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Article type: Research Article
Authors: Gauny, Stacey S. | Andya, James | Thomson, James | Young, John D. | Winkelhake, Jeffrey L.;
Affiliations: Departments of Pharmacology and Process and Product Development, Cetus Corporation, Emeryville, CA, USA
Note: [] Address reprint requests to Dr. J. Winkelhake at his present address: Cytel Corporation, 11099 N. Torrey Pines Road, La Jolla, CA 92037, USA.
Abstract: Pharmacologic studies of human immunoglobulins (IgM) in non-primate animal models, whether directed toward efficacy or toxicity, rely on pharmacokinetic parameters to achieve optimal doses and schedules. In rodents, human IgMs have an effective circulatory half-life of 11 h and a plasma clearance rate of 0.044 ml/min/kg. Studies of a new group of human monoclonal antibodies (hMAb) specific for Gram-negative bacteria and endotoxin revealed an IgM molecule, hMAb-10058, which, when purified from tissue culture medium, exhibited a suprisingly short circulatory lifetime in rodents. Investigations into possible explanations for this short circulatory half-life resulted in the development of a simple and efficient method for producing hMAbs in the immunodeficient NIH-3 mouse (bg × nu × XID). This method of production of hMAb-10058 had dramatic effects on its half-life. Whereas hMAb-10058 produced in serum-free, defined medium had a clearance rate of 14.4 ml/min/kg and an effective half-life of 0.12 h, the same hMAb-10058 raised in mouse ascites had a decreased clearance rate of 0.092 ml/min/kg and an increased effective half-life of 12 h. This 100-fold enhancement of the hMAb's half-life was not affected by the purification process. Some potential molecular structures involved in the circulatory half-life of this hMAb are discussed.
Keywords: immunoglobulin (IgM), human monoclonal antibody (hMAb), pharmacokinetics, clearance rate, NIH-3 mouse, ascites
DOI: 10.3233/HAB-1991-2105
Journal: Human Antibodies, vol. 2, no. 1, pp. 33-38, 1991
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