BR96-Dox provides a unique strategy to deliver doxorubicin to Le(Y)-expressing tumor and was well tolerated at doses of 700 mg/m(2) every 3 weeks. BR96-Dox was not associated with the typical side-effect profile of native doxorubicin and can potentially deliver high doses of doxorubicin to antigen-expressing tumors. A phase II study in doxorubicin-sensitive tumors is warranted.
Background. Previous studies in the literature have suggested that radiolabeled F(ab′)2 fragments might be superior to whole immunoglobulin G (IgG) for imaging and therapy of cancer because of their greater penetration in tumors. To test this hypothesis, the authors compared tumor and normal tissue uptake along with plasma clearance of 125I‐labeled monoclonal antibody (MoAb) IMMU‐4 whole IgG with its 131I‐labeled F(ab′)2 fragment.
Methods. Five patients with either liver metastases from colorectal cancer (n = 4) or intact primary tumors (n = 1) received a combination of 125I‐IMMU‐4 IgG (2 mCi/1 mg) plus131I‐IMMU‐4 F(ab′)2 (10 mCi/1 mg) as a single 1‐hour intravenous infusion on day 1. Serial blood samples were taken for up to 72 hours postinfusion to determine plasma clearance of each MoAb. On days 3–9, patients underwent exploratory laparotomy in which biopsies of tumor as well as normal tissues (liver, normal colon, lymph node, and blood) were obtained. Tissues were weighed and counted in a gamma counter, and the percent of injected dose per kilogram (%ID/kg) of each antibody, along with the radiolocalization index (RI), was computed (RI = %ID/kg tumor. %ID/kg normal tissue).
Results. Tumor uptake of both antibodies (2.3 ± 0.53 %ID/kg) was significantly higher than that of normal tissues (0.56 ± 0.12; P < 0.001), except for blood (2.8 ± 0.83), resulting in an RI ≥ 3. There were no significant differences in uptake (%ID/g) between F(ab′)2 and IgG (F[ab′]2 = 2.0 ± 0.57; IgG = 2.6 ± 0.94). The mean ± SD of plasma T½ was slightly shorter for F(ab′)2 (28.8 ± 7.2 hours) than for IgG (45.9 ± 16.7; P = 0.08).
Conclusion. In short, the biodistribution and pharmacokinetics of IMMU‐4 F(ab′)2 were comparable to those of IMMU‐4‐IgG. Cancer 1994; 73:850–7.
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