Design of a phase I clinical trial to evaluate intratumoral delivery of ErbB-targeted chimeric antigen receptor T-cells in locally advanced or recurrent head and neck cancer

May C I van Schalkwyk; Sophie E Papa; Jean-Pierre Jeannon; Teresa Guerrero Urbano; James F Spicer; John Maher

doi:10.1089/humc.2013.144

Design of a phase I clinical trial to evaluate intratumoral delivery of ErbB-targeted chimeric antigen receptor T-cells in locally advanced or recurrent head and neck cancer

Hum Gene Ther Clin Dev. 2013 Sep;24(3):134-42. doi: 10.1089/humc.2013.144.

Authors

May C I van Schalkwyk¹, Sophie E Papa, Jean-Pierre Jeannon, Teresa Guerrero Urbano, James F Spicer, John Maher

Affiliation

¹ 1 Department of Research Oncology, King's Health Partners Integrated Cancer Centre , King's College London, London SE1 9RT, United Kingdom .

PMID: 24099518
DOI: 10.1089/humc.2013.144

Abstract

Despite several advances, 5-year survival in patients with head and neck squamous cell carcinoma (HNSCC) remains unchanged at only 50%. The commonest cause of death is locally advanced/recurrent disease. Consequently, there is an unmet need for new approaches to improve local control in HNSCC. T4 immunotherapy is an autologous cell therapy in which peripheral blood T-cells are genetically engineered using a retroviral vector to coexpress two chimeric receptors: (i) T1E28z is a chimeric antigen receptor that engages multiple ErbB dimers that are commonly upregulated in HNSCC; (ii) 4αβ is a chimeric cytokine receptor that converts the weak mitogenic stimulus provided by interleukin (IL)-4 into a strong and selective growth signal, allowing preferential expansion and enrichment of T4(+) T-cells ex vivo. T4 immunotherapy exerts antitumor activity against HNSCC cell lines and tumors in vivo, without significant toxicity. Human T4(+) T-cells also engage mouse ErbB receptors, permitting safety testing in SCID Beige mice. Severe toxicity caused by cytokine release syndrome ensues when human T4(+) T-cells are administered at high doses to mice, particularly with advanced tumor burdens. However, such toxicity is not required for efficacy and is never seen if T-cells are administered by the intratumoral route. To exploit this, we have designed a first-in-man clinical trial in which T4(+) T-cells are administered to patients with locally advanced/recurrent HNSCC. Cells will be administered at a single sitting to multiple sites around the viable tumor circumference. A 3+3 dose escalation design will be used, starting at 10(7) cells (cohort 1), escalating to 10(9) cells (cohort 5). If maximum tolerated dose remains undefined, cohorts 6/7 will receive either low- or high-dose cyclophosphamide before 10(9) T4(+) T-cells. A panel of routine/in-house assays and imaging techniques will be used to monitor safety, efficacy, perturbation of endogenous antitumor immunity, immunogenicity, and T-cell trafficking.

Trial registration: ClinicalTrials.gov NCT01818323.

Publication types

Clinical Trial, Phase I
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Carcinoma, Squamous Cell / therapy*
Female
Genes, erbB*
Genetic Therapy*
Head and Neck Neoplasms / therapy*
Humans
Immunotherapy*
Male
Receptors, Antigen / genetics
Receptors, Antigen / immunology
Receptors, Cytokine / genetics
Receptors, Cytokine / immunology
Recombinant Proteins / administration & dosage
Recombinant Proteins / adverse effects
Recombinant Proteins / pharmacokinetics
Research Design
T-Lymphocytes / immunology
T-Lymphocytes / transplantation

Substances

Receptors, Antigen
Receptors, Cytokine
Recombinant Proteins

Associated data

ClinicalTrials.gov/NCT01818323

Grants and funding

PA12-06/PCUK_/Prostate Cancer UK/United Kingdom