Abstract

Monoclonal antibodies have been developed and characterized that are reactive with antigens present on human gliomas, medulloblastomas and tumors that metastasize to the central nervous system. The hypothesis of this project is that these antibodies, when combined with the appropriate nuclide, could be used to deliver therapeutic levels of radiation more selectively to these tumors. Because they offer different advantages, both the beta emitter iodine-131 and the alpha emitter astatine-211 will be investigated. The beta particles of I-131 have a range in tissue of 1-2 mm, facilitating the irradiation of proximal antigen negative or poorly perfused tumor cells. The alpha particles of At-211 have a greater radio-biological effectiveness and a range of only a few cell diameters, minimizing the dose to neighboring normal brain or spinal tissues. These antibodies will be labeled with these nuclides using the ATE procedure, a method which we developed which decreases the loss of label from the antibody due to dehalogenation in vivo.
The specific aims of this project are: a) to label these monoclonal antibodies with I-131 and At-211 using the ATE method without adversely affecting the immunoreactivity and affinity constant of the antibody; b) to determine the pharmacokinetics of I-131 and At-211 labeled anti-glioma and medulloblastoma monoclonal and antibody fragments in subcutaneous and intracranial human tumor xenograft models; c) to measure the radiotoxicity in vitro of I- 131 and At-211 labeled antibodies in both antigen-positive and control human tumor cell lines; and d) to determine the therapeutic potential of I-131 and At-211 labeled anti-glioma and medulloblastoma antibodies and fragments in athymic mice and rats bearing subcutaneous and intracranial human tumor xenografts. Combinations of labeled antibodies and multiple dose regimens will also be investigated. These studies will hopefully provide the basis for clinical radiotherapeutic trials in patients with gliomas, medulloblastomas and carcinomatosis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Specialized Center (P50)
Project #
5P50NS020023-08
Application #
3861356
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
8
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Duke University
Department
Type
DUNS #
071723621
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Saraswathula, Anirudh; Reap, Elizabeth A; Choi, Bryan D et al. (2016) Serum elevation of B lymphocyte stimulator does not increase regulatory B cells in glioblastoma patients undergoing immunotherapy. Cancer Immunol Immunother 65:205-11
Slastnikova, Tatiana A; Rosenkranz, Andrey A; Zalutsky, Michael R et al. (2015) Modular nanotransporters for targeted intracellular delivery of drugs: folate receptors as potential targets. Curr Pharm Des 21:1227-38
Huang, Dong-Sheng; Wang, Zhaohui; He, Xu-Jun et al. (2015) Recurrent TERT promoter mutations identified in a large-scale study of multiple tumour types are associated with increased TERT expression and telomerase activation. Eur J Cancer 51:969-76
Mitchell, Duane A; Batich, Kristen A; Gunn, Michael D et al. (2015) Tetanus toxoid and CCL3 improve dendritic cell vaccines in mice and glioblastoma patients. Nature 519:366-9
Koumarianou, Eftychia; Slastnikova, Tatiana A; Pruszynski, Marek et al. (2014) Radiolabeling and in vitro evaluation of (67)Ga-NOTA-modular nanotransporter--a potential Auger electron emitting EGFR-targeted radiotherapeutic. Nucl Med Biol 41:441-9
Choi, Bryan D; Suryadevara, Carter M; Gedeon, Patrick C et al. (2014) Intracerebral delivery of a third generation EGFRvIII-specific chimeric antigen receptor is efficacious against human glioma. J Clin Neurosci 21:189-90
Brown, Michael C; Dobrikova, Elena Y; Dobrikov, Mikhail I et al. (2014) Oncolytic polio virotherapy of cancer. Cancer 120:3277-86
Miao, Hongsheng; Choi, Bryan D; Suryadevara, Carter M et al. (2014) EGFRvIII-specific chimeric antigen receptor T cells migrate to and kill tumor deposits infiltrating the brain parenchyma in an invasive xenograft model of glioblastoma. PLoS One 9:e94281
Killela, Patrick J; Pirozzi, Christopher J; Healy, Patrick et al. (2014) Mutations in IDH1, IDH2, and in the TERT promoter define clinically distinct subgroups of adult malignant gliomas. Oncotarget 5:1515-25
Lathia, Justin D; Li, Meizhang; Sinyuk, Maksim et al. (2014) High-throughput flow cytometry screening reveals a role for junctional adhesion molecule a as a cancer stem cell maintenance factor. Cell Rep 6:117-29

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