1. Academic Validation
  2. Development of methotrexate alpha-peptides as prodrugs for activation by enzyme-monoclonal antibody conjugates

Development of methotrexate alpha-peptides as prodrugs for activation by enzyme-monoclonal antibody conjugates

  • Adv Enzyme Regul. 1997:37:77-92. doi: 10.1016/s0065-2571(96)00011-8.
F M Huennekens 1
Affiliations

Affiliation

  • 1 Department of Molecular and Experimental Medicine, Scripps Research Institute, La Jolla, CA 92037, USA.
Abstract

Selective delivery of lethal concentrations of drugs to tumors, allowing the latter to be eradicated without damage to other tissues, continues to be a major goal in Cancer chemotherapy. Prodrugs (i.e. drugs that have been derivatized to prevent uptake into cells or interaction with targets), activated by enzyme-monoclonal antibody conjugates positioned at tumor sites, offer promise for achieving this objective. Methotrexate alpha-peptides (derivatives in which an amino acid is linked to the alpha-carboxyl group of the glutamate moiety) are ideal prodrugs, since they are not transported into cells and can be converted to the parent drug by carboxypeptidases. The L,L-diastereomer of MTX-alpha-Phe, synthesized in good yield by treatment of the p-nitrophenyl ester of 4-amino-4-deoxy-10-methylpteroic acid with Glu-alpha-Phe, was hydrolyzed readily by Carboxypeptidase A (CP-A). Conjugate was prepared by derivatizing the Enzyme and monoclonal antibody KS1/4 with linkers containing maleimide and sulfhydryl groups, respectively; interaction of these groups to form a stable thioether bond joined the proteins. When administered in vitro to UCLA-P3 human lung adenocarcinoma cells (CA. 5 x 10(4) antibody binding sites/cell) that had been pre-treated with the conjugate (whose antibody KS1/4 is targeted to these cells), and excess conjugate removed by extensive washing, MTX-Phe (ID50 = 6.3 x 10(-8) M) approached the toxicity of MTX (ID50 = 4.5 x 10(-8) M). In the absence of conjugate, MTX-Phe was much less toxic (ID50 = 2.2 x 10(-6) M).

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