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Targeting gp100 and TRP-2 with a DNA vaccine: incorporating T cell epitopes with a human IgG1 antibody induces potent T cell responses that are associated with favourable clinical outcome in a phase I/II trial

Patel, Poulam M.; Ottensmeier, Christian H.; Mulatero, Clive; Lorigan, Paul; Plummer, Ruth; Pandha, Hardev S.; Elsheikh, Somaia; Hadjimichael, Efthymios; Villasanti, Naty; Cunnell, Michelle; Metheringham, Rachael L.; Brentville, Victoria A.; Machado, Lee; Daniels, Ian; Gijon, Mohamed; Hannaman, Drew; Durrant, Lindy

Authors

POULAM PATEL POULAM.PATEL@NOTTINGHAM.AC.UK
Professor of Clinical Oncology

Christian H. Ottensmeier

Clive Mulatero

Paul Lorigan

Ruth Plummer

Hardev S. Pandha

Somaia Elsheikh

Efthymios Hadjimichael

Naty Villasanti

Michelle Cunnell

Rachael L. Metheringham

Victoria A. Brentville

Lee Machado

Ian Daniels

Mohamed Gijon

Drew Hannaman

Lindy Durrant



Abstract

A DNA vaccine, SCIB1, incorporating two CD8 and two CD4 epitopes from TRP-2/gp100 was evaluated in patients with metastatic melanoma. Each patient received SCIB1 via intramuscular injection with electroporation. The trial was designed to find the safest dose of SCIB1 which induced immune/clinical responses in patients with or without tumour. Fifteen patients with tumor received SCIB1 doses of 0.4-8░mg whilst 20 fully-resected patients received 2–8░mg doses. Twelve patients elected to continue immunization every 3 months for up to 39 months. SCIB1 induced dose-dependent T cell responses in 88% of patients with no serious adverse effects or dose limiting toxicities. The intensity of the T cell responses was significantly higher in patients receiving 4░mg doses without tumor when compared to those with tumor (p< 0.01). In contrast, patients with tumor showed a significantly higher response to the 8░mg dose than the 4░mg dose (p< 0.03) but there was no significant difference in the patients without tumor. One of 15 patients with measurable disease showed an objective tumor response and 7/15 showed stable disease. 5/20 fully-resected patients have experienced disease recurrence but all remained alive at the cut-off date with a median observation time of 37 months. A positive clinical outcome was associated with MHC-I and MHC-II expression on tumors prior to therapy (p = 0.027).

We conclude that SCIB1 is well tolerated and stimulates potent T cell responses in melanoma patients. It deserves further evaluation as a single agent adjuvant therapy or in combination with checkpoint inhibitors in advanced disease.

Citation

Patel, P. M., Ottensmeier, C. H., Mulatero, C., Lorigan, P., Plummer, R., Pandha, H. S., …Durrant, L. (2018). Targeting gp100 and TRP-2 with a DNA vaccine: incorporating T cell epitopes with a human IgG1 antibody induces potent T cell responses that are associated with favourable clinical outcome in a phase I/II trial. OncoImmunology, 7(6), Article e1433516. https://doi.org/10.1080/2162402X.2018.1433516

Journal Article Type Article
Acceptance Date Jan 22, 2018
Online Publication Date Feb 1, 2018
Publication Date Jun 30, 2018
Deposit Date Feb 15, 2018
Publicly Available Date Aug 20, 2018
Journal Oncoimmunology
Print ISSN 2162-4011
Electronic ISSN 2162-402X
Publisher Taylor & Francis Open
Peer Reviewed Peer Reviewed
Volume 7
Issue 6
Article Number e1433516
DOI https://doi.org/10.1080/2162402X.2018.1433516
Keywords Immunotherapy, vaccine, melanoma, T-cell
Public URL https://nottingham-repository.worktribe.com/output/909353
Publisher URL http://www.tandfonline.com/doi/full/10.1080/2162402X.2018.1433516

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