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Germline and Somatic Genetic Variants in the p53 Pathway Interact to Affect Cancer Risk, Progression, and Drug Response.
Zhang, Ping; Kitchen-Smith, Isaac; Xiong, Lingyun; Stracquadanio, Giovanni; Brown, Katherine; Richter, Philipp H; Wallace, Marsha D; Bond, Elisabeth; Sahgal, Natasha; Moore, Samantha; Nornes, Svanhild; De Val, Sarah; Surakhy, Mirvat; Sims, David; Wang, Xuting; Bell, Douglas A; Zeron-Medina, Jorge; Jiang, Yanyan; Ryan, Anderson J; Selfe, Joanna L; Shipley, Janet; Kar, Siddhartha; Pharoah, Paul D; Loveday, Chey; Jansen, Rick; Grochola, Lukasz F; Palles, Claire; Protheroe, Andrew; Millar, Val; Ebner, Daniel V; Pagadala, Meghana; Blagden, Sarah P; Maughan, Timothy S; Domingo, Enric; Tomlinson, Ian; Turnbull, Clare; Carter, Hannah; Bond, Gareth L.
Afiliação
  • Zhang P; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Kitchen-Smith I; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Xiong L; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Stracquadanio G; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Brown K; Weatherall Institute of Molecular Medicine, University of Oxford, John Radcliffe Hospital, Oxford, United Kingdom.
  • Richter PH; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Wallace MD; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Bond E; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Sahgal N; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Moore S; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Nornes S; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • De Val S; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Surakhy M; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Sims D; Weatherall Institute of Molecular Medicine, University of Oxford, John Radcliffe Hospital, Oxford, United Kingdom.
  • Wang X; Environmental Epigenomics and Disease Group, Immunity, Inflammation, and Disease Laboratory, National Institute of Environmental Health Sciences-National Institutes of Health, Research Triangle Park, North Carolina.
  • Bell DA; Environmental Epigenomics and Disease Group, Immunity, Inflammation, and Disease Laboratory, National Institute of Environmental Health Sciences-National Institutes of Health, Research Triangle Park, North Carolina.
  • Zeron-Medina J; Ludwig Institute for Cancer Research, University of Oxford, Nuffield Department of Clinical Medicine, Old Road Campus Research Building, Oxford, United Kingdom.
  • Jiang Y; Sarcoma Molecular Pathology Team, Divisions of Molecular Pathology and Cancer Therapeutics, The Institute of Cancer Research, Sutton, Surrey, United Kingdom.
  • Ryan AJ; CRUK & MRC Oxford Institute for Radiation Oncology, University of Oxford, Department of Oncology, Old Road Campus Research Building, Oxford, United Kingdom.
  • Selfe JL; CRUK & MRC Oxford Institute for Radiation Oncology, University of Oxford, Department of Oncology, Old Road Campus Research Building, Oxford, United Kingdom.
  • Shipley J; Sarcoma Molecular Pathology Team, Divisions of Molecular Pathology and Cancer Therapeutics, The Institute of Cancer Research, Sutton, Surrey, United Kingdom.
  • Kar S; Sarcoma Molecular Pathology Team, Divisions of Molecular Pathology and Cancer Therapeutics, The Institute of Cancer Research, Sutton, Surrey, United Kingdom.
  • Pharoah PD; Department of Public Health and Primary Care, University of Cambridge, Cambridge, United Kingdom.
  • Loveday C; Department of Public Health and Primary Care, University of Cambridge, Cambridge, United Kingdom.
  • Jansen R; Division of Genetics and Epidemiology, The Institute of Cancer Research, London, United Kingdom.
  • Grochola LF; Amsterdam UMC, Vrije Universiteit Amsterdam, Department of Psychiatry, Amsterdam Neuroscience, the Netherlands.
  • Palles C; Department of Surgery, Cantonal Hospital Winterthur, Switzerland.
  • Protheroe A; Institute of Cancer and Genomic Sciences, University of Birmingham, Birmingham, United Kingdom.
