Abstract

This proposal is a competitive renewal for a Program grant whose purpose is to develop effective therapy for incurable B cell malignancies and breast adenocarcinoma using radiolabeled antibodies. Durable clinical responses have been achieved in the majority of 58 patients with B cell malignancies, primarily NHL, that were treated with Lym-1 and 20 patients with breast adenocarcinoma using primarily Chimeric L6 antibody. All of these patients were resistant to standard therapy. chimeric L6 showed profound biological activity that may have enhanced the radiation effect in the patients, but therapy was sometimes interrupted by an antiglobulin response. The efficacy of these radiolabeled antibodies is remarkable when one considers that they were used in isolation, and improvements could lead to cure of incurable disease. Enhancement strategies to improve the therapeutic index including various radionuclides and radiochemistries for conjugation, fractionation of therapy, agents to increase delivery to the tumor, immunoabsorption to decrease radiation to normal tissues, colony stimulating factors and stem cell marrow reconstitution were found to have merit. Of these factors we have chosen to focus on the radionuclide and radiochemistry to increase radiation to the malignancy, Interleukin-2 to increase tumor uptake and radiation, and stem cell marrow reconstitution to extend the maximum tolerated dose. Because state of the art macrocyclic chelates are available through Project 4, Project 1 proposes a Phase II trial of 67Cu-BAT-Lym-1 and 90Y- BAD-ChL6 with stem cell marrow reconstitution. Cyclosporin A will be used in Project to prevent antiglobulin response. The therapeutic index of 67 Cu-BAT-Lym-1 and 90Y-BAD-ChL6 is several times that of the corresponding 131I antibody because of tumor retention. Interleukin-2 is to be used to enhance tumor uptake in Project 1 and, if effective, will be used in Project 2. Similarly, strategies found to be effective in Project 2 will be added to the trials in Project 1. In addition to the development of macrocycles for 67 Cu, 111In and 90Y, and methods for site specific attachment to specific antibodies residues, Lym-1 has been sequenced and a single chain antibody prepared by genetic engineering in Project 4. this proposal includes generation of additional engineered constructs and their exploration as therapeutic agents. Strengths of the Program include an interdisciplinary group that has established their commitment and cohesiveness, and the clinical relevance of the proposed therapeutic agents. Projects 1 and 2 benefit from new constructs and radiochemistry generated in Project 4 and from opportunities for comparisons of the biology of breast cancer and B cell malignancies. Project 4 benefits from feedback of biologic and clinical information generated in Projects 1 and 2 for new constructs and radiochemistry. The information form this Program is relevant to the use of other conjugated and unconjugated antibodies.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
3P01CA047829-11S2
Application #
6145982
Study Section
Special Emphasis Panel (SRC (18))
Program Officer
Hecht, Toby T
Project Start
1988-07-15
Project End
1999-09-29
Budget Start
1998-05-01
Budget End
1999-09-29
Support Year
11
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of California Davis
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
094878337
City
Davis
State
CA
Country
United States
Zip Code
95618

  Publications

Schellinger, Joan G; Kudupudi, Avinash; Natarajan, Arutselvan et al. (2012) A general chemical synthesis platform for crosslinking multivalent single chain variable fragments. Org Biomol Chem 10:1521-6
Saludes, Jonel P; Natarajan, Arutselvan; DeNardo, Sally J et al. (2010) The remarkable stability of chimeric, sialic acid-derived alpha/delta-peptides in human blood plasma. Chem Biol Drug Des 75:455-60
Kumaresan, Pappanaicken R; Luo, Juntao; Lam, Kit S (2009) On-demand cleavable linkers for radioimmunotherapy. Methods Mol Biol 539:191-211
DeNardo, G L; Mirick, G R; Hok, S et al. (2009) Molecular specific and cell selective cytotoxicity induced by a novel synthetic HLA-DR antibody mimic for lymphoma and leukemia. Int J Oncol 34:511-6
Balhorn, Rod; Hok, Saphon; DeNardo, Sally et al. (2009) Hexa-arginine enhanced uptake and residualization of selective high affinity ligands by Raji lymphoma cells. Mol Cancer 8:25
Sulchek, Todd; Friddle, Raymond; Ratto, Timothy et al. (2009) Single-molecule approach to understanding multivalent binding kinetics. Ann N Y Acad Sci 1161:74-82
DeNardo, Gerald L; Natarajan, Arutselvan; Hok, Saphon et al. (2008) Nanomolecular HLA-DR10 antibody mimics: A potent system for molecular targeted therapy and imaging. Cancer Biother Radiopharm 23:783-96
Natarajan, Arutselvan; Xiong, Cheng-Yi; Gruettner, Cordula et al. (2008) Development of multivalent radioimmunonanoparticles for cancer imaging and therapy. Cancer Biother Radiopharm 23:82-91
Lehmann, Joerg; Natarajan, Arutselvan; Denardo, Gerald L et al. (2008) Short communication: nanoparticle thermotherapy and external beam radiation therapy for human prostate cancer cells. Cancer Biother Radiopharm 23:265-71
Kumaresan, Pappanaicken R; Luo, Juntao; Song, Aimin et al. (2008) Evaluation of ketone-oxime method for developing therapeutic on-demand cleavable immunoconjugates. Bioconjug Chem 19:1313-8

Showing the most recent 10 out of 187 publications