Herceptin-geldanamycin Immunoconjugates: Pharmacokinetics, Biodistribution, and Enhanced Antitumor Activity

Overview

Journal Cancer Res

Specialty Oncology

Date 2004 Feb 20

PMID 14973048

Citations 19

Authors

Raya Mandler

Hisataka Kobayashi

Ella R Hinson

Martin W Brechbiel

Thomas A Waldmann

Affiliations

Soon will be listed here.

Abstract

The efficacy of monoclonal antibodies (mAbs) as single agents in targeted cancer therapy has proven to be limited. Arming mAbs with a potent toxic drug could enhance their activity. Here we report that conjugating geldanamycin (GA) to the anti-HER2 mAb Herceptin improved the activity of Herceptin. The IC(50)s of the immunoconjugate H-GA were 10-200-fold lower than that of Herceptin in antiproliferative assays, depending on the cell line. The H-GA mode of action involved HER2 degradation, which was partially lactacystin sensitive and thus proteasome dependent. The linkage between GA and Herceptin remained stable in the circulation, as suggested by the pharmacokinetics of Herceptin and conjugated GA, which were almost identical and significantly different from that of free GA. Tumor uptake of Herceptin and H-GA were similar (52 +/- 7 and 43 +/- 7% of the initial injected dose per gram tissue, respectively; P = 0.077), indicating no apparent damage attributable to conjugation. Therapy experiments in xenograft-bearing mice consisted of weekly i.p. doses, 4 mg/kg for 4 months. H-GA showed a greater antitumor effect than Herceptin because it induced tumor regression in 69% of the recipients compared with 7% by Herceptin alone. Median survival time was 145 days as opposed to 78 days, and 31% of the recipients remained tumor free 2 months after therapy was terminated versus 0% in the Herceptin group. Enhancement of Herceptin activity could be of significant clinical value. In addition, the chemical linkage and the considerations in therapeutic regimen described here could be applied to other immunoconjugates for targeted therapy of a broad spectrum of cancers.

Citing Articles

Payload diversification: a key step in the development of antibody-drug conjugates.

Conilh L, Sadilkova L, Viricel W, Dumontet C J Hematol Oncol. 2023; 16(1):3.

PMID: 36650546 PMC: 9847035. DOI: 10.1186/s13045-022-01397-y.

Monitoring In Vivo Performances of Protein-Drug Conjugates Using Site-Selective Dual Radiolabeling and Ex Vivo Digital Imaging.

Cahuzac H, Sallustrau A, Malgorn C, Beau F, Barbe P, Babin V J Med Chem. 2022; 65(9):6953-6968.

PMID: 35500280 PMC: 9833330. DOI: 10.1021/acs.jmedchem.2c00401.

Targeted delivery of heat shock protein 90 inhibitors prevents growth of HER2-positive tumor.

Lim K, Lee D, Han S, Bull D, Won Y Biomaterials. 2021; 273:120817.

PMID: 33894402 PMC: 8130452. DOI: 10.1016/j.biomaterials.2021.120817.

Analytical Methods for the Detection and Quantification of ADCs in Biological Matrices.

Cahuzac H, Devel L Pharmaceuticals (Basel). 2020; 13(12).

PMID: 33327644 PMC: 7765153. DOI: 10.3390/ph13120462.

Current LC-MS-based strategies for characterization and quantification of antibody-drug conjugates.

Zhu X, Huo S, Xue C, An B, Qu J J Pharm Anal. 2020; 10(3):209-220.

PMID: 32612867 PMC: 7322744. DOI: 10.1016/j.jpha.2020.05.008.