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Development of an allosteric adhesion GPCR nanobody with therapeutic potential

A nanobody was identified that targets the N-terminal fragment of the adhesion G-protein-coupled receptor ADGRG2, allosterically enhances activation by the natural agonist dehydroepiandrosterone and restores signaling in mutant receptors.

Yuan Zheng
Dan Jiang
Shiqing Feng
Research15 May 2025
Nature Chemical Biology

Volume: 21, P: 1519-1530
Structural insights into the mechanisms of urea permeation and distinct inhibition modes of urea transporters

Here, authors present cryo-EM structures and simulations of urea transporter members in resting-, transport-, or inactive-states bound with synthetic competitive, uncompetitive or noncompetitive inhibitor.

Shen-Ming Huang
Zhi-Zhen Huang
Jin-Peng Sun
ResearchOpen Access26 Nov 2024
Nature Communications

Volume: 15, P: 1-17
Structural characterization of the urea transporter bound to the orally bioavailable inhibitor E3

Shen-ming Huang
Bo-yang Cai
Jin-peng Sun
Research16 Jun 2025
Acta Pharmacologica Sinica

P: 1-9
Tethered peptide activation mechanism of the adhesion GPCRs ADGRG2 and ADGRG4

Cryo-electron microscopy structures of three adhesion G protein-coupled receptors (aGPCRs) complexes provide insight into the tethered activation mechanism of aGPCRs and show the potential for rational design of agonists.

Peng Xiao
Shengchao Guo
Xiao Yu
Research13 Apr 2022
Nature

Volume: 604, P: 771-778
Structural studies of phosphorylation-dependent interactions between the V2R receptor and arrestin-2

The interaction between a GPCR, such as the vasopressin receptor-2 (V2R), and arrestin depends on the receptors’ phosphorylation pattern. Here authors use FRET and NMR to analyze the phosphorylation patterns of the V2R-arrestin complex and show that phospho-interactions are the key determinants of selective arrestin conformational states and correlated functions.

Qing-Tao He
Peng Xiao
Xiao Yu
ResearchOpen Access22 Apr 2021
Nature Communications

Volume: 12, P: 1-16
DeSiphering receptor core-induced and ligand-dependent conformational changes in arrestin via genetic encoded trimethylsilyl ¹H-NMR probe

Characterization of dynamic conformational changes in membrane protein complexes by NMR spectroscopy remains challenging. Here authors report the site-specific incorporation of 4-trimethylsilyl phenylalanine (TMSiPhe) into proteins, which enabled the characterization of multiple conformational states of a phospho-β2 adrenergic receptor/β-arrestin-1 complex in response to different receptor ligands.

Qi Liu
Qing-tao He
Jin-peng Sun
ResearchOpen Access25 Sept 2020
Nature Communications

Volume: 11, P: 1-17
Core-shell heterostructured multiwalled carbon nanotubes@reduced graphene oxide nanoribbons/chitosan, a robust nanobiocomposite for enzymatic biosensing of hydrogen peroxide and nitrite

Veerappan Mani
Mani Govindasamy
Sheng-Tung Huang
ResearchOpen Access19 Sept 2017
Scientific Reports

Volume: 7, P: 1-10

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Development of an allosteric adhesion GPCR nanobody with therapeutic potential

Structural insights into the mechanisms of urea permeation and distinct inhibition modes of urea transporters

Structural characterization of the urea transporter bound to the orally bioavailable inhibitor E3

Tethered peptide activation mechanism of the adhesion GPCRs ADGRG2 and ADGRG4

Structural studies of phosphorylation-dependent interactions between the V2R receptor and arrestin-2

DeSiphering receptor core-induced and ligand-dependent conformational changes in arrestin via genetic encoded trimethylsilyl 1H-NMR probe

Core-shell heterostructured multiwalled carbon nanotubes@reduced graphene oxide nanoribbons/chitosan, a robust nanobiocomposite for enzymatic biosensing of hydrogen peroxide and nitrite

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DeSiphering receptor core-induced and ligand-dependent conformational changes in arrestin via genetic encoded trimethylsilyl ¹H-NMR probe