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. 1985 Mar;26(3):283-92.

Tumor location using F(ab')2 mu from a monoclonal IgM antibody: pharmacokinetics

  • PMID: 2857779

Tumor location using F(ab')2 mu from a monoclonal IgM antibody: pharmacokinetics

B Ballou et al. J Nucl Med. 1985 Mar.

Abstract

A monoclonal IgM antibody (anti-SSEA-1) and its divalent antigen-binding peptic fragment [F(ab')2 mu] were compared as in vivo tumor localization reagents in mouse teratocarcinomas. F(ab')2 mu is cleared more rapidly than whole antibody from the whole body, blood, and all tested organs (t1/2 for whole antibody approximately 18 hr; t1/2 for F(ab')2 mu, 12 hr). A corresponding average improvement in tumor-to-tissue ratio is observed 48 hr after injection and earlier. However, the affinity of the F(ab')2 mu for antigen is much lower, and a smaller fraction of the antibody fragment is retained in the tumor than with whole antibody. The fragment was not retained by animals bearing nonantigenic tumors.

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