HER2 chimeric antigen receptor T cell immunotherapy is an effective treatment for diffuse intrinsic pontine glioma

Author:

Wang Stacie S123ORCID,Davenport Alexander J1ORCID,Iliopoulos Melinda1,Hughes-Parry Hannah E1ORCID,Watson Katherine A1ORCID,Arcucci Valeria1ORCID,Mulazzani Matthias1ORCID,Eisenstat David D23ORCID,Hansford Jordan R4ORCID,Cross Ryan S1ORCID,Jenkins Misty R156ORCID

Affiliation:

1. Immunology Division, The Walter and Eliza Hall Institute of Medical Research , Parkville, VIC , Australia

2. Murdoch Children’s Research Institute , Parkville, VIC , Australia

3. Children’s Cancer Centre, Royal Children’s Hospital , Parkville, VIC , Australia

4. Michael Rice Cancer Centre, Women’s and Children’s Hospital, South Australia Health and Medical Research Institute, South Australia ImmunoGENomics Cancer Institute, University of Adelaide , Adelaide, South Australia , Australia

5. Department of Medical Biology, University of Melbourne , Parkville , Australia

6. Department of Biochemistry, La Trobe Institute for Molecular Science , Bundoora, VIC Australia

Abstract

Abstract Background Diffuse intrinsic pontine glioma (DIPG) and other diffuse midline gliomas (DMG) of the thalamus and spinal cord are rare but devastating high-grade glial tumors of childhood with no curative treatment. Despite aggressive treatment attempts the prognosis has remained poor. Chimeric antigen receptor (CAR) T cell therapy has been identified as a promising new approach in the treatment of DMG tumors; however, additional targets are urgently required given known tumor heterogeneity and the prospect of antigen escape of this cancer. Methods Using cell surface mass spectrometry, we detected high HER2 cell surface protein across a panel of patient-derived DIPG cells, thereby identifying an existing CAR T cell therapy for use in DIPG. Primary human T cells were transduced to express a second-generation HER2 CAR and interrogated for efficacy against patient-derived DIPG cells. Results HER2 CAR T cells demonstrated potent and antigen-specific cytotoxicity and cytokine secretion when co-cultured with patient-derived DIPG cells. Furthermore, HER2 CAR T cells provided a significant regression in intracranial DIPG xenograft tumors. Conclusions HER2 CAR T cells are already in clinic development and are well tolerated in pediatric patients. Here we provide strong preclinical evidence for the inclusion of DIPG patients in future pediatric CNS tumor HER2 CAR T cell clinical trials.

Funder

German Cancer Aid

National Health and Medical Research Council

Robert Connor Dawes Foundation

Isabella and Marcus Foundation

Victorian Paediatric Cancer Consortium

Cancer Australia

Publisher

Oxford University Press (OUP)

Subject

Surgery,Oncology,Neurology (clinical)

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