SBIR-STTR Award

Improving Ovarian Cancer Treatment by Targeting a Novel Epitope of MUC16
Award last edited on: 4/2/19

Sponsored Program
STTR
Awarding Agency
NIH : NCI
Total Award Amount
$190,591
Award Phase
1
Solicitation Topic Code
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Principal Investigator
Rachel Hannah Kravitz

Company Information

NeoClone LLC (AKA: NeoClone Biotechnology International LLC)

1202 Ann Street
Madison, WI 53713
   (608) 260-8190
   info@neoclone.com
   www.neoclone.com

Research Institution

University of Wisconsin

Phase I

Contract Number: 1R41CA132520-01A2
Start Date: 6/1/09    Completed: 5/31/10
Phase I year
2009
Phase I Amount
$190,591
The CA125 antigen is a well known marker for monitoring the recurrence and progression of epithelial ovarian cancer. It is now clear that this antigen is a repeating peptide epitope that is present within the protein backbone of the recently identified mucin MUC16. This mucin is expressed on the surface of ovarian tumor cells (hereafter referred to as csMUC16). A specific proteolytic event results in shedding of MUC16 (hereafter referred to as sMUC16). The sMUC16 can be detected in the serum and is also present in copious amounts in the peritoneal fluid of ovarian cancer patients. The csMUC16 binds to mesothelin, a glycoprotein present on the mesothelial cells and this interaction facilitates peritoneal metastasis of ovarian tumor cells. The sMUC16 present in the peritoneal fluid is unable to inhibit the interaction between csMUC16 and mesothelin. These and other observations suggest specific differences in the biochemical composition of sMUC16 and csMUC16. Because of these structural differences, antibodies that show a preference for csMUC16 isoforms over sMUC16 may be utilized as immunotherapeutic agents against ovarian tumors. Such reagents would have the advantage of targeting the ovarian tumor cells in the presence of high amounts of sMUC16 that is shed in the peritoneal environment. Current immunotherapeutic approaches targeting MUC16 are competed by sMUC16 and thus are limited in their efficacy. The first specific aim of this Phase I STTR proposal is to develop antibodies that preferentially recognize csMUC16. Such specific antibodies will be generated using multiple tolerization immunization approaches. The ABL- MYC technology developed by Neoclone will help us generate an extensive panel of csMUC16 specific antibodies using several different tolerization approaches in a relatively short time period. In the second specific aim, these antibodies will be further characterized for specificity and the relative affinities of the generated antibodies against csMUC16 and sMUC16 will be calculated using Surface Plasmon Resonance and flow cytometry based protocols. The antibodies will be functionally screened for their ability to interrupt the mesothelin interaction. These anti-csMUC16 specific antibodies can then be conjugated with toxins, radiolabels and other agents, or humanized and used as therapeutic agents against ovarian tumors. The therapeutic utility of the antibodies generated will be investigated in the Phase II of this STTR proposal.

Public Health Relevance:
Because of the late stage of diagnosis and high rate of recurrence, ovarian cancer is a particularly deadly disease. We propose to develop monoclonal antibodies that will identify unique epitopes specific for a mucin (MUC16) that is highly expressed on ovarian tumors. These antibodies will be extremely useful materials for creation of therapeutic agents that can efficiently target and cytolyze ovarian tumors in the peritoneum.

Public Health Relevance Statement:
Project Narrative Because of the late stage of diagnosis and high rate of recurrence, ovarian cancer is a particularly deadly disease. We propose to develop monoclonal antibodies that will identify unique epitopes specific for a mucin (MUC16) that is highly expressed on ovarian tumors. These antibodies will be extremely useful materials for creation of therapeutic agents that can efficiently target and cytolyze ovarian tumors in the peritoneum.

Project Terms:
ADCC; ATGN; Affect; Affinity; Antibodies; Antibody -dependent cell cytotoxicity; Antibody Specificity; Antibody-Dependent Cellular Cytotoxicity; Antigenic Determinants; Antigens; Ascitic Fluid; Assay; Binding; Binding (Molecular Function); Binding Determinants; Bioassay; Biochemical; Biologic Assays; Biological Assay; Blood Serum; CA-125; CA-125 Antigen; CA125; Cancer Antigen 125; Cancer Patient; Cancer Treatment; Cancer of the Ovary; Carbohydrate Antigen 125; Cell Communication; Cell Cytoxicity, Antibody-Dependent; Cell Interaction; Cell surface; Cell-to-Cell Interaction; Cells; Chemicals; Competitive Binding; Cytofluorometry, Flow; Cytolysis; Diagnosis; Disease; Disorder; ELISA; Effectiveness; Environment; Enzyme-Linked Immunosorbent Assay; Epithelial Neoplasm of the Ovary; Epithelial Tumor of the Ovary; Epithelial ovarian cancer; Epitopes; Event; Figs; Figs - dietary; Flow Cytofluorometries; Flow Cytometry; Flow Microfluorimetry; Glycans; Glycoproteins; Goals; Immune; Immune response; Immunization; Immunologic Stimulation; Immunological Stimulation; Immunostimulation; Immunotherapeutic agent; Isoforms; Lysis; Malignant Cell; Malignant Neoplasm Therapy; Malignant Neoplasm Treatment; Malignant Ovarian Neoplasm; Malignant Ovarian Tumor; Malignant Tumor of the Ovary; Malignant neoplasm of ovary; Mammals, Mice; Masks; Mesothelial Cell; Metastasis; Metastasize; Metastatic Neoplasm; Metastatic Tumor; Mice; Microfluorometry, Flow; Moab, Clinical Treatment; Molecular; Molecular Interaction; Molecular Weight; Monitor; Monitoring for Recurrence; Monoclonal Antibodies; Mucins; Mucus Glycoprotein; Murine; Mus; Neoplasm Metastasis; Outcome; Ovarian; Ovarian Epithelial Tumor; Ovarian Surface Epithelial-Stromal Tumor; Ovarian Surface-Epithelial Stromal Neoplasm; Ovarian Tumor; Ovary Neoplasms; PERNUM; Peptides; Peripheral; Peritoneal; Peritoneal Effusion; Peritoneal Fluid; Peritoneum; Phase; Polysaccharides; Process; Protein Isoforms; Proteins; Protocol; Protocols documentation; Radiolabeled; Reagent; Recurrence; Recurrent; Relative; Relative (related person); Research; STTR; Secondary Neoplasm; Secondary Tumor; Sensitization, Immunologic; Sensitization, Immunological; Serum; Small Business Technology Transfer Research; Soluble Mpf/Mesothelin-Related Protein; Specificity; Spinal Column; Spine; Staging; Surface; Surface Plasmon Resonance; System; System, LOINC Axis 4; Technology; Therapeutic; Therapeutic Agents; Time; Toxin; Tumor Cell; Tumor Cell Line; Tumor Cell Migration; Tumor of the Ovary; Vertebral column; Woman; antibody dependent cell mediated cytotoxicity; anticancer therapy; backbone; base; cancer cell; cancer metastasis; cancer therapy; disease/disorder; flow cytophotometry; gene product; host response; immunogen; immunologic preparation; immunoresponse; immunotherapeutics; improved; megakaryocyte potentiating factor; mesothelin; neoplastic cell; novel; ovarian cancer; ovarian neoplasm; preference; prevent; preventing; public health relevance; radiolabel; radiotracer; response; tumor

Phase II

Contract Number: ----------
Start Date: 00/00/00    Completed: 00/00/00
Phase II year
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Phase II Amount
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