Regressions and cures of melanoma xenografts following treatment with monoclonal antibody β-lactamase conjugates in combination with anticancer prodrugs

Cephalosporin doxorubicin (C-Dox) and 7-(4-carboxybutanamido)-cephalosporin mustard (CCM) are prodrugs that are catalytically converted by Enterobacter cloacae beta-lactamase (bL) to the active anticancer agents doxorubicin and phenylenediamine mustard, respectively. Both prodrugs were less cytotoxi...

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Bibliographic Details
Published in:Cancer research (Chicago, Ill.) Ill.), 1995-08, Vol.55 (16), p.3558-3563
Main Authors: KERR, D. E, SCHREIBER, G. J, VRUDHULA, V. M, SVENSSON, H. P, HELLSTRÖM, I, HELLSTRÖM, K. E, SENTER, P. D
Format: Article
Language:English
Subjects:
Animals
Antibodies, Monoclonal - therapeutic use
Antigens, Neoplasm
Antineoplastic agents
beta-Lactamases - administration & dosage
Biological and medical sciences
Cephalosporins
Chemotherapy
Doxorubicin - administration & dosage
Female
Humans
Immunoconjugates
Medical sciences
Melanoma - drug therapy
Melanoma-Specific Antigens
Mice
Mice, Nude
Neoplasm Proteins - immunology
Neoplasm Transplantation
Nitrogen Mustard Compounds - administration & dosage
Pharmacology. Drug treatments
Prodrugs - administration & dosage
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Summary:Cephalosporin doxorubicin (C-Dox) and 7-(4-carboxybutanamido)-cephalosporin mustard (CCM) are prodrugs that are catalytically converted by Enterobacter cloacae beta-lactamase (bL) to the active anticancer agents doxorubicin and phenylenediamine mustard, respectively. Both prodrugs were less cytotoxic to the 3677 human melanoma line than their respective drugs and were activated in an immunologically specific manner by 96.5-bL, a mAb-bL conjugate that binds to 3677 cell surface antigens. Similar results were obtained using the CCM prodrug on SK-MEL 28 human melanoma cells. Experiments in mice with established s.c. 3677 tumors demonstrated that although no tumors were cured in mice receiving the 96.5-bL/C-Dox combination, the activities were greater than those obtained from systemic doxorubicin treatment or from administration of the nonbinding conjugate P1.17-bL in combination with C-Dox. In contrast, when CCM was used as a prodrug, cures of established 3677 tumors were obtained in 80% of the 96.5-bL treated animals. This combination was also able to induce regressions of large 3677 tumor masses (800 mm3) without any apparent toxic side effects. We conclude that 96.5-bL in combination with C-Dox or CCM has greater antitumor activity than systemic treatment with the corresponding drugs and that CCM is a more effective prodrug than C-Dox for treating human 3677 melanoma xenografts.
ISSN:0008-5472
1538-7445