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    Protein kinase C isozymes, novel phorbol ester receptors and cancer chemotherapy.

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    Authors
    Barry, O P
    Kazanietz, M G
    Affiliation
    Cork Cancer Research Center and Department of Medicine, Clinical Science, Building, Cork University Hospital, Wilton Road, Cork, Ireland., goggieie@yahoo.com
    Issue Date
    2012-02-03T15:11:23Z
    MeSH
    Animals
    Antineoplastic Agents/chemistry/*metabolism
    Binding Sites
    *Caenorhabditis elegans Proteins
    Drug Design
    Humans
    Phorbols/chemistry/*metabolism
    Protein Kinase C/antagonists & inhibitors/*chemistry/*metabolism/physiology
    Receptors, Drug/chemistry/*metabolism
    
    Metadata
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    Citation
    Curr Pharm Des. 2001 Nov;7(17):1725-44.
    Journal
    Current pharmaceutical design
    URI
    http://hdl.handle.net/10147/209067
    PubMed ID
    11562308
    Abstract
    Recent years have seen extensive growth in the understanding of the role(s) of the various PKC isozymes and novel receptors for the phorbol ester tumor promoters. The PKC family of serine-threonine kinases is an important regulator of signaling cascades that control cell proliferation and death, and therefore represent targets for cancer therapy. While past interests have focused on PKC-selective inhibitors, more recently, intensive research has been underway for selective activators and inhibitors for each individual PKC isozyme. In the past few years a large number of PKC activators and inhibitors with potential as anticancer agents have been developed. A number of these compounds are already in Phase II clinical testing. As a new generation of cancer chemotherapeutic agents are designed, developed and put through a series of rigorous clinical trials, we can anticipate achieving exquisite control over PKC-mediated regulatory pathways, leading ultimately to a greater understanding of different cancers.
    Language
    eng
    ISSN
    1381-6128 (Print)
    1381-6128 (Linking)
    Collections
    Cork University Hospital

    entitlement

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