Abstract

The broad long-term goal of this project is to harness the physical and chemical properties of metallic elements to the diagnosis and treatment of cancer. Bifunctional chelating agents are powerful molecules tightly attaching metal ions to biological molecules. Thus the enhanced combined properties of the conjugates can probe specifically, report function, and treat living tumors.
Specific aims are to produce new anti-hapten monoclonal antibodies (MoAbs) with high affinity and specificity for the metal chelates of In, Ga, Y, and Tc; to study the biological behavior of new bifunctional monoclonal antibodies having one tumor specific binding site and the other chelate (hapten or biotin) specific; to use these new agents in a novel pretargeted immunoscintigraphy technique in which antibody and radiolabel are given separately, to lower liver and blood background and improve tumor to background ratios; to determine the optimum interval between bifunctional MoAb and radiolabeled hapten or biotin-chelate, determine the effect of """"""""chase"""""""" agents and make early images at 1 to 3 hours using Tc-99m and Ga-68 with the ultimate aim of making SPECT and PET tumor images in cancer patients;: to study new macrocyclic chelators for increased in vivo and in vivo stability and kinetic inertness to ligand exchange with In-111, Tc-99m, Ga-68, and Y-90 MoAbs; to use various metabolizable chelate-antibody linkers to increase clearance of background activity via the kidney; to carry out tumoricidal experiments using pretargeting of tumors and Y-90 chelates; to carry out clinical scintillation imaging using both PET and SPECT in human cancer patients with the most promising agents. The Methodology involves hybridoma technology using specially designed antigens, screening mice with radiolabeled antigen, tumor mouse distribution of new bifunctional antibodies with dual specificity for tumor and chelate, use of an avidin- biotin system in a pretargeted immunoscintigraphy method with 1-2 hr images using Tc-99m and Ga-68 and therapy with Y-90. These studies should provide methods for reducing background and improving the effectiveness of monoclonal antibodies in tumor imaging and therapy. These methods will provide the clinician with an """"""""instant kit"""""""" that can be labeled with readily available radionuclides economically, for easy application in todays nuclear medicine department.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA028343-13
Application #
3168094
Study Section
Diagnostic Radiology Study Section (RNM)
Project Start
1980-07-01
Project End
1994-06-30
Budget Start
1992-07-01
Budget End
1994-06-30
Support Year
13
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Type
Schools of Medicine
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Lubic, S P; Goodwin, D A; Meares, C F et al. (2001) Biodistribution and dosimetry of pretargeted monoclonal antibody 2D12.5 and Y-Janus-DOTA in BALB/c mice with KHJJ mouse adenocarcinoma. J Nucl Med 42:670-8
Goodwin, D A; Meares, C F (1999) Pretargeted peptide imaging and therapy. Cancer Biother Radiopharm 14:145-52
Goodwin, D A; Meares, C F; Osen, M (1998) Biological properties of biotin-chelate conjugates for pretargeted diagnosis and therapy with the avidin/biotin system. J Nucl Med 39:1813-8
Goodwin, D A; Meares, C F (1997) Pretargeting: general principles; October 10-12, 1996. Cancer 80:2675-80
Goodwin, D A (1995) Tumor pretargeting: almost the bottom line. J Nucl Med 36:876-9
Goodwin, D A; Meares, C F; Watanabe, N et al. (1994) Pharmacokinetics of pretargeted monoclonal antibody 2D12.5 and 88Y-Janus-2-(p-nitrobenzyl)-1,4,7,10-tetraazacyclododecanetetraacetic acid (DOTA) in BALB/c mice with KHJJ mouse adenocarcinoma: a model for 90Y radioimmunotherapy. Cancer Res 54:5937-46
Watanabe, N; Goodwin, D A; Meares, C F et al. (1994) Immunogenicity in rabbits and mice of an antibody-chelate conjugate: comparison of (S) and (R) macrocyclic enantiomers and an acyclic chelating agent. Cancer Res 54:1049-54
Goodwin, D A; Lang, E V; Atwood, J E et al. (1993) Viability and biodistribution of 68Ga MPO-labelled human platelets. Nucl Med Commun 14:1023-9
Goodwin, D A; Meares, C F; McTigue, M et al. (1992) Pretargeted immunoscintigraphy: effect of hapten valency on murine tumor uptake. J Nucl Med 33:2006-13
Marincola, F M; Drucker, B J; Keeling, C A et al. (1989) The in vivo distribution of human peripheral blood lymphocytes and lymphokine-activated killer cells adoptively transferred in human pancreatic cancer-bearing nude mice. Surgery 105:79-85

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