Jérôme Cabana scite author profile

Background: G protein-coupled receptors (GPCRs) modulate a plethora of physiological processes. Results: The determination of 38 ligand/receptor contacts enabled the evidence-based modeling of a GPCR structure. Conclusion: The proposed GPCR structure assumes four interaction clusters with its ligand, which adopts a vertical binding mode. Significance: Elucidating the structure of GPCRs is central to their understanding and has several implications, e.g. rational drug design.

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Critical Hydrogen Bond Formation for Activation of the Angiotensin II Type 1 Receptor

Cabana

Holleran

Beaulieu

et al. 2013

Journal of Biological Chemistry

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Background:The N111G and N111W mutations make the AT 1 receptor constitutively active and inactivable, respectively. Results: The orientation and interactions of D74 2.50 are influenced by the residue at position 111 3.35 . Conclusion: H-bond formation between D742.50 and N46 1.50 is critical for AT 1 receptor activation. Significance: This novel molecular switch could be involved in the GPCR activation mechanism as it involves highly conserved residues D 2.50 and N 1.50 .

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Identification of Distinct Conformations of the Angiotensin-II Type 1 Receptor Associated with the Gq/11 Protein Pathway and the β-Arrestin Pathway Using Molecular Dynamics Simulations

Cabana

Holleran

Leduc

et al. 2015

Journal of Biological Chemistry

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Background: The N111G and D74N mutations bias the AT 1 receptor for the G q/11 and ␤-arrestin pathways, respectively. Results: Structural rearrangements of theAT 1 receptor are induced by the N111G mutation and AngII. Conclusion: Activation of the G q/11 and ␤-arrestin pathways is associated with a decreased and increased stability, respectively, of the ground state of the receptor. Significance: Distinct conformations of AT 1 receptor are associated with distinct pathways.

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Jérôme Cabana

Impact of guideline-consistent therapy on outcome of patients with healthcare-associated and community-acquired pneumonia

Structure of the Human Angiotensin II Type 1 (AT1) Receptor Bound to Angiotensin II from Multiple Chemoselective Photoprobe Contacts Reveals a Unique Peptide Binding Mode

Critical Hydrogen Bond Formation for Activation of the Angiotensin II Type 1 Receptor

Identification of Distinct Conformations of the Angiotensin-II Type 1 Receptor Associated with the Gq/11 Protein Pathway and the β-Arrestin Pathway Using Molecular Dynamics Simulations

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