Therapeutic afucosylated monoclonal antibody and bispecific T-cell engagers for T-cell acute lymphoblastic leukemia

6533b862fe1ef96bd12c63c5

RESEARCH PRODUCT

Therapeutic afucosylated monoclonal antibody and bispecific T-cell engagers for T-cell acute lymphoblastic leukemia

Pierpaolo Correale Andrea Ghelli Luserna Di Rorà Francesco Conforti Gaetanina Golino Caterina Riillo Andrea Biondi Massimo Martino Giada Juli Francesca Scionti Pierfrancesco Tassone Daniele Caracciolo Emanuela Altomare Gabriella Talarico Eugénie Duroyon Eugénie Duroyon Beatrice Belmonte Nicoletta Polerà Ludovic Lhermitte Ludovic Lhermitte Chiara Buracchi Marco Rossi Vahid Asnafi Vahid Asnafi Andrea Ballerini Katia Grillone Simona Sestito Markus Hildinger Greta Alampi Ciro Botta Maria Eugenia Gallo Cantafio Maria Teresa Di Martino Anna Maria Ferrari Antonio Giordano Mariamena Arbitrio Pierosandro Tagliaferri Licia Pensabene Alessandro Gulino Daniela Concolino Giovanni Martinelli Michelangelo Iannone Claudio Tripodo Giuseppe Gaipa

subject

Cytotoxicity Immunologic Cancer Research 2434 T-Lymphocytes Mice SCID afucosylated monoclonal antibody Lymphocyte Activation Precursor T-Cell Lymphoblastic Leukemia-Lymphoma Epitopes Jurkat Cells Antineoplastic Agents Immunological Antibody Specificity Mice Inbred NOD antigens Antibodies Bispecific Tumor Microenvironment Immunology and Allergy antibodies hematologic neoplasms 1506 RC254-282 Antibody-dependent cell-mediated cytotoxicity Leukosialin bispecific T-cell engagers medicine.diagnostic_test biology hematological malignancie Neoplasms. Tumors. Oncology. Including cancer and carcinogens medicine.anatomical_structure antibodie Oncology translational medical research Molecular Medicine Immunohistochemistry Female immunotherapy Antibody T-ALL T-cell engagers T-cell acute lymphoblastic leukemia medicine.drug_class T cell Immunology Settore MED/08 - Anatomia Patologica Monoclonal antibody Antibodies Monoclonal Humanized Flow cytometry T Acute Lymphoblastic Leukemia antigen Antigen Phagocytosis medicine Animals Humans hematological malignancies Cell Proliferation Pharmacology T-cell engager business.industry hematological malignancies; antibodies; antigens; hematologic neoplasms; immunotherapy; neoplasm; T-ALL; T-cell engagers; translational medical research; translational research Basic Tumor Immunology Xenograft Model Antitumor Assays translational research Cancer research biology.protein neoplasm business hematologic neoplasm neoplasm

description

BackgroundT-cell acute lymphoblastic leukemia (T-ALL) is an aggressive disease with a poor cure rate for relapsed/resistant patients. Due to the lack of T-cell restricted targetable antigens, effective immune-therapeutics are not presently available and the treatment of chemo-refractory T-ALL is still an unmet clinical need. To develop novel immune-therapy for T-ALL, we generated an afucosylated monoclonal antibody (mAb) (ahuUMG1) and two different bispecific T-cell engagers (BTCEs) against UMG1, a unique CD43-epitope highly and selectively expressed by T-ALL cells from pediatric and adult patients.MethodsUMG1 expression was assessed by immunohistochemistry (IHC) on a wide panel of normal tissue microarrays (TMAs), and by flow cytometry on healthy peripheral blood/bone marrow-derived cells, on 10 different T-ALL cell lines, and on 110 T-ALL primary patient-derived cells. CD43-UMG1 binding site was defined through a peptide microarray scanning. ahuUMG1 was generated by Genetic Glyco-Engineering technology from a novel humanized mAb directed against UMG1 (huUMG1). BTCEs were generated as IgG1-(scFv)2 constructs with bivalent (2+2) or monovalent (2+1) CD3ε arms. Antibody dependent cellular cytotoxicity (ADCC), antibody dependent cellular phagocytosis (ADCP) and redirected T-cell cytotoxicity assays were analysed by flow cytometry. In vivo antitumor activity of ahUMG1 and UMG1-BTCEs was investigated in NSG mice against subcutaneous and orthotopic xenografts of human T-ALL.ResultsAmong 110 T-ALL patient-derived samples, 53 (48.1%) stained positive (24% of TI/TII, 82% of TIII and 42.8% of TIV). Importantly, no expression of UMG1-epitope was found in normal tissues/cells, excluding cortical thymocytes and a minority (<5%) of peripheral blood T lymphocytes. ahUMG1 induced strong ADCC and ADCP on T-ALL cells in vitro, which translated in antitumor activity in vivo and significantly extended survival of treated mice. Both UMG1-BTCEs demonstrated highly effective killing activity against T-ALL cells in vitro. We demonstrated that this effect was specifically exerted by engaged activated T cells. Moreover, UMG1-BTCEs effectively antagonized tumor growth at concentrations >2 log lower as compared with ahuUMG1, with significant mice survival advantage in different T-ALL models in vivo.ConclusionAltogether our findings, including the safe UMG1-epitope expression profile, provide a framework for the clinical development of these innovative immune-therapeutics for this still orphan disease.

year	journal	country	edition	language
2021-02-01

10.1136/jitc-2020-002026 https://dx.doi.org/10.1136/jitc-2020-002026