conformational freedom
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Molecules ◽  
2021 ◽  
Vol 26 (23) ◽  
pp. 7100
Author(s):  
Marek P. Szymański ◽  
Marcin Grajda ◽  
Agnieszka Szumna

Electronic circular dichroism (ECD) can be used to study various aspects of self-assembly (definition of stoichiometric ratios, chirality amplification during self-assembly, host-guest complexation). In this work, we show that ECD is a valuable tool for monitoring the self-assembly of chiral peptide-based capsules. By analyzing the signs, intensities, and temperature dependences of ECD bands, the effects of the non-specific processes can be separated from the restriction of intramolecular motion (RIM) caused by discrete self-assembly. Analysis of experimental and theoretical ECD spectra show that the differences between assembled and