International Journal of Molecular Sciences (Jun 2024)

EGFRvIII Confers Sensitivity to Saracatinib in a STAT5-Dependent Manner in Glioblastoma

  • Mylan R. Blomquist,
  • Ryan Eghlimi,
  • Angad Beniwal,
  • Dustin Grief,
  • David G. Nascari,
  • Landon Inge,
  • Christopher P. Sereduk,
  • Serdar Tuncali,
  • Alison Roos,
  • Hannah Inforzato,
  • Ritin Sharma,
  • Patrick Pirrotte,
  • Shwetal Mehta,
  • Shannon P. Fortin Ensign,
  • Joseph C. Loftus,
  • Nhan L. Tran

DOI
https://doi.org/10.3390/ijms25116279
Journal volume & issue
Vol. 25, no. 11
p. 6279

Abstract

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Glioblastoma (GBM) is the most common primary malignant brain tumor in adults, with few effective treatments. EGFR alterations, including expression of the truncated variant EGFRvIII, are among the most frequent genomic changes in these tumors. EGFRvIII is known to preferentially signal through STAT5 for oncogenic activation in GBM, yet targeting EGFRvIII has yielded limited clinical success to date. In this study, we employed patient-derived xenograft (PDX) models expressing EGFRvIII to determine the key points of therapeutic vulnerability within the EGFRvIII-STAT5 signaling axis in GBM. Our findings reveal that exogenous expression of paralogs STAT5A and STAT5B augments cell proliferation and that inhibition of STAT5 phosphorylation in vivo improves overall survival in combination with temozolomide (TMZ). STAT5 phosphorylation is independent of JAK1 and JAK2 signaling, instead requiring Src family kinase (SFK) activity. Saracatinib, an SFK inhibitor, attenuates phosphorylation of STAT5 and preferentially sensitizes EGFRvIII+ GBM cells to undergo apoptotic cell death relative to wild-type EGFR. Constitutively active STAT5A or STAT5B mitigates saracatinib sensitivity in EGFRvIII+ cells. In vivo, saracatinib treatment decreased survival in mice bearing EGFR WT tumors compared to the control, yet in EGFRvIII+ tumors, treatment with saracatinib in combination with TMZ preferentially improves survival.

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