Your search keyword '"smFRET"' showing total 8 results

1. Partial agonism in heteromeric GLUK2/GLUK5 kainate receptor.

Author

Paudyal, Nabina, Das, Anindita, Carrillo, Elisa, Berka, Vladimir, and Jayaraman, Vasanthi

Abstract

Kainate receptors are a subtype of ionotropic glutamate receptors that form transmembrane channels upon binding glutamate. Here, we have investigated the mechanism of partial agonism in heteromeric GluK2/K5 receptors, where the GluK2 and GluK5 subunits have distinct agonist binding profiles. Using single‐molecule Förster resonance energy transfer, we found that at the bi‐lobed agonist‐binding domain, the partial agonist AMPA‐bound receptor occupied intermediate cleft closure conformational states at the GluK2 cleft, compared to the more open cleft conformations in apo form and more closed cleft conformations in the full agonist glutamate‐bound form. In contrast, there is no significant difference in cleft closure states at the GluK5 agonist‐binding domain between the partial agonist AMPA‐ and full agonist glutamate‐bound states. Additionally, unlike the glutamate‐bound state, the dimer interface at the agonist‐binding domain is not decoupled in the AMPA‐bound state. Our findings suggest that partial agonism observed with AMPA binding is mediated primarily due to differences in the GluK2 subunit, highlighting the distinct contributions of the subunits towards activation. [ABSTRACT FROM AUTHOR]

Published

2025

2. A competition smFRET assay to study ligand‐induced conformational changes of the dengue virus protease.

Author

Maus, Hannah, Hinze, Gerald, Hammerschmidt, Stefan Josef, Basché, Thomas, and Schirmeister, Tanja

Abstract

Ligand binding to proteins often is accompanied by conformational transitions. Here, we describe a competition assay based on single molecule Förster resonance energy transfer (smFRET) to investigate the ligand‐induced conformational changes of the dengue virus (DENV) NS2B‐NS3 protease, which can adopt at least two different conformations. First, a competitive ligand was used to stabilize the closed conformation of the protease. Subsequent addition of the allosteric inhibitor reduced the fraction of the closed conformation and simultaneously increased the fraction of the open conformation, demonstrating that the allosteric inhibitor stabilizes the open conformation. In addition, the proportions of open and closed conformations at different concentrations of the allosteric inhibitor were used to determine its binding affinity to the protease. The KD value observed is in accordance with the IC50 determined in the fluorometric assay. Our novel approach appears to be a valuable tool to study conformational transitions of other proteases and enzymes. [ABSTRACT FROM AUTHOR]

Published

2023

3. Alteration of the Conformational Dynamics of a DNA Hairpin by α‐Synuclein in the Presence of Aqueous Two‐Phase Systems.

Author

Mukherjee, Sanjib K., Knop, Jim‐Marcel, Möbitz, Simone, and Winter, Roland H. A.

Subjects

*FLUORESCENCE resonance energy transfer, *HAIRPIN (Genetics), *DNA, *PARKINSON'S disease, *HIGH pressure chemistry

Abstract

The effect of an amyloidogenic intrinsically disordered protein, α‐synuclein, which is associated with Parkinson's disease (PD), on the conformational dynamics of a DNA hairpin (DNA‐HP) was studied by employing the single‐molecule Förster resonance energy transfer method. The open‐to‐closed conformational equilibrium of the DNA‐HP is drastically affected by binding of monomeric α‐synuclein to the loop region of the DNA‐HP. Formation of a protein‐bound intermediate conformation is fostered in the presence of an aqueous two‐phase system mimicking intracellular liquid‐liquid phase separation. Using pressure modulation, additional mechanistic information about the binding complex could be retrieved. Hence, in addition to toxic amyloid formation, α‐synuclein may alter expression profiles of disease‐modifying genes in PD. Furthermore, these findings might also have significant bearings on the understanding of the physiology of organisms thriving at high pressures in the deep sea. [ABSTRACT FROM AUTHOR]

Published

2020

4. Chemical Protein Synthesis Enabled Mechanistic Studies on the Molecular Recognition of K27‐linked Ubiquitin Chains.

Author

Pan, Man, Zheng, Qingyun, Ding, Shan, Zhang, Lujia, Qu, Qian, Wang, Tian, Hong, Danning, Ren, Yujing, Liang, Lujun, Chen, Chunlai, Mei, Ziqing, and Liu, Lei

Subjects

*CHEMOSELECTIVITY, *RECOMBINANT proteins, *PROTEIN expression, *FLUORESCENCE resonance energy transfer, *MOLECULAR recognition

Abstract

New synthetic strategies that exploited the strengths of both chemoselective ligation and recombinant protein expression were developed to prepare K27 di‐ubiquitins (diUb), which enabled mechanistic studies on the molecular recognition of K27‐linked Ubs by single‐molecule Förster resonance energy transfer (smFRET) and X‐ray crystallography. The results revealed that free K27 diUb adopted a compact conformation, whereas upon binding to UCHL3, K27 diUb was remodeled to an open conformation. The K27 isopeptide bond remained rigidly buried inside the diUb moiety during binding, an interesting unique structural feature that may explain the distinctive biological function of K27 Ub chains. [ABSTRACT FROM AUTHOR]

Published

2019

5. The N-Terminal Domain of ALS-Linked TDP-43 Assembles without Misfolding.

Author

Tsoi, Phoebe S., Choi, Kyoung ‐ Jae, Leonard, Paul G., Sizovs, Antons, Moosa, Mahdi Muhammad, MacKenzie, Kevin R., Ferreon, Josephine C., and Ferreon, Allan Chris M.

