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Designer Small-Molecule Control System Based on Minocycline-Induced Disruption of Protein-Protein Interaction.

Ram JhaAlexander KinnaAlastair HotblackReyisa BughdaAnna BulekIsaac GannonTudor IlcaChristopher AllenKatarina LambAbigail DolorIan ScottFarhaan ParekhJames E SillibourneShaun CordobaShimobi OnuohaSimon ThomasMathieu FerrariMartin Pule
Published in: ACS chemical biology (2024)
A versatile, safe, and effective small-molecule control system is highly desirable for clinical cell therapy applications. Therefore, we developed a two-component small-molecule control system based on the disruption of protein-protein interactions using minocycline, an FDA-approved antibiotic with wide availability, excellent biodistribution, and low toxicity. The system comprises an anti-minocycline single-domain antibody (sdAb) and a minocycline-displaceable cyclic peptide. Here, we show how this versatile system can be applied to OFF-switch split CAR systems (MinoCAR) and universal CAR adaptors (MinoUniCAR) with reversible, transient, and dose-dependent suppression; to a tunable T cell activation module based on MyD88/CD40 signaling; to a controllable cellular payload secretion system based on IL12 KDEL retention; and as a cell/cell inducible junction. This work represents an important step forward in the development of a remote-controlled system to precisely control the timing, intensity, and safety of therapeutic interventions.
Keyphrases
  • small molecule
  • protein protein
  • cell therapy
  • stem cells
  • single cell
  • physical activity
  • computed tomography
  • immune response
  • inflammatory response
  • high intensity
  • drug induced