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Data from Targeting a Glioblastoma Cancer Stem-Cell Population Defined by EGF Receptor Variant III

Posted on 2023-03-30 - 22:23
Abstract

The relationship between mutated proteins and the cancer stem-cell population is unclear. Glioblastoma tumors frequently express EGFRvIII, an EGF receptor (EGFR) variant that arises via gene rearrangement and amplification. However, expression of EGFRvIII is restricted despite the prevalence of the alteration. Here, we show that EGFRvIII is highly coexpressed with CD133 and that EGFRvIII+/CD133+ defines the population of cancer stem cells (CSC) with the highest degree of self-renewal and tumor-initiating ability. EGFRvIII+ cells are associated with other stem/progenitor markers, whereas markers of differentiation are found in EGFRvIII cells. EGFRvIII expression is lost in standard cell culture, but its expression is maintained in tumor sphere culture, and cultured cells also retain the EGFRvIII+/CD133+ coexpression, self-renewal, and tumor initiating abilities. Elimination of the EGFRvIII+/CD133+ population using a bispecific antibody reduced tumorigenicity of implanted tumor cells better than any reagent directed against a single epitope. This work demonstrates that a mutated oncogene can have CSC-specific expression and be used to specifically target this population. Cancer Res; 74(4); 1238–49. ©2013 AACR.

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Cancer Research

AUTHORS (12)

  • David R. Emlet
    Puja Gupta
    Marina Holgado-Madruga
    Catherine A. Del Vecchio
    Siddhartha S. Mitra
    Shuang-Yin Han
    Gordon Li
    Kristin C. Jensen
    Hannes Vogel
    Linda Wei Xu
    Stephen S. Skirboll
    Albert J. Wong
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