Subjects

*DNA-binding proteins, *PROTEIN folding, *NEURODEGENERATION, *OLIGOMERIZATION, *BIOPHYSICS, *C-terminal binding proteins

Abstract

Transactivation response element (TAR) DNA-binding protein 43 (TDP-43) misfolding is implicated in several neurodegenerative diseases characterized by aggregated protein inclusions. Misfolding is believed to be mediated by both the N- and C-terminus of TDP-43; however, the mechanistic basis of the contribution of individual domains in the process remained elusive. Here, using single-molecule fluorescence and ensemble biophysical techniques, and a wide range of pH and temperature conditions, we show that TDP-43NTD is thermodynamically stable, well-folded and undergoes reversible oligomerization. We propose that, in full-length TDP-43, association between folded N-terminal domains enhances the propensity of the intrinsically unfolded C-terminal domains to drive pathological aggregation. [ABSTRACT FROM AUTHOR]

Published

2017

6. Osmolyte Effects on the Conformational Dynamics of a DNA Hairpin at Ambient and Extreme Environmental Conditions.

Author

Patra, Satyajit, Anders, Christian, Erwin, Nelli, and Winter, Roland

Subjects

*HAIRPIN (Genetics), *FLUORESCENCE resonance energy transfer, *CONFORMATIONAL analysis, *UREA, *ENTROPY

Abstract

The structural dynamics of a DNA hairpin (Hp) are studied in the absence and presence of the two natural osmolytes trimethylamine-N-oxide (TMAO) and urea at ambient and extreme environmental conditions, including high pressures and high temperatures, by using single-molecule Förster resonance energy transfer and fluorescence correlation spectroscopy. The effect of pressure on the conformational dynamics of the DNA Hp is investigated on a single-molecule level, providing novel mechanistic insights into its conformational conversions. Different from canonical DNA duplex structures of similar melting points, the DNA Hp is found to be rather pressure sensitive. The combined temperature and pressure dependent data allow dissection of the folding free energy into its enthalpic, entropic, and volumetric contributions. The folded conformation is effectively stabilized by the compatible osmolyte TMAO not only at high temperatures, but also at high pressures and in the presence of the destabilizing co-solute urea. [ABSTRACT FROM AUTHOR]

Published

2017

7. Structured m RNA induces the ribosome into a hyper-rotated state.

Author

Qin, Peiwu, Yu, Dongmei, Zuo, Xiaobing, and Cornish, Peter V

Abstract

During protein synthesis, mRNA and tRNA are moved through the ribosome by the process of translocation. The small diameter of the mRNA entrance tunnel only permits unstructured mRNA to pass through. However, there are structured elements within mRNA that present a barrier for translocation that must be unwound. The ribosome has been shown to unwind RNA in the absence of additional factors, but the mechanism remains unclear. Here, we show using single molecule Förster resonance energy transfer and small angle X-ray scattering experiments a new global conformational state of the ribosome. In the presence of the frameshift inducing dnaX hairpin, the ribosomal subunits are driven into a hyper-rotated state and the L1 stalk is predominantly in an open conformation. This previously unobserved conformational state provides structural insight into the helicase activity of the ribosome and may have important implications for understanding the mechanism of reading frame maintenance. [ABSTRACT FROM AUTHOR]

Published

2014

8. Mechanistic insights into antibiotic action on the ribosome through single-molecule fluorescence imaging.

Author

Wang, Leyi, Wasserman, Michael R., Feldman, Michael B., Altman, Roger B., and Blanchard, Scott C.

Abstract

Single-molecule fluorescence imaging has provided unprecedented access to the dynamics of ribosome function, revealing transient intermediate states that are critical to ribosome activity. Imaging platforms have now been developed that are capable of probing many hundreds of molecules simultaneously at temporal and spatial resolutions approaching the sub-millisecond time and the sub-nanometer scales. These advances enable both steady- and pre-steady state measurements of individual steps in the translation process as well as processive reactions. The data generated using these methods have yielded new, quantitative structural and kinetic insights into ribosomal activity. They have also shed light on the mechanisms of antibiotic targeting the translation apparatus, revealing features of the structure–function relationship that would be difficult to obtain by other means. This review provides an overview of the types of information that can be obtained using such imaging platforms and a blueprint for using the technique to assess how small-molecule antibiotics alter macromolecular functions. [ABSTRACT FROM AUTHOR]

Published

2011