  • Millar V; Oxford Cancer and Haematology Centre, Oxford University Hospitals NHS Foundation Trust, Oxford, United Kingdom.
  • Ebner DV; Target Discovery Institute, University of Oxford, Nuffield Department of Medicine, Oxford, United Kingdom.
  • Pagadala M; Target Discovery Institute, University of Oxford, Nuffield Department of Medicine, Oxford, United Kingdom.
  • Blagden SP; Department of Medicine, University of California, San Diego, La Jolla, California.
  • Maughan TS; Department of Oncology, University of Oxford, Oxford, United Kingdom.
  • Domingo E; Department of Oncology, University of Oxford, Oxford, United Kingdom.
  • Tomlinson I; Department of Oncology, University of Oxford, Oxford, United Kingdom.
  • Turnbull C; Institute of Cancer and Genomic Sciences, University of Birmingham, Birmingham, United Kingdom.
  • Carter H; Division of Genetics and Epidemiology, The Institute of Cancer Research, London, United Kingdom.
  • Bond GL; Department of Medicine, University of California, San Diego, La Jolla, California. G.Bond.1@bham.ac.uk hkcarter@health.ucsd.edu.
Cancer Res ; 81(7): 1667-1680, 2021 04 01.
Article em En | MEDLINE | ID: mdl-33558336
ABSTRACT
Insights into oncogenesis derived from cancer susceptibility loci (SNP) hold the potential to facilitate better cancer management and treatment through precision oncology. However, therapeutic insights have thus far been limited by our current lack of understanding regarding both interactions of these loci with somatic cancer driver mutations and their influence on tumorigenesis. For example, although both germline and somatic genetic variation to the p53 tumor suppressor pathway are known to promote tumorigenesis, little is known about the extent to which such variants cooperate to alter pathway activity. Here we hypothesize that cancer risk-associated germline variants interact with somatic TP53 mutational status to modify cancer risk, progression, and response to therapy. Focusing on a cancer risk SNP (rs78378222) with a well-documented ability to directly influence p53 activity as well as integration of germline datasets relating to cancer susceptibility with tumor data capturing somatically-acquired genetic variation provided supportive evidence for this hypothesis. Integration of germline and somatic genetic data enabled identification of a novel entry point for therapeutic manipulation of p53 activities. A cluster of cancer risk SNPs resulted in increased expression of prosurvival p53 target gene KITLG and attenuation of p53-mediated responses to genotoxic therapies, which were reversed by pharmacologic inhibition of the prosurvival c-KIT signal. Together, our results offer evidence of how cancer susceptibility SNPs can interact with cancer driver genes to affect cancer progression and identify novel combinatorial therapies.

SIGNIFICANCE:

These results offer evidence of how cancer susceptibility SNPs can interact with cancer driver genes to affect cancer progression and present novel therapeutic targets.
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Texto completo: 1 Coleções: 01-internacional Temas: Geral / Tipos_de_cancer / Outros_tipos Base de dados: MEDLINE Assunto principal: Proteína Supressora de Tumor p53 / Resistencia a Medicamentos Antineoplásicos / Neoplasias Tipo de estudo: Diagnostic_studies / Etiology_studies / Observational_studies / Prognostic_studies / Risk_factors_studies / Systematic_reviews Limite: Animals / Female / Humans / Male Idioma: En Revista: Cancer Res Ano de publicação: 2021 Tipo de documento: Article País de afiliação: Reino Unido
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Coleções: 01-internacional Temas: Geral / Tipos_de_cancer / Outros_tipos Base de dados: MEDLINE Assunto principal: Proteína Supressora de Tumor p53 / Resistencia a Medicamentos Antineoplásicos / Neoplasias Tipo de estudo: Diagnostic_studies / Etiology_studies / Observational_studies / Prognostic_studies / Risk_factors_studies / Systematic_reviews Limite: Animals / Female / Humans / Male Idioma: En Revista: Cancer Res Ano de publicação: 2021 Tipo de documento: Article País de afiliação: Reino Unido