Distribution of Radiolabeled Human and Mouse Monoclonal IgM Antibodies in Murine Models

Distribution of Radiolabeled Human and Mouse Monoclonal IgM Antibodies in Murine Models

The distribution and kinetics of six human and one murine monoclonal IgM antibodies (MoAb) were studied in BALB/c mice. Labeling was with 111In, 75Se, and 125I. The monomers and pentamers of certain MoAbs were studied. Human distribution studies were also performed. The serum containing [111In]MoAb...

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Bibliographic Details
Published in:The Journal of nuclear medicine (1978) Vol. 29; no. 10; pp. 1688 - 1696
Main Authors: Halpern, Samuel E, Hagan, Philip L, Chen, Agnes, Birdwell, Charles R, Bartholomew, Richard M, Burnett, Karen G, David, Gary S, Poggenburg, Kenneth, Merchant, Bruce, Carlo, Dennis J
Format: Journal Article
Language:English
Published: United States Soc Nuclear Med 01-10-1988
Subjects:
Animals
Antibodies, Monoclonal
Humans
Immunoglobulin M
Indium Radioisotopes
Iodine Radioisotopes
Mice
Mice, Inbred BALB C
Selenium Radioisotopes
Tissue Distribution
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Summary:The distribution and kinetics of six human and one murine monoclonal IgM antibodies (MoAb) were studied in BALB/c mice. Labeling was with 111In, 75Se, and 125I. The monomers and pentamers of certain MoAbs were studied. Human distribution studies were also performed. The serum containing [111In]MoAb was obtained from one of the patients 24 hr after administration and injected into mice which were then killed and assayed for 111In distribution. In general, the [75Se] and [111In]MoAbs had distribution and kinetic patterns that were similar while the 125I-labeled MoAbs dehalogenated after 4 hr. Monomers and pentamers had highly similar distributions suggesting that the distribution of IgMs may be based on factors other than molecular size. The murine IgM showed a somewhat different distribution in mice than did human IgMs. Serum from the patient containing [111In]MoAb had a distribution in mice similar to that of the patient with high liver and gastrointestinal uptake. The human imaging indicates that it is possible to target tumor with human IgM MoAbs, but significant problems remain in regard to their clinical use.
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ISSN:0161-5505
1535-5667