T-cell bispecific antibodies (TCBs) crosslink tumor and T-cells to induce tumor cell killing. While TCBs are very potent, on-target off-tumor toxicity remains a challenge when selecting targets. Here, we describe a protease-activated anti-folate receptor 1 TCB (Prot-FOLR1-TCB) equipped with an anti-idiotypic anti-CD3 mask connected to the anti-CD3 Fab through a tumor protease-cleavable linker. The potency of this Prot- FOLR1-TCB is recovered following protease-cleavage of the linker releasing the anti-idiotypic anti-CD3 scFv. In vivo, the Prot-FOLR1-TCB mediates antitumor efficacy comparable to the parental FOLR1-TCB whereas a noncleavable control Prot-FOLR1-TCB is inactive. In contrast, killing of bronchial epithelial and renal cortical cells with low FOLR1 expression is prevented compared to the parental FOLR1-TCB. The findings are confirmed for mesothelin as alternative tumor antigen. Thus, masking the anti-CD3 Fab fragment with an anti-idiotypic mask and cleavage of the mask by tumor-specific proteases can be applied to enhance specificity and safety of TCBs.
- Geiger, M.
- Stubenrauch, K. G.
- Sam, J.
- Richter, W. F.
- Jordan, G.
- Eckmann, J.
- Hage, C.
- Nicolini, V.
- Freimoser-Grundschober, A.
- Ritter, M.
- Lauer, M. E.
- Stahlberg, H.
- Ringler, P.
- Patel, J.
- Sullivan, E.
- Grau-Richards, S.
- Endres, S.
- Kobold, S.
- Umana, P.
- Brunker, P.
- Klein, C.
Keywords
- Animals
- Antibodies, Bispecific/chemistry/*immunology/*metabolism/therapeutic use
- CD3 Complex/*immunology
- Cell Line, Tumor
- Folate Receptor 1/*immunology
- GPI-Linked Proteins/immunology
- Humans
- Immunotherapy
- Lymphocyte Activation/drug effects
- Mice
- Molecular Targeted Therapy
- Peptide Hydrolases/*metabolism
- T-Lymphocytes/*immunology
- Xenograft Model Antitumor Assays
