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

被引:15
作者
Caracciolo, Daniele [1 ]
Riillo, Caterina [1 ]
Ballerini, Andrea [2 ]
Gaipa, Giuseppe [3 ]
Lhermitte, Ludovic [4 ,5 ]
Rossi, Marco [1 ]
Botta, Cirino [6 ]
Duroyon, Eugenie [4 ,5 ]
Grillone, Katia [1 ]
Gallo Cantafio, Maria Eugenia [1 ]
Buracchi, Chiara [3 ]
Alampi, Greta [3 ]
Gulino, Alessandro [7 ]
Belmonte, Beatrice [7 ]
Conforti, Francesco [8 ]
Golino, Gaetanina [1 ]
Juli, Giada [1 ]
Altomare, Emanuela [1 ]
Polera, Nicoletta [1 ]
Scionti, Francesca [1 ]
Arbitrio, Mariamena [9 ]
Iannone, Michelangelo [9 ]
Martino, Massimo [10 ]
Correale, Pierpaolo [11 ]
Talarico, Gabriella [12 ]
Ghelli Luserna di Rora, Andrea [13 ]
Ferrari, Anna [13 ]
Concolino, Daniela [14 ]
Sestito, Simona [14 ]
Pensabene, Licia [14 ]
Giordano, Antonio [15 ]
Hildinger, Markus [16 ]
Di Martino, Maria Teresa [1 ]
Martinelli, Giovanni [13 ]
Tripodo, Claudio [7 ]
Asnafi, Vahid [4 ,5 ]
Biondi, Andrea [3 ]
Tagliaferri, Pierosandro [1 ]
Tassone, Pierfrancesco [1 ,15 ]
机构
[1] Magna Graecia Univ Catanzaro, Dept Expt & Clin Med, Catanzaro, Italy
[2] BiovelocITA Srl, Milan, Italy
[3] Univ Milano Bicocca, Osped San Gerardo, Ctr Ric M Tettamanti, Clin Pediat, Monza, Italy
[4] Univ Paris, Inst Necker Enfants Malades, Inst Natl Rech Med, U1151, Paris, France
[5] Hop Necker Enfants Malad, AP HP, Lab Oncohematol, Paris, France
[6] Annunziata Hosp, Hematol Unit, Cosenza, Italy
[7] Univ Palermo, Human Pathol Sect, Dept Hlth Sci, Tumor Immunol Unit, Palermo, Italy
[8] Annunziata Hosp, Pathol Unit, Cosenza, Italy
[9] IRIB CNR, Catanzaro, Italy
[10] Grande Osped Metropolitano Bianchi Melacrino More, Dept Hematooncol & Radiotherapy, Stem Cell Transplant Program, Clin Sect, Reggio Di Calabria, Italy
[11] Bianchi Melacrino Morelli Grand Metropolitan Hosp, Med Oncol Unit, Reggio Di Calabria, Italy
[12] Pugliese Ciaccio Hosp, Immunotransfus Serv Unit, Catanzaro, Italy
[13] Ist Sci Romagnolo Studio & Cura Tumori IRST IRCCS, Meldola, Italy
[14] Magna Graecia Univ Catanzaro, Pediat Unit, Dept Med & Surg Sci, Catanzaro, Italy
[15] Temple Univ, Coll Sci & Technol, Ctr Biotechnol, Sbarro Inst Canc Res & Mol Med, Philadelphia, PA 19122 USA
[16] Evitria, Zurich, Switzerland
关键词
hematologic neoplasms; immunotherapy; translational medical research; antibodies; antigens; neoplasm; hematological malignancies; T-ALL; T-cell engagers; translational research;
D O I
10.1136/jitc-2020-002026
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background T-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. Methods UMG1 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) CD3 epsilon 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. Results Among 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. Conclusion Altogether 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.
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页数:14
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