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      Molecular Markers in Glioma

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          Abstract

          Gliomas are the most malignant and aggressive form of brain tumors, and account for the majority of brain cancer related deaths. Malignant gliomas, including glioblastoma are treated with radiation and temozolomide, with only a minor benefit in survival time. A number of advances have been made in understanding glioma biology, including the discovery of cancer stem cells, termed glioma stem cells (GSC). Some of these advances include the delineation of molecular hetereogeneity both between tumors from different patients as well as within tumors from the same patient. Such research highlights the importance of identifying and validating molecular markers in glioma. This review, intended as a practical resource for both clinical and basic investigators, summarizes some of the more well-known molecular markers (MGMT, 1p/19q, IDH, EGFR, p53, PI3K, Rb, and RAF), discusses how they are identified, and what, if any, clinical relevance they many have, in addition to discussing some of the specific biology for these markers. Additionally, we discuss identification methods for studying putative GSC’s (CD133, CD15, A2B5, Nestin, ALDH1, Proteasome activity, ABC transporters, and Label-retention). While much research has been done on these markers, there is still a significant amount that we do not yet understand, which may account for some conflicting reports in the literature. Furthermore, it is unlikely that the investigator will be able to utilize one single marker to prospectively identify and isolate GSC from all, or possibly, any gliomas.

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          Author and article information

          Journal
          8309335
          5024
          J Neurooncol
          J. Neurooncol.
          Journal of neuro-oncology
          0167-594X
          1573-7373
          17 March 2017
          23 February 2017
          September 2017
          01 September 2018
          : 134
          : 3
          : 505-512
          Affiliations
          [1 ]Semel Institute for Neuroscience and Human Behavior and the Department of Psychiatry and Biobehavioral Research, David Geffen School of Medicine at UCLA, Los Angeles, CA 90095
          [2 ]Department of Molecular and Medical Pharmacology and Pediatrics, David Geffen School of Medicine at UCLA, Los Angeles, CA 90095
          Author notes
          Address correspondence to: Harley Kornblum, MD, PhD, Room 341 NRB, 635 Charles E. Young Drive South, Los Angeles, CA 90095, Hkornblum@ 123456mednet.ucla.edu
          Article
          PMC5568999 PMC5568999 5568999 nihpa855188
          10.1007/s11060-017-2379-y
          5568999
          28233083
          359340c3-cccb-4e83-9369-442431e975cc
          History
          Categories
          Article

          Pathways,and Mutations,Glioblastoma,Moledular Markers,Glioma Stem Cell

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