Artículo
The nitrone spin trap 5,5‑dimethyl‑1‑pyrroline N‑oxide binds to toll-like receptor-2-TIR-BB-loop domain and dampens downstream inflammatory signaling
Muñoz, Marcos David
; Gutierrez, Lucas Joel
; Delignat, Sandrine; Russick, Jules; Gomez-Mejiba, Sandra Esther
; Lacroix Desmazes, Sebastien; Enriz, Ricardo Daniel
; Ramirez, Dario
Fecha de publicación:
01/06/2019
Editorial:
Elsevier Science
Revista:
Biochimica et Biophysica Acta - Molecular Basis of Disease
ISSN:
0925-4439
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
The nitrone spin trap 5,5‑dimethyl‑1‑pyrroline N‑oxide (DMPO) dampens endotoxin-induced and TLR4-driven priming of macrophages, but the mechanism remains unknown. The available information suggests a direct binding of DMPO to the TIR domain, which is shared between TLRs. However, TLR2-TIR domain is the only TLR that have been crystallized. Our in silico data show that DMPO binds to four specific residues in the BB-loop within the TLR2-TIR domain. Our functional analysis using hTLR2.6-expressing HEKs cells showed that DMPO can block zymosan-triggered-TLR2-mediated NF-κB activation. However, DMPO did not affect the overall TLR2-MyD88 protein-protein interaction. DMPO binds to the BB-loop in the TIR-domain and dampens downstream signaling without affecting the overall TIR-MyD88 interaction. These data encourage the use of DMPO-derivatives as potential mechanism-based inhibitors of TLR-triggered inflammation.
Palabras clave:
BB-LOOP
,
DMPO
,
MECHANISM-BASED DRUG
,
SIGNAL TRANSDUCTION
,
TIR DOMAIN
,
TLR2
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Articulos(IMIBIO-SL)
Articulos de INST. MULTIDICIPLINARIO DE INV. BIO. DE SAN LUIS
Articulos de INST. MULTIDICIPLINARIO DE INV. BIO. DE SAN LUIS
Citación
Muñoz, Marcos David; Gutierrez, Lucas Joel; Delignat, Sandrine; Russick, Jules; Gomez-Mejiba, Sandra Esther; et al.; The nitrone spin trap 5,5‑dimethyl‑1‑pyrroline N‑oxide binds to toll-like receptor-2-TIR-BB-loop domain and dampens downstream inflammatory signaling; Elsevier Science; Biochimica et Biophysica Acta - Molecular Basis of Disease; 1865; 6; 1-6-2019; 1152-1159
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