Antibody-drug conjugates have transformed the treatment of cancer, yet their clinical utility can be limited by suboptimal tumor penetration, complex manufacturing, and safety concerns. Replacing antibodies with low-molecular-weight ligands enables the generation of small molecule-drug conjugates with enhanced tumor-targeting performance. Here, we report the results of a proof-of-concept study in canine cancer patients with OncoFAP glidotin, a small molecule-based targeted cytotoxic directed against Fibroblast Activation Protein. OncoFAP glidotin was evaluated in a dose-escalation trial in eight client-owned pet dogs bearing spontaneous FAP-positive tumors. The agent displayed an excellent safety profile, with no severe treatment-related adverse events. Six (75%) patients responded to the therapy. A tumor volume reduction of up to ∼88% in target lesions was observed on whole-body computed tomography, after only 4 weeks of treatment. These findings support further translational development activities of OncoFAP glidotin for both human and veterinary cancer patients.
A Small-Molecule Drug Conjugate Targeting FAP Exhibits Potent Activity in Dogs with Spontaneous Tumors / A. Galbiati, P. Roccabianca, S. Dell'Aere, M. Bocci, L. Auletta, R. Ferrari, A. Ubiali, E.M. Gariboldi, E. Marsala, P. Faviana, F. Bartoli, B. Zoanni, E. Gilardoni, M. Longo, D. Neri, D. Stefanello, S. Cazzamalli. - In: JOURNAL OF MEDICINAL CHEMISTRY. - ISSN 0022-2623. - (2026 May 16), pp. 1-13. [Epub ahead of print] [10.1021/acs.jmedchem.6c00682]
A Small-Molecule Drug Conjugate Targeting FAP Exhibits Potent Activity in Dogs with Spontaneous Tumors
A. GalbiatiCo-primo
;P. RoccabiancaCo-primo
;S. Dell'AereSecondo
;L. Auletta;R. Ferrari;A. Ubiali;E.M. Gariboldi;E. Marsala;B. Zoanni;E. Gilardoni;M. Longo;D. StefanelloCo-ultimo
;
2026
Abstract
Antibody-drug conjugates have transformed the treatment of cancer, yet their clinical utility can be limited by suboptimal tumor penetration, complex manufacturing, and safety concerns. Replacing antibodies with low-molecular-weight ligands enables the generation of small molecule-drug conjugates with enhanced tumor-targeting performance. Here, we report the results of a proof-of-concept study in canine cancer patients with OncoFAP glidotin, a small molecule-based targeted cytotoxic directed against Fibroblast Activation Protein. OncoFAP glidotin was evaluated in a dose-escalation trial in eight client-owned pet dogs bearing spontaneous FAP-positive tumors. The agent displayed an excellent safety profile, with no severe treatment-related adverse events. Six (75%) patients responded to the therapy. A tumor volume reduction of up to ∼88% in target lesions was observed on whole-body computed tomography, after only 4 weeks of treatment. These findings support further translational development activities of OncoFAP glidotin for both human and veterinary cancer patients.
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