Transactivation Domain , 1996, Science.

[106] Shaomeng Wang,et al. Targeting apoptosis pathways for new cancer therapeutics. , 2014, Annual review of medicine.

[107] Wei-Guo Zhu,et al. p53: Structure, Function and Therapeutic Applications , 2006 .

[108] A. Fersht,et al. Structural basis for understanding oncogenic p53 mutations and designing rescue drugs , 2006, Proceedings of the National Academy of Sciences.

[109] A. Levine,et al. A Single Nucleotide Polymorphism in the MDM2 Promoter Attenuates the p53 Tumor Suppressor Pathway and Accelerates Tumor Formation in Humans , 2004, Cell.

[110] V. Baron,et al. Mutant p53 initiates a feedback loop that involves Egr-1/EGF receptor/ERK in prostate cancer cells , 2010, Oncogene.

[111] J. Lunec,et al. Chemical Inhibition of Wild-Type p53-Induced Phosphatase 1 (WIP1/PPM1D) by GSK2830371 Potentiates the Sensitivity to MDM2 Inhibitors in a p53-Dependent Manner , 2016, Molecular Cancer Therapeutics.

[112] Sachiko Iseki,et al. Inability of p53-reactivating compounds Nutlin-3 and RITA to overcome p53 resistance in tumor cells deficient in p53Ser46 phosphorylation. , 2012, Biochemical and biophysical research communications.

[113] P. Kleiblova,et al. Inhibition of WIP1 phosphatase sensitizes breast cancer cells to genotoxic stress and to MDM2 antagonist nutlin-3 , 2016, Oncotarget.

[114] Jan Bergman,et al. PRIMA-1 reactivates mutant p53 by covalent binding to the core domain. , 2009, Cancer cell.

[115] J. Weinstein,et al. Profiling SLCO and SLC22 genes in the NCI-60 cancer cell lines to identify drug uptake transporters , 2008, Molecular Cancer Therapeutics.

[116] J. Niland,et al. The MDM2 gene amplification database. , 1998, Nucleic acids research.

[117] Jie Zhao,et al. Inhibition of alpha(4) integrin mediated adhesion was involved in the reduction of B16-F10 melanoma cells lung colonization in C57BL/6 mice treated with gambogic acid. , 2008, European journal of pharmacology.

[118] Jie Zhao,et al. Gambogic acid mediates apoptosis as a p53 inducer through down-regulation of mdm2 in wild-type p53-expressing cancer cells , 2008, Molecular Cancer Therapeutics.

[119] Y. Xu,et al. A common gain of function of p53 cancer mutants in inducing genetic instability , 2010, Oncogene.

[120] K. Wiman,et al. Reactivation of mutant p53 and induction of apoptosis in human tumor cells by maleimide analogs. , 2017, The Journal of Biological Chemistry.

[121] M. E. Sousa,et al. Xanthone derivatives: new insights in biological activities. , 2005, Current medicinal chemistry.

[122] Kelli J. Glenn,et al. Activation of p53 by the MDM2 inhibitor RG7112 impairs thrombopoiesis. , 2014, Experimental hematology.

[123] Maxwell D Cummings,et al. Enhanced pharmacokinetic properties of 1,4-benzodiazepine-2,5-dione antagonists of the HDM2-p53 protein-protein interaction through structure-based drug design. , 2006, Bioorganic & medicinal chemistry letters.

[124] P. Jeffrey,et al. Crystal structure of a p53 tumor suppressor-DNA complex: understanding tumorigenic mutations. , 1994, Science.

[125] M. Weller,et al. O6‐methylguanine DNA methyltransferase and p53 status predict temozolomide sensitivity in human malignant glioma cells , 2006, Journal of neurochemistry.

[126] D. Hallahan,et al. Radiosensitization of lung cancer by nutlin, an inhibitor of murine double minute 2 , 2006, Molecular Cancer Therapeutics.

[127] N. Cárdenas-Rodríguez,et al. Medicinal properties of mangosteen (Garcinia mangostana). , 2008, Food and chemical toxicology : an international journal published for the British Industrial Biological Research Association.

[128] S. Jackson,et al. Regulation of p53 in response to DNA damage , 1999, Oncogene.

[129] S. Schnitt,et al. Classification and prognosis of invasive breast cancer: from morphology to molecular taxonomy , 2010, Modern Pathology.

[130] M. Protopopova,et al. Small molecule RITA binds to p53, blocks p53–HDM-2 interaction and activates p53 function in tumors , 2004, Nature Medicine.

[131] Xin Lu,et al. Live or let die: the cell's response to p53 , 2002, Nature Reviews Cancer.

[132] Shaomeng Wang,et al. A small molecule that disrupts Mdm2-p53 binding activates p53, induces apoptosis, and sensitizes lung cancer cells to chemotherapy , 2008, Cancer biology & therapy.

[133] L. Vassilev,et al. Targeting the p53–MDM2 interaction to treat cancer , 2004, British Journal of Cancer.

