RosettaGPCR: Multiple Template Homology Modeling of GPCRs with Rosetta

Bender, Brian J.; Marlow, Brennica; Meiler, Jens

doi:10.1101/2019.12.13.875237

Cited by 3 publications

(2 citation statements)

References 48 publications

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“…The GnRHR sequence was first aligned with sequences for 34 GPCR crystal structures obtained from GPCRdb ( http://www.gpcrdb.org ) ( Isberg et al, 2016 ). Manual adjustments were then made to account for well-known conserved residues in loop regions and TM domains ( Bender et al, 2019 ). OCTOPUS was used to define the TM domains, and the two disulfide bonds were defined manually ( Millar et al, 2004 ; Viklund and Elofsson, 2008 ).…”

Section: Methodsmentioning

confidence: 99%

Molecular basis for the evolved instability of a human G-protein coupled receptor

et al. 2021

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Section: Methodsmentioning

confidence: 99%

Molecular basis for the evolved instability of a human G-protein coupled receptor

et al. 2021

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“…These residues are typically chosen by comparing different crystal structures, which have identified common allosteric switches/connectors that subtly change their conformation leading to large-scale rewiring of contacts and active receptor conformations [ 29 , 30 , 31 , 33 , 34 , 179 , 180 , 181 ]. The selection of sites-of-interest is certainly most straightforward if the atomic structure of the receptor has been determined, although homology models give workable starting points [ 182 , 183 , 184 ]. By combining information from several sites, a comprehensive picture can be constructed for a given receptor, which covers the energy profile and structural alterations of different loci when the receptor is stimulated with different ligands or interacts with different transducers.…”

Section: A Receptor’s Perspectivementioning

confidence: 99%

Capturing Peptide–GPCR Interactions and Their Dynamics

Kaiser

Coin

2020

Molecules

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Many biological functions of peptides are mediated through G protein-coupled receptors (GPCRs). Upon ligand binding, GPCRs undergo conformational changes that facilitate the binding and activation of multiple effectors. GPCRs regulate nearly all physiological processes and are a favorite pharmacological target. In particular, drugs are sought after that elicit the recruitment of selected effectors only (biased ligands). Understanding how ligands bind to GPCRs and which conformational changes they induce is a fundamental step toward the development of more efficient and specific drugs. Moreover, it is emerging that the dynamic of the ligand–receptor interaction contributes to the specificity of both ligand recognition and effector recruitment, an aspect that is missing in structural snapshots from crystallography. We describe here biochemical and biophysical techniques to address ligand–receptor interactions in their structural and dynamic aspects, which include mutagenesis, crosslinking, spectroscopic techniques, and mass-spectrometry profiling. With a main focus on peptide receptors, we present methods to unveil the ligand–receptor contact interface and methods that address conformational changes both in the ligand and the GPCR. The presented studies highlight a wide structural heterogeneity among peptide receptors, reveal distinct structural changes occurring during ligand binding and a surprisingly high dynamics of the ligand–GPCR complexes.

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Molecular Basis for the Evolved Instability of a Human G-Protein Coupled Receptor

Chamness

Zelt

Kuntz

et al. 2019

Preprint

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Membrane proteins are prone to misfolding and degradation. This is particularly true for mammalian forms of the gonadotropin-releasing hormone receptor (GnRHR). Though they function at the plasma membrane, mammalian GnRHRs tend to accumulate within the secretory pathway. Their apparent instability is believed to have evolved in response to selection for attenuated GnRHR activity. Nevertheless, the structural basis of this adaptation remains unclear. We find that this adaptation coincides with a C-terminal truncation and an increase in the polarity of its transmembrane (TM) domains. This enhanced polarity compromises the translocon-mediated cotranslational folding of two TM domains. Moreover, replacing a conserved polar residue in TM6 with an ancestral hydrophobic residue partially restores GnRHR expression with minimal impact on function. An evolutionary analysis suggests variations in the polarity of this residue are associated with reproductive differences. Our findings suggest the marginal energetics of cotranslational folding can be exploited to tune membrane protein fitness.

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RosettaGPCR: Multiple Template Homology Modeling of GPCRs with Rosetta

Cited by 3 publications

References 48 publications

Molecular basis for the evolved instability of a human G-protein coupled receptor

Molecular basis for the evolved instability of a human G-protein coupled receptor

Capturing Peptide–GPCR Interactions and Their Dynamics

Molecular Basis for the Evolved Instability of a Human G-Protein Coupled Receptor

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