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NS10282

Genomic integrity and instability mechanisms in the pathogenesis and potential personalized targeted treatment of prostate cancer.

Project goals

Genomic integrity and instability mechanisms in the pathogenesis and potential personalized targeted treatment of prostate cancer. PI: J. Bártek The key topic of this project is analysis of cell cycle checkpoints and genome integrity maintenance mechanisms (e.g. in radio/chemotherapy) in prostate cancer, to better understand molecular pathogenesis, treatment responsiveness or resistance, and the role of cancer stem cells in these processes. We will use cell culture and gene transfer models, clinical material and a wide range of immunohistochemical, cell and molecular biology methods. The project will elucidate resistance to standard treatment, predictive assessment and individualized management, especially in androgen-independent prostate tumours, to provide new insights into genetic instability and proposals for combining standard radio/chemotherapy and targeted modulation of DNA damage signaling and repair pathways. This project should therefore address one of the major concerns in current oncology.

Keywords

prostate-cancercell-cyclepathogenesis/mechanismsstem-cellsDNA-damagesignalingDNA repairtargeted-therapy

Public support

  • Provider

    Ministry of Health

  • Programme

    Departmental Programme of Research and Development - MH II from 2008 to 2011

  • Call for proposals

    VaV pro Ministerstvo zdravotnictví II 2 (SMZ0200901)

  • Main participants

  • Contest type

    VS - Public tender

  • Contract ID

    NS10282-3/2009

Alternative language

  • Project name in Czech

    Mechanismy integrity a nestability genomu v patogeneze a potenciální individualizovaná molekulárně-cílená léčba karcinomu prostaty

  • Annotation in Czech

    Mechanismy integrity a nestability genomu v patogeneze a potenciální individualizovaná molekulárně-cílená léčba karcinomu prostaty Hl. řešitel J. Bártek Předmětem projektu je studium mechanismů regulace buněčného cyklu a integrity genomu (např. u radio-a chemoterapie) u rakoviny prostaty, s cílem lépe pochopit molekulární patogenezi, citlivost či rezistenci na léčbu a úlohu nádorových kmenových buněk v těchto procesech. K řešení bude využito modelů buněčných kultur a genového přenosu, klinického materiálu a imunohistochemie a metod buněčné a molekulární biologie. Projekt přispěje k objasnění rezistence na klasickou léčbu, k odhadu odpovědi na terapii a k přiblížení individualizace léčby, zejména u obtížně léčitelných, na androgenech nezávislych nadorůprostaty, včetně lepšího pochopení genetické nestability a návrhu strategie kombinace klasické radio-/chemoterapie a molekulárně-cílené modulace signalizace a opravy poškozené DNA. Projekt tedy přispěje k řešení závažného problému současné onkologie.

Scientific branches

  • R&D category

    NV - Nonindustrial research (Applied research excluded Industrial research)

  • CEP classification - main branch

    FD - Oncology and haematology

  • CEP - secondary branch

    EB - Genetics and molecular biology

  • CEP - another secondary branch

  • 10603 - Genetics and heredity (medical genetics to be 3)
    10604 - Reproductive biology (medical aspects to be 3)
    10605 - Developmental biology
    10608 - Biochemistry and molecular biology
    10609 - Biochemical research methods
    30101 - Human genetics
    30204 - Oncology
    30205 - Hematology

Completed project evaluation

  • Provider evaluation

    V - Vynikající výsledky projektu (s mezinárodním významem atd.)

  • Project results evaluation

    The project dealt with mechanisms of cellular response to DNA damage in different types of tumor cells to clarify the origin and development of prostate cancer.

Solution timeline

  • Realization period - beginning

    Jan 1, 2009

  • Realization period - end

    Dec 31, 2011

  • Project status

    U - Finished project

  • Latest support payment

    Aug 8, 2011

Data delivery to CEP

  • Confidentiality

    S - Úplné a pravdivé údaje o projektu nepodléhají ochraně podle zvláštních právních předpisů

  • Data delivery code

    CEP12-MZ0-NS-U/09:3

  • Data delivery date

    Oct 31, 2013

Finance

  • Total approved costs

    5,158 thou. CZK

  • Public financial support

    5,148 thou. CZK

  • Other public sources

    0 thou. CZK

  • Non public and foreign sources

    9 thou. CZK

Recognised costs

5 158 CZK thou.

Public support

5 148 CZK thou.

0%

Provider

Ministry of Health

CEP

FD - Oncology and haematology

Solution period

01. 01. 2009 - 31. 12. 2011

Similar projects(10)

Analysis and targeting of DNA damage signaling and repair mechanisms in glioblastomas and glioblastoma stem cells as a strategy to elucidate pathogenesis and search for individualized targeted treatments combined with standard therapy (NT11065) Study of the mechanism of neoadjuvant chemotherapy-induced cell death and mechanism of chemotherapy resistance in patient with breast carcinoma (NS10575) Role of transposable elements and PIWI-interacting RNAs in myelodysplastic syndrome and their potential clinical applications (NU20-03-00412)