A phase I clinical trial of dendritic cell immunotherapy in HCV-infected individuals

Gowans, Eric J.; Roberts, Stuart; Jones, Kathryn; Dinatale, Irene; Latour, Philippe A.; Chua, Brendan; Eriksson, Emily M.Y.; Chin, Ruth; Li, Shuo; Wall, Dominic M.; Sparrow, Rosemary L.; Moloney, Jude; Loudovaris, Maureen; Ffrench, Rosemary; Prince, H. Miles; Hart, Derek; Zeng, Weng; Torresi, Joseph; Brown, Lorena E.; Jackson, David C.

doi:10.1016/j.jhep.2010.05.007

« Previous Next »Journal of Hepatology
Volume 53, Issue 4 , Pages 599-607, October 2010

A phase I clinical trial of dendritic cell immunotherapy in HCV-infected individuals

Eric J. Gowans
- Virology Program, Burnet Institute, G.P.O. Box 2284, Melbourne, Vic. 3001, Australia
- Corresponding author. Present address: Women’s and Children’s Health Research Institute, 72 King William Road, North Adelaide, SA 5006, Australia. Tel.: +61 8 8161 7443; fax: +61 8 8239 0267.
Stuart Roberts
- Department of Gastroenterology, The Alfred Hospital, Commercial Road, Melbourne, Vic. 3004, Australia
Kathryn Jones
- Virology Program, Burnet Institute, G.P.O. Box 2284, Melbourne, Vic. 3001, Australia
Irene Dinatale
- Department of Microbiology and Immunology, The University of Melbourne, Parkville, Vic. 3010, Australia
Philippe A. Latour
- Virology Program, Burnet Institute, G.P.O. Box 2284, Melbourne, Vic. 3001, Australia
Brendan Chua
- Department of Microbiology and Immunology, The University of Melbourne, Parkville, Vic. 3010, Australia
Emily M.Y. Eriksson
- Department of Microbiology and Immunology, The University of Melbourne, Parkville, Vic. 3010, Australia
Ruth Chin
- Department of Infectious Diseases, Austin Hospital, Heidelberg, Vic., Australia
Shuo Li
- Virology Program, Burnet Institute, G.P.O. Box 2284, Melbourne, Vic. 3001, Australia
Dominic M. Wall
- Centre for Blood Cell Therapies, Peter MacCallum Cancer Centre, St. Andrews Place, East Melbourne, Vic. 3002, Australia
Rosemary L. Sparrow
- Australian Red Cross Blood Service, Kavanagh Street, South Melbourne, Vic. 3205, Australia
Jude Moloney
- Centre for Blood Cell Therapies, Peter MacCallum Cancer Centre, St. Andrews Place, East Melbourne, Vic. 3002, Australia
Maureen Loudovaris
- Centre for Blood Cell Therapies, Peter MacCallum Cancer Centre, St. Andrews Place, East Melbourne, Vic. 3002, Australia
Rosemary Ffrench
- Virology Program, Burnet Institute, G.P.O. Box 2284, Melbourne, Vic. 3001, Australia
H. Miles Prince
- Centre for Blood Cell Therapies, Peter MacCallum Cancer Centre, St. Andrews Place, East Melbourne, Vic. 3002, Australia
- Faculty of Medicine, Dentistry and Health Sciences, The University of Melbourne, Parkville, Vic. 3052, Australia
Derek Hart
- Mater Medical Research Institute, Aubigny Place, Raymond Terrace, South Brisbane, Qld 4101, Australia
Weng Zeng
- Department of Microbiology and Immunology, The University of Melbourne, Parkville, Vic. 3010, Australia
Joseph Torresi
- Department of Infectious Diseases, Austin Hospital, Heidelberg, Vic., Australia
Lorena E. Brown
- Department of Microbiology and Immunology, The University of Melbourne, Parkville, Vic. 3010, Australia
David C. Jackson
- Department of Microbiology and Immunology, The University of Melbourne, Parkville, Vic. 3010, Australia

Received 28 September 2009; received in revised form 11 May 2010; accepted 30 May 2010. published online 29 June 2010.

Background & Aims

HCV patients who fail conventional interferon-based therapy have limited treatment options. Dendritic cells are central to the priming and development of antigen-specific CD4⁺ and CD8⁺ T cell immunity, necessary to elicit effective viral clearance. The aim of the study was to investigate the safety and efficacy of vaccination with autologous dendritic cells loaded with HCV-specific cytotoxic T cell epitopes.

Methods

We examined the potential of autologous monocyte-derived dendritic cells (MoDC), presenting HCV-specific HLA A2.1-restricted cytotoxic T cell epitopes, to influence the course of infection in six patients who failed conventional therapy. Dendritic cells were loaded and activated ex vivo with lipopeptides. In this phase 1 dose escalation study, all patients received a standard dose of cells by the intradermal route while sequential patients received an increased dose by the intravenous route.

Results

No patient showed a severe adverse reaction although all experienced transient minor side effects. HCV-specific CD8⁺ T cell responses were enumerated in PBMC by ELIspot for interferon-γ. Patients generated de novo responses, not only to peptides presented by the cellular vaccine but also to additional viral epitopes not represented in the lipopeptides, suggestive of epitope spreading. Despite this, no increases in ALT levels were observed. However, the responses were not sustained and failed to influence the viral load, the anti-HCV core antibody response and the level of circulating cytokines.

Conclusions

Immunotherapy using autologous MoDC pulsed with lipopeptides was safe, but was unable to generate sustained responses or alter the outcome of the infection. Alternative dosing regimens or vaccination routes may need to be considered to achieve therapeutic benefit.

Abbreviations: HCV, hepatitis C virus, DC, dendritic cells, IFN, interferon, LN, lymph nodes, CTL, cytotoxic T lymphocyte, PBMC, peripheral blood mononuclear cells, SFC, spot forming cells, MoDC, monocyte-derived dendritic cells, IDU, intravenous drug user, ULN, upper limit of normal, ID, intradermal, IV, intravenous