[134] S. Berg,et al. MDM2 inhibition sensitizes neuroblastoma to chemotherapy-induced apoptotic cell death , 2006, Molecular Cancer Therapeutics.

[135] E. García-Martín,et al. Expression of paclitaxel-inactivating CYP3A activity in human colorectal cancer: implications for drug therapy , 2002, British Journal of Cancer.

[136] B. Katzenellenbogen,et al. Molecular mechanisms of estrogen action: selective ligands and receptor pharmacology , 2000, The Journal of Steroid Biochemistry and Molecular Biology.

[137] M. Oren,et al. The p53-Mdm2 module and the ubiquitin system. , 2003, Seminars in cancer biology.

[138] L. Vassilev,et al. Mouse double minute antagonist Nutlin-3a enhances chemotherapy-induced apoptosis in cancer cells with mutant p53 by activating E2F1 , 2007, Oncogene.

[139] A. Rajasekaran,et al. Estrogen Receptor-α Binds p53 Tumor Suppressor Protein Directly and Represses Its Function* , 2006, Journal of Biological Chemistry.

[140] Chih-Yi Chen,et al. Mutant p53 confers chemoresistance in non-small cell lung cancer by upregulating Nrf2 , 2015, Oncotarget.

[141] Shaomeng Wang,et al. Small Molecule Inhibitors of MDM2-p53 and MDMX-p53 Interactions as New Cancer Therapeutics , 2013 .

[142] Hsiao-Huei Wu,et al. MDM2--master regulator of the p53 tumor suppressor protein. , 2000, Gene.

[143] Maxwell D Cummings,et al. Discovery and cocrystal structure of benzodiazepinedione HDM2 antagonists that activate p53 in cells. , 2005, Journal of medicinal chemistry.

[144] Su Qiu,et al. Structure-based design of spiro-oxindoles as potent, specific small-molecule inhibitors of the MDM2-p53 interaction. , 2006, Journal of medicinal chemistry.

[145] Frank M Boeckler,et al. Targeted rescue of a destabilized mutant of p53 by an in silico screened drug , 2008, Proceedings of the National Academy of Sciences.

[146] Shaomeng Wang,et al. Targeting the MDM2-p53 Protein-Protein Interaction for New Cancer Therapeutics , 2012 .

[147] V. Grinkevich,et al. Rescue of the apoptotic-inducing function of mutant p53 by small molecule RITA. , 2010, Cell Cycle.

[148] D. Lane,et al. Cancer. p53, guardian of the genome. , 1992, Nature.

[149] G. Selivanova,et al. Dual Targeting of Wild-Type and Mutant p53 by Small Molecule RITA Results in the Inhibition of N-Myc and Key Survival Oncogenes and Kills Neuroblastoma Cells In Vivo and In Vitro , 2013, Clinical Cancer Research.

[150] H. Kantarjian,et al. Activation of p53 signaling by MI-63 induces apoptosis in acute myeloid leukemia cells , 2010, Leukemia & lymphoma.

[151] Weisi Wang,et al. Identification of novel inhibitors of p53–MDM2 interaction facilitated by pharmacophore-based virtual screening combining molecular docking strategy , 2013 .

[152] Jianbiao Zhou,et al. PRIMA-1met (APR-246) inhibits growth of colorectal cancer cells with different p53 status through distinct mechanisms , 2015, Oncotarget.

[153] L. Donehower,et al. P53 genotype as a determinant of ER expression and tamoxifen response in the MMTV-Wnt-1 model of mammary carcinogenesis , 2011, Breast Cancer Research and Treatment.

[154] J. Momand,et al. Identification of FDA‐approved Drugs that Computationally Bind to MDM2 , 2012, Chemical biology & drug design.

[155] A. Levine,et al. Allele-specific p53 mutant reactivation. , 2012, Cancer cell.

[156] P. Hersey,et al. Up-regulation of Mcl-1 is critical for survival of human melanoma cells upon endoplasmic reticulum stress. , 2008, Cancer research.

[157] A. Janin,et al. TP53 Status and Response to Treatment in Breast Cancers , 2011, Journal of biomedicine & biotechnology.

[158] C. Creighton,et al. SAR405838: A Novel and Potent Inhibitor of the MDM2:p53 Axis for the Treatment of Dedifferentiated Liposarcoma , 2015, Clinical Cancer Research.

[159] Nuria Llecha,et al. 6‐Hydroxydopamine activates the mitochondrial apoptosis pathway through p38 MAPK‐mediated, p53‐independent activation of Bax and PUMA , 2008, Journal of neurochemistry.

[160] Yi Sun,et al. Targeting p53 for Novel Anticancer Therapy. , 2010, Translational oncology.

[161] A. Batova,et al. Chemistry and biology of the caged Garcinia xanthones. , 2010, Chemistry.

[162] K. Kinzler,et al. Disruption of p53 in human cancer cells alters the responses to therapeutic agents. , 1999, The Journal of clinical investigation.