Enhancing Natural Killer and CD8+ T Cell-Mediated Anticancer Cytotoxicity and Proliferation of CD8+ T Cells with HLA-E Monospecific Monoclonal Antibodies

Mepur H Ravindranath; Edward J Filippone; Asokan Devarajan; Shahab Asgharzadeh

doi:10.1089/mab.2018.0043

Enhancing Natural Killer and CD8⁺ T Cell-Mediated Anticancer Cytotoxicity and Proliferation of CD8⁺ T Cells with HLA-E Monospecific Monoclonal Antibodies

Monoclon Antib Immunodiagn Immunother. 2019 Apr;38(2):38-59. doi: 10.1089/mab.2018.0043.

Authors

Mepur H Ravindranath¹, Edward J Filippone², Asokan Devarajan³, Shahab Asgharzadeh⁴

Affiliations

¹ 1 Department of Hematology and Oncology, Children's Hospital, Los Angeles, California.
² 2 Division of Nephrology, Department of Medicine, Sidney Kimmel Medical College, Thomas Jefferson University, Philadelphia, Pennsylvania.
³ 3 Division of Cardiology, Department of Medicine, David Geffen School of Medicine, University of California Los Angeles, Los Angeles, California.
⁴ 4 Department of Pediatrics and Pathology, Children's Hospital, Keck School of Medicine, USC, Los Angeles, California.

Abstract

Cytotoxic NK/CD8⁺ T cells interact with MHC-I ligands on tumor cells through either activating or inhibiting receptors. One of the inhibitory receptors is CD94/NKG2A. The NK/CD8⁺ T cell cytotoxic capability is lost when tumor-associated human leukocyte antigen, HLA-E, binds the CD94/NKG2A receptor, resulting in tumor progression and reduced survival. Failure of cancer patients to respond to natural killer (NK) cell therapies could be due to HLA-E overexpression in tumor tissues. Preventing the inhibitory receptor-ligand interaction by either receptor- or ligand-specific monoclonal antibodies (mAbs) is an innovative passive immunotherapeutic strategy for cancer. Since receptors and ligands can be monomeric or homo- or heterodimeric proteins, the efficacy of mAbs may rely on their ability to distinguish monospecific (private) functional epitopes from nonfunctional common (public) epitopes. We developed monospecific anti-HLA-E mAbs (e.g., TFL-033) that recognize only HLA-E-specific epitopes, but not epitopes shared with other HLA class-I loci as occurs with currently available polyreactive anti-HLA-E mAbs. Interestingly the amino acid sequences in the α1 and α2 helices of HLA-E, critical for the recognition of the mAb TFL-033, are strikingly the same sequences recognized by the CD94/NKG2A inhibitory receptors on NK/CD8⁺ cells. Such monospecific mAbs can block the CD94/NKG2A interaction with HLA-E to restore NK cell and CD8⁺ anticancer cell cytotoxicity. Furthermore, the HLA-E monospecific mAbs significantly promoted the proliferation of the CD4^-/CD8⁺ T cells. These monospecific mAbs are also invaluable for the specific demonstration of HLA-E on tumor biopsies, potentially indicating those tumors most likely to respond to such therapy. Thus, they can be used to enhance passive immunotherapy once phased preclinical studies and clinical trials are completed. On principle, we postulate that NK cell passive immunotherapy should capitalize on both of these features of monospecific HLA-E mAbs, that is, the specific determination HLA-E expression on a particular tumor and the enhancement of NK cell/CD8⁺ cytotoxicity if HLA-E positive.

Keywords: human leukocyte antigen; mean fluorescent intensity; monoclonal antibody; monospecific versus polyreactive; natural killer receptors; single antigen bead assay.

Publication types

Review

MeSH terms

Animals
Antibodies, Monoclonal / immunology*
CD8-Positive T-Lymphocytes / immunology*
Cell Proliferation
Cytotoxicity, Immunologic / immunology*
HLA-E Antigens
Histocompatibility Antigens Class I / immunology*
Humans
Immunity, Cellular
Killer Cells, Natural / immunology*
Neoplasms / immunology*
Neoplasms / pathology*
Receptors, Immunologic

Substances

Antibodies, Monoclonal
Histocompatibility Antigens Class I
Receptors, Immunologic