Immunotherapy with antibody-targeted HLA class I complexes: results of in vivo tumour cell killing and therapeutic vaccination

Philip Savage; Julian Dyson; Maggie Milrain; Douglas Mathews; Ben King; H T Claude Chan; Linda Barber; Agamemnon Epenetos; Graham Ogg; Andrew McMichael; Martin J Glennie; Ruth R French

doi:10.1159/000107416

Immunotherapy with antibody-targeted HLA class I complexes: results of in vivo tumour cell killing and therapeutic vaccination

Tumour Biol. 2007;28(4):205-11. doi: 10.1159/000107416. Epub 2007 Aug 20.

Authors

Philip Savage¹, Julian Dyson, Maggie Milrain, Douglas Mathews, Ben King, H T Claude Chan, Linda Barber, Agamemnon Epenetos, Graham Ogg, Andrew McMichael, Martin J Glennie, Ruth R French

Affiliation

¹ Department of Medical Oncology, Charing Cross Hospital, London, UK. pmsavage@hhnt.nhs.uk

PMID: 17709989
DOI: 10.1159/000107416

Abstract

Background: The delivery of antibody-targeted major histocompatibility complex (MHC) class I complexes containing immunogenic peptides to the surface of tumour cells allows cytotoxic T lymphocytes (CTLs) of non-tumour specificity to recognise and kill the tumour cell. Previous studies have demonstrated the activity of this system in vitro and in a simple pre-clinical model. This system has also been shown to be an effective method of expanding antigen-specific CTLs in vitro when used to target MHC class I complexes to the surface of B cells.

Methods: Mice were immunised with ovalbumin and the survival of EL4Hu20 lymphoma cells targeted with H2-D(b)/Ova complexes and control MHC complexes was compared by FACS analysis. A tumour protection assay was performed where immunised mice were injected B16Hu20 melanoma cells targeted with H2-K(b)/Ova or control complexes. T cell expansion in vivo was examined by administering B cells targeted with MHC class I/peptide complexes and assessing T cell expansion by tetramer analysis.

Results: In vivo killing of H2-D(b)/Ova-targeted lymphoma cells in the immunised mice was demonstrated with these cells present at only 12% of the level of the control cells. In contrast, in non-immunised mice the survival of H2-D(b)/Ova-targeted and control cells was comparable. In the tumour protection assay, injection of melanoma cells targeted with H2-K(b)/Ova complexes resulted in the development of only a solitary metastasis in each mouse. This compared to an average of 130 metastases in the control mice injected with B16Hu20 cells targeted with a control MHC peptide complex. In vivo CTL expansion was demonstrated after a single intravenous administration of Daudi B cells coated with H2-D(b)/Uty complexes produced an increase in the proportion of Uty-reactive CTLs from 3.3 to 21.5%.

Conclusion: This study supports the development of antibody-delivered MHC complexes as a method of producing CTL-mediated lysis of cancer cells in vivo. As a therapeutic vaccine, the system may provide an effective approach for expanding oligoclonal T cell responses in vivo in the treatment of malignancy and infectious diseases.

MeSH terms

Animals
B-Lymphocytes / metabolism
Cancer Vaccines
Cell Separation
Female
HLA Antigens / chemistry*
Histocompatibility Antigens Class I / chemistry*
Immunotherapy / methods*
Mice
Mice, Inbred BALB C
Mice, Inbred C57BL
Mice, Transgenic
Neoplasms / metabolism*
T-Lymphocytes / metabolism
T-Lymphocytes, Cytotoxic / metabolism

Substances

Cancer Vaccines
HLA Antigens
Histocompatibility Antigens Class I

Abstract

MeSH terms

Substances

Grants and funding