Abstract

The central hypothesis of this Specialized Center of Research on Malignant Human Gliomas and Medulloblastoma is that there are qualitatively and quantitatively distinctive molecular expression patterns associated with these brain neoplasms that are different from those of normal adult central nervous system and other body organs and tissues; and that these molecular differences may be biologically important. Moreover, we hypothesize and have preliminary data to support the idea, that monoclonal antibodies that are monospecific or that react with restricted epitopes on these brain tumor-associated molecules can be prepared (Project Ia), and that they can be exploited diagnostically and therapeutically against gliomas and medulloblastoma, first in human xenograft systems (Projects IIb, IIc) and ultimately in human clinical trials (Project III). The purpose of Project Ia1 is to provide state-of-the-art support in ganglioside and carbohydrate biochemistry for the monoclonal antibody development and characterization against gangliosides in Project Ia and to identify any antibodies generated in Projects Ib and Ic that react with carbohydrate epitopes, expressed both on gangliosides, glycolipids, and glycoproteins. Our project will first identify cell lines, xenografts, and glioma and medulloblastoma biopsies that contain qualitatively or quantitatively distinctive ganglioside molecules and purify and structurally characterize these molecules. This will provide both cellular and molecular reagents for immunization and monoclonal antibody selection. We will then assist in epitope mapping and identify antibodies of most restricted specificity. These well- characterized monoclonal antibodies will then be used to identify any new tumor-associated gangliosides cross-reactive with these antibodies through shared epitopes.
Our specific aims are: a) To examine gangliosides from various areas of the human nervous system, peripheral nerves, glioma cell lines, carcinomas of the gastrointestinal tract and meconium, characterize their chemical structure and to make a quantitative determination of their distribution. b) To isolate pure gangliosides from the sources which the quantitative determinations have shown to be optimal from a quantitative and qualitative point of view. c) To develop quantitative analytical methods, including thin-layer chromatography, mass-spec-trometry, permethylation, enzymatic degradation and immunoaffinity determinations, for the characterization of the gangliosides, and for the determination of the antigenic determinants (epitope specificity) of monoclonal antibodies directed against gangliosides.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Specialized Center (P50)
Project #
5P50NS020023-07
Application #
3882298
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
7
Fiscal Year
1990
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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