Ad-CD40L mobilizes CD4 T cells for the treatment of brainstem tumors

Phonphimon Wongthida, Matthew R. Schuelke, Christopher B. Driscoll, Timothy Kottke, Jill M. Thompson, Jason Tonne, Cathy Stone, Amanda L. Huff, Cynthia Wetmore, James A. Davies, Alan L. Parker, Laura Evgin, Richard G. Vile

Research output: Contribution to journalArticlepeer-review

Abstract

Background: Diffuse midline glioma, formerly DIPG (diffuse intrinsic pontine glioma), is the deadliest pediatric brainstem tumor with median survival of less than one year. Here, we investigated (i) whether direct delivery of adenovirus-expressing cluster of differentiation (CD)40 ligand (Ad-CD40L) to brainstem tumors would induce immune-mediated tumor clearance and (ii) if so, whether therapy would be associated with a manageable toxicity due to immune-mediated inflammation in the brainstem. Methods: Syngeneic gliomas in the brainstems of immunocompetent mice were treated with Ad-CD40L and survival, toxicity, and immune profiles determined. A clinically translatable vector, whose replication would be tightly restricted to tumor cells, rAd-Δ24-CD40L, was tested in human patient-derived diffuse midline gliomas and immunocompetent models. Results: Expression of Ad-CD40L restricted to brainstem gliomas by pre-infection induced complete rejection, associated with immune cell infiltration, of which CD4+ T cells were critical for therapy. Direct intratumoral injection of Ad-CD40L into established brainstem tumors improved survival and induced some complete cures but with some acute toxicity. RNA-sequencing analysis showed that Ad-CD40L therapy induced neuroinflammatory immune responses associated with interleukin (IL)-6, IL-1β, and tumor necrosis factor α. Therefore, to generate a vector whose replication, and transgene expression, would be tightly restricted to tumor cells, we constructed rAd-Δ24-CD40L, the backbone of which has already entered clinical trials for diffuse midline gliomas. Direct intratumoral injection of rAd-Δ24-CD40L, with systemic blockade of IL-6 and IL-1β, generated significant numbers of cures with readily manageable toxicity. Conclusions: Virus-mediated delivery of CD40L has the potential to be effective in treating diffuse midline gliomas without obligatory neuroinflammation-associated toxicity.

Original languageEnglish (US)
Pages (from-to)1757-1770
Number of pages14
JournalNeuro-oncology
Volume22
Issue number12
DOIs
StatePublished - Dec 1 2020

Keywords

  • CD40L
  • adenovirus
  • brainstem tumors
  • immunotherapy
  • tertiary lymphoid structure

ASJC Scopus subject areas

  • Oncology
  • Clinical Neurology
  • Cancer Research

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