Literature DB >> 19951140

Molecularly targeted therapies for malignant glioma: rationale for combinatorial strategies.

Nikhil G Thaker1, Ian F Pollack.   

Abstract

Median survival of patients with malignant glioma (MG) from time of diagnosis is approximately 1 year, despite surgery, irradiation and conventional chemotherapy. Improving patient outcome relies on our ability to develop more effective therapies that are directed against the unique molecular aberrations within a patient's tumor. Such molecularly targeted therapies may provide novel treatments that are more effective than conventional chemotherapeutics. Recently developed therapeutic strategies have focused on targeting several core glioma signaling pathways, including pathways mediated by growth-factors, PI3K/Akt/PTEN/mTOR, Ras/Raf/MEK/MAPK and other vital pathways. However, given the molecular diversity, heterogeneity and diverging and converging signaling pathways associated with MG, it is unlikely that any single agent will have efficacy in more than a subset of tumors. Overcoming these therapeutic barriers will require multiple agents that can simultaneously inhibit these processes, providing a rationale for combination therapies. This review summarizes the currently implemented single-agent and combination molecularly targeted therapies for MG.

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Year:  2009        PMID: 19951140      PMCID: PMC2819818          DOI: 10.1586/ern.09.116

Source DB:  PubMed          Journal:  Expert Rev Neurother        ISSN: 1473-7175            Impact factor:   4.618


  211 in total

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  17 in total

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Authors:  Benjamin A Hoff; Mahaveer S Bhojani; John Rudge; Thomas L Chenevert; Charles R Meyer; Stefanie Galbán; Timothy D Johnson; Judith Sebolt Leopold; Alnawaz Rehemtulla; Brian D Ross; Craig J Galbán
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10.  Mitochondrial dysfunction RAD51, and Ku80 proteolysis promote apoptotic effects of Dinaciclib in Bcl-xL silenced cells.

Authors:  Daniel R Premkumar; Esther P Jane; Swetha Thambireddy; Philip A Sutera; Jonathon M Cavaleri; Ian F Pollack
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