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A conformation-specific ON-switch for controlling CAR T cells with an orally available drug.


ABSTRACT: Molecular ON-switches in which a chemical compound induces protein-protein interactions can allow cellular function to be controlled with small molecules. ON-switches based on clinically applicable compounds and human proteins would greatly facilitate their therapeutic use. Here, we developed an ON-switch system in which the human retinol binding protein 4 (hRBP4) of the lipocalin family interacts with engineered hRBP4 binders in a small molecule-dependent manner. Two different protein scaffolds were engineered to bind to hRBP4 when loaded with the orally available small molecule A1120. The crystal structure of an assembled ON-switch shows that the engineered binder specifically recognizes the conformational changes induced by A1120 in two loop regions of hRBP4. We demonstrate that this conformation-specific ON-switch is highly dependent on the presence of A1120, as demonstrated by an ?500-fold increase in affinity upon addition of the small molecule drug. Furthermore, the ON-switch successfully regulated the activity of primary human CAR T cells in vitro. We anticipate that lipocalin-based ON-switches have the potential to be broadly applied for the safe pharmacological control of cellular therapeutics.

SUBMITTER: Zajc CU 

PROVIDER: S-EPMC7334647 | biostudies-literature | 2020 Jun

REPOSITORIES: biostudies-literature

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A conformation-specific ON-switch for controlling CAR T cells with an orally available drug.

Zajc Charlotte U CU   Dobersberger Markus M   Schaffner Irene I   Mlynek Georg G   Pühringer Dominic D   Salzer Benjamin B   Djinović-Carugo Kristina K   Steinberger Peter P   De Sousa Linhares Annika A   Yang Nicole J NJ   Obinger Christian C   Holter Wolfgang W   Traxlmayr Michael W MW   Lehner Manfred M  

Proceedings of the National Academy of Sciences of the United States of America 20200617 26


Molecular ON-switches in which a chemical compound induces protein-protein interactions can allow cellular function to be controlled with small molecules. ON-switches based on clinically applicable compounds and human proteins would greatly facilitate their therapeutic use. Here, we developed an ON-switch system in which the human retinol binding protein 4 (hRBP4) of the lipocalin family interacts with engineered hRBP4 binders in a small molecule-dependent manner. Two different protein scaffolds  ...[more]

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