| Literature DB >> 25667438 |
Philip Lee1, Ben Murphy1, Rickey Miller1, Vivek Menon1, Naren L Banik2, Pierre Giglio3, Scott M Lindhorst1, Abhay K Varma1, William A Vandergrift1, Sunil J Patel1, Arabinda Das4.
Abstract
Glioblastoma is the most common and deadliest of malignant primary brain tumors (Grade IV astrocytoma) in adults. Current standard treatments have been improving but patient prognosis still remains unacceptably devastating. Glioblastoma recurrence is linked to epigenetic mechanisms and cellular pathways. Thus, greater knowledge of the cellular, genetic and epigenetic origin of glioblastoma is the key for advancing glioblastoma treatment. One rapidly growing field of treatment, epigenetic modifiers; histone deacetylase inhibitors (HDACis), has now shown much promise for improving patient outcomes through regulation of the acetylation states of histone proteins (a form of epigenetic modulation) and other non-histone protein targets. HDAC inhibitors have been shown, in a pre-clinical setting, to be effective anticancer agents via multiple mechanisms, by up-regulating expression of tumor suppressor genes, inhibiting oncogenes, inhibiting tumor angiogenesis and up-regulating the immune system. There are many HDAC inhibitors that are currently in pre-clinical and clinical stages of investigation for various types of cancers. This review will explain the theory of epigenetic cancer therapy, identify HDAC inhibitors that are being investigated for glioblastoma therapy, explain the mechanisms of therapeutic effects as demonstrated by pre-clinical and clinical studies and describe the current status of development of these drugs as they pertain to glioblastoma therapy. CopyrightEntities:
Keywords: Clinical trials; epigenetics; glioblastoma; histone deacetylase inhibitor; preclinical trials; review
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Year: 2015 PMID: 25667438 PMCID: PMC6052863
Source DB: PubMed Journal: Anticancer Res ISSN: 0250-7005 Impact factor: 2.480