Copper-67 radioimmunotherapy and growth inhibition by anti-L1-cell adhesion molecule monoclonal antibodies in a therapy model of ovarian cancer metastasis.

Karin Knogler Jürgen Grünberg Kurt Zimmermann Susan Cohrs Michael Honer Simon Ametamey Peter Altevogt Mina Fogel P August Schubiger Ilse Novak-Hofer

Clin Cancer Res

Center for Radiopharmaceutical Science, ETH-PSI-USZ, Paul Scherrer Institute, CH-5232 Villigen, Switzerland.

Published: January 2007

The study focused on the therapeutic potential of (67)Cu-labeled mutated anti-L1 monoclonal antibodies in treating ovarian cancer in mice.
Two specific mutations in the antibodies were created to enhance their ability to clear from the blood and target tumors more effectively.
Results indicated that one mutation (chCE7agl) not only provided significant tumor reduction and improved survival rates when used alone or in combination with another antibody, but also showed better biodistribution, suggesting its potential for more effective cancer treatment.

Purpose: We examined the tumor-targeting and therapeutic effects of (67)Cu-labeled single amino acid mutant forms of anti-L1 monoclonal antibody chCE7 in nude mice with orthotopically implanted SKOV3ip human ovarian carcinoma cells.

Experimental Design: For radioimmunotherapy, chCE7 antibodies with a mutation of histidine 310 to alanine (chCE7H310A) and a mutation of asparagine 297 to glutamine (chCE7agl) were generated to achieve more rapid blood clearance. Biodistributions of (67)Cu-4-(1,4,8,11-tetraazacyclotetradec-1-yl)-methyl benzoic acid tetrachloride (CPTA)-labeled mutant antibodies were measured in nude mice bearing SKOV3ip human ovarian cancer metastases. The effects of single i.v. injections of (67)Cu-chCE7agl alone on tumor reduction and survival were investigated. In addition, a combination of low-dose (67)Cu-radioimmunotherapy with unlabeled anti-L1 antibody L1-11A on survival was investigated.

Results: (67)Cu-CPTA-chCE7agl showed high (up to 49% ID/g) and persistent (up to 168 h) uptake in SKOV3ip metastases, with low levels in normal tissues. (67)Cu-CPTA-chCE7H310A revealed a shorter half-life in the blood and a lower tumor uptake and retention. A single low dose of 4 MBq of (67)Cu-chCE7agl reduced tumor growth but did not prolong survival significantly, whereas a single 10.5 MBq dose of (67)Cu-chCE7agl reduced tumor growth and prolonged survival significantly. The combination of unlabeled monoclonal antibody L1-11A with a subtherapeutic dose of (67)Cu-radioimmunotherapy also prolonged survival significantly.

Conclusion: The results show improved pharmacokinetics and biodistributions as well as the therapeutic effect of the (67)Cu-labeled single amino acid mutant chCE7agl. Therapeutic data indicate, for the first time, the feasibility of combining anti-L1-directed growth inhibition and (67)Cu-radioimmunotherapy, thereby increasing the efficiency of antibody treatment of metastatic ovarian carcinoma.

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http://dx.doi.org/10.1158/1078-0432.CCR-06-1486	DOI Listing

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