Structure-Activity Relationship and Signaling of New Chimeric CXCR4 Agonists.

Mona, Christine E; Besserer-Offroy, Élie; Cabana, Jérôme; Lefrançois, Marilou; Boulais, Philip E; Lefebvre, Marie-Reine; Leduc, Richard; Lavigne, Pierre; Heveker, Nikolaus; Marsault, Éric; Escher, Emanuel

Mona, Christine E; Besserer-Offroy, Élie; Cabana, Jérôme; Lefrançois, Marilou; Boulais, Philip E; Lefebvre, Marie-Reine; Leduc, Richard; Lavigne, Pierre; Heveker, Nikolaus; Marsault, Éric; Escher, Emanuel.

Afiliação

Mona CE; Department of Pharmacology-Physiology, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Besserer-Offroy É; Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Cabana J; Department of Pharmacology-Physiology, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Lefrançois M; Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Boulais PE; Department of Pharmacology-Physiology, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Lefebvre MR; Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Leduc R; Department of Pharmacology-Physiology, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Lavigne P; Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Heveker N; Department of Pharmacology-Physiology, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Marsault É; Institut de Pharmacologie de Sherbrooke, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.
Escher E; Department of Pharmacology-Physiology, Université de Sherbrooke , Sherbrooke, QC J1H 5N4, Canada.

J Med Chem ; 59(16): 7512-24, 2016 08 25.

Article em En | MEDLINE | ID: mdl-27434274

RESUMO

The CXCR4 receptor binds with meaningful affinities only CXCL12 and synthetic antagonists/inverse agonists. We recently described high affinity synthetic agonists for this chemokine receptor, obtained by grafting the CXCL12 N-terminus onto the inverse agonist T140. While those chimeric molecules behave as agonists for CXCR4, their binding and activation mode are unknown. The present SAR of those CXCL12-oligopeptide grafts reveals the key determinants involved in CXCR4 activation. Position 3 (Val) controls affinity, whereas position 7 (Tyr) acts as an efficacy switch. Chimeric molecules bearing aromatic residues in position 3 possess high binding affinities for CXCR4 and are Gαi full agonists with robust chemotactic properties. Fine-tuning of electron-poor aromatic rings in position 7 enhances receptor activation. To rationalize these results, a homology model of a receptor-ligand complex was built using the published crystal structures of CXCR4. Molecular dynamics simulations reveal further details accounting for the observed SAR for this series.

Assuntos

Peptídeos/farmacologia; Receptores CXCR4/agonistas; Relação Dose-Resposta a Droga; Humanos; Simulação de Dinâmica Molecular; Estrutura Molecular; Peptídeos/síntese química; Peptídeos/química; Transdução de Sinais/efeitos dos fármacos; Relação Estrutura-Atividade

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Peptídeos / Receptores CXCR4 Limite: Humans Idioma: En Ano de publicação: 2016 Tipo de documento: Article

Texto completo

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PubMed Links

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Peptídeos / Receptores CXCR4 Limite: Humans Idioma: En Ano de publicação: 2016 Tipo de documento: Article