Literature DB >> 7736688

Problems of delivery of monoclonal antibodies. Pharmaceutical and pharmacokinetic solutions.

R M Reilly1, J Sandhu, T M Alvarez-Diez, S Gallinger, J Kirsh, H Stern.   

Abstract

Monoclonal antibodies to tumour-associated antigens have great theoretical potential for the specific targeting of radioactivity and anti-neoplastic agents to tumours. The clinical success of monoclonal antibody-based cancer diagnosis and therapy depends, however, on solving a number of pharmacokinetic delivery problems. These include: (i) slow elimination of monoclonal antibodies from the blood and poor vascular permeability; (ii) low and heterogeneous tumour uptake; (iii) cross-reactivity with normal tissues; (iv) metabolism of monoclonal antibody conjugates; and (v) immunogenicity of murine forms in humans. As a result of extensive pharmaceutical and pharmacokinetic research conducted over the past 10 to 15 years, several potential solutions to these delivery problems have been identified. Blood concentrations of antibody conjugates may be reduced through regional administration, the use of antibody fragments, interventional strategies and various pre-targeting techniques. Tumour uptake may be increased through administration of higher doses, or the use of agents to increase tumour vascular permeability. Tumour retention of antibody conjugates may be improved by inhibition of metabolism, by using more stable linkage chemistry. Alternatively, normal tissue retention may be decreased through the use of metabolisable chemical linkages inserted between the antibody and conjugated moiety. Very small antigen-binding fragments and peptides that exhibit improved tumour penetration and more rapid elimination from the blood and normal tissues have been prepared by genetic engineering techniques. Chimeric (mouse/human) and human monoclonal antibodies have been developed to circumvent the problem of immunogenicity. Future research will continue to be focused on improvements in the design of monoclonal antibodies for tumour targeting, with the ultimate goal of finally uncovering the 'magic bullet' envisioned by Paul Ehrlich almost a century ago.

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Year:  1995        PMID: 7736688     DOI: 10.2165/00003088-199528020-00004

Source DB:  PubMed          Journal:  Clin Pharmacokinet        ISSN: 0312-5963            Impact factor:   6.447


  128 in total

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3.  Rapid tumor penetration of a single-chain Fv and comparison with other immunoglobulin forms.

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Journal:  Cancer Res       Date:  1992-06-15       Impact factor: 12.701

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6.  Exchange of macromolecules between plasma and peritoneal cavity in ascites tumor-bearing, normal, and serotonin-injected mice.

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Journal:  Cancer Res       Date:  1989-10-01       Impact factor: 12.701

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Journal:  Cancer Cells       Date:  1991-03

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Journal:  Cancer Res       Date:  1991-11-01       Impact factor: 12.701

9.  Intratumoral generation of 5-fluorouracil mediated by an antibody-cytosine deaminase conjugate in combination with 5-fluorocytosine.

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Journal:  Cancer Res       Date:  1994-05-15       Impact factor: 12.701

10.  Colorectal tumors: scintigraphy with In-111 anti-CEA monoclonal antibody and correlation with surgical, histopathologic, and immunohistochemical findings.

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Journal:  Radiology       Date:  1988-03       Impact factor: 11.105

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7.  Population pharmacokinetics of antifibroblast activation protein monoclonal antibody F19 in cancer patients.

Authors:  P Tanswell; P Garin-Chesa; W J Rettig; S Welt; C R Divgi; E S Casper; R D Finn; S M Larson; L J Old; A M Scott
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8.  The effect of metal-chelating polymers (MCPs) for 111In complexed via the streptavidin-biotin system to trastuzumab Fab fragments on tumor and normal tissue distribution in mice.

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9.  Anti-VEGF single-chain antibody GLAF-1 encoded by oncolytic vaccinia virus significantly enhances antitumor therapy.

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10.  Efficient production of human bivalent and trivalent anti-MUC1 Fab-scFv antibodies in Pichia pastoris.

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