The National Cancer Institute seeks parties to license human monoclonal antibodies and immunoconjugates and co-develop, evaluate, and/or commercialize large-scale antibody production and hepatocellular carcinoma (HCC) xenograft mouse models. An advantage of these monoclonal antibodies as a potential therapeutic is their specificity, which would reduce deleterious side-effects. HCC is the most common form of liver cancer, and is among the more deadly cancers in the world. There is a need for new treatments that can be successfully applied to a large population of patients.
Glypican-3 (GPC3) is a cell surface protein that is preferentially expressed on HCC cells.Researchers at the NCI Laboratory of Molecular Biology demonstrated that a soluble form of GPC3 that is incapable of cell signaling can inhibit the growth of HCC cells. This suggests that blocking GPC3 signaling could serve as a therapeutic approach for treating HCC.
This opportunity to collaborate with NCI researchers or license the technology covers monoclonal antibodies (mAb) against GPC3 and their use, either by themselves or as the targeting domain for an immunotoxin, antibody drug conjugate (ADC) or chimeric antigen receptors (CARs), for the treatment of GPC3-expressing cancers such as HCC. Specifically, this involves two distinct monoclonal antibodies to GPC3 generated by the researchers. The first monoclonal antibody (HN3) binds to a conformational epitope on the cell surface domain of GPC3. The second monoclonal antibody (HS20) binds specifically to heparin sulfate chains on GPC3. By blocking GPC3 function, these antibodies can inhibit the growth of HCC cells, thereby decreasing the ability of tumors to grow and metastasize. Furthermore, by using the antibodies to target a toxin to only those cells that express GPC3, cancer cells can be eliminated while healthy, essential cells remain unharmed. Thus, monoclonal antibodies to GPC3 (and corresponding immunotoxins) represent a novel therapeutic candidate for treatment of HCC, as well as other cancers associated with the differential expression of GPC3.