Problem: While the 5-year relative survival rate for patients with local or regional prostate cancer is nearly 100%, the 5-year relative survival rate drops to 32% for patients with metastatic or advanced disease. These patients may initially respond to available therapies, but most patients will develop therapy resistance and succumb to disease. Solution: A CAR construct that targets specific sugar-bearing prostate cancer cells and a subset of breast cancer cells. Technology: The inventors designed a CAR construct that targets metastatic prostate cancer, based on the first structurally defined F77 sugar antigen. About 85% of metastatic prostate cancer cells express this unique antigen. This novel CAR construct exhibited exquisite specificity and efficacy in highly relevant human prostate cancer cell lines, RWPE1 and RWPE2. F77 CAR-T cells effectively killed prostate cancer cells both in vitro and in vivo models. Advantages:
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Figure 1. % Cytolysis determined through xCELLigence impedance measurement at 5:1 E:T ratio of CAR T cells and cancer cells. % Cytolysis for cancer cells was calculated after 24 h of cancer cell addition (A) PC3, (B) RWPE-1, (C) RWPE-2, and every 5 h after effector cells addition. Impedance monitoring was validated using T cells without any CAR (NTD), F77 CAR1, F77 CAR2 and control CAR effector (cells over GFP labeled target cells at E:T ratios of 5:1. Normalized Cell Index (NCI) was used to calculate % Cytolysis and plotted ± SEM. Significance of difference in activity of each CAR compared to NTD was determined using One-way ANOVA followed by Dunnett's correction for multiple comparisons. Asterisks indicate significance (** p<0.0001 and ns refers to p≥0.05). Figure 2. Treatment of mice bearing PC3 subcutaneous tumors with F77 effector cells leads to tumor regression (n=5). Intellectual Property:
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Docket: 21-9684