Autocrine-based selection of ligands for personalized CAR-T therapy of lymphoma.
Alexey V StepanovOleg V MarkovIvan V ChernikovDaniil V GladkikhHongkai ZhangTeresa JonesAlexandra V Sen'kovaElena L ChernolovskayaMarina A ZenkovaRoman S KalininMaria P RubtsovaAlexander N MeleshkoDmitry D GenkinAlexey A BelogurovJia XieAlexander G GabibovRichard A LernerPublished in: Science advances (2018)
We report the development of a novel platform to enhance the efficacy and safety of follicular lymphoma (FL) treatment. Since lymphoma is a clonal malignancy of a diversity system, every tumor has a different antibody on its cell surface. Combinatorial autocrine-based selection is used to rapidly identify specific ligands for these B cell receptors on the surface of FL tumor cells. The selected ligands are used in a chimeric antigen receptor T cell (CAR-T) format for redirection of human cytotoxic T lymphocytes. Essentially, the format is the inverse of the usual CAR-T protocol. Instead of being a guide molecule, the antibody itself is the target. Thus, these studies raise the possibility of personalized treatment of lymphomas using a private antibody binding ligand that can be obtained in a few weeks.