| Literature DB >> 28003549 |
Aldo Borroto1, Diana Reyes-Garau1, M Angeles Jiménez2, Esther Carrasco3, Beatriz Moreno4, Sara Martínez-Pasamar4, José R Cortés5, Almudena Perona1, David Abia1, Soledad Blanco1, Manuel Fuentes6, Irene Arellano1, Juan Lobo1, Haleh Heidarieh1, Javier Rueda1, Pilar Esteve1, Danay Cibrián5, Ana Martinez-Riaño1, Pilar Mendoza1, Cristina Prieto1, Enrique Calleja1, Clara L Oeste1, Alberto Orfao6, Manuel Fresno1, Francisco Sánchez-Madrid5, Antonio Alcamí1, Paola Bovolenta1, Pilar Martín5, Pablo Villoslada4, Antonio Morreale1, Angel Messeguer3, Balbino Alarcon7.
Abstract
Modulating T cell activation is critical for treating autoimmune diseases but requires avoiding concomitant opportunistic infections. Antigen binding to the T cell receptor (TCR) triggers the recruitment of the cytosolic adaptor protein Nck to a proline-rich sequence in the cytoplasmic tail of the TCR's CD3ε subunit. Through virtual screening and using combinatorial chemistry, we have generated an orally available, low-molecular weight inhibitor of the TCR-Nck interaction that selectively inhibits TCR-triggered T cell activation with an IC50 (median inhibitory concentration) ~1 nM. By modulating TCR signaling, the inhibitor prevented the development of psoriasis and asthma and, furthermore, exerted a long-lasting therapeutic effect in a model of autoimmune encephalomyelitis. However, it did not prevent the generation of a protective memory response against a mouse pathogen, suggesting that the compound might not exert its effects through immunosuppression. These results suggest that inhibiting an immediate TCR signal has promise for treating a broad spectrum of human T cell-mediated autoimmune and inflammatory diseases.Entities:
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Year: 2016 PMID: 28003549 DOI: 10.1126/scitranslmed.aaf2140
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956