AlloCAR T™

Our process for manufacturing our off-the-shelf AlloCAR T™ products first involves collecting white blood cells from healthy donors. The collected cells are then screened, tested, and shipped to a central processing facility, where the T cells are isolated and stored frozen, creating an inventory of healthy donor cells for manufacturing. This means that a larger portion of eligible patients, including those who are critically ill and have T cells that are difficult to harvest or expand, can potentially receive treatment, without having to undergo leukapheresis (a laboratory procedure in which a patient’s white blood cells are separated and the remaining blood cells and plasma are returned to the patient).

Next, the T cells are engineered to express CARs, which recognize certain cell surface proteins that are expressed in hematologic or solid tumors. ALLO-501A, our lead investigational product which utilizes our Alloy manufacturing process, targets CD19 for the treatment of relapsed or refractory (r/r) Large B Cell Lymphoma (LBCL). Our next two most advanced products are ALLO-715, which targets BCMA for the treatment of r/r Multiple Myeloma and ALLO-316 which targets CD70 and is currently being investigated for the treatment of clear cell renal cell carcinoma. These are just the first in a line of AlloCAR T™ products we plan to develop.

The next step in the process involves gene editing to reduce the risk of graft versus host disease (GvHD) and allogeneic rejection. A T cell receptor gene is knocked out to avoid GvHD. The CD52 gene is knocked out to render the CAR T product resistant to anti-CD52 antibody treatment. ALLO-647, our investigational anti-CD52 monoclonal antibody, can therefore be used to suppress the host immune system and potentially allow the AlloCAR T™ to stay engrafted to achieve full therapeutic impact.

The engineered T cells then undergo a purification step and are ultimately cryopreserved in vials for on demand delivery to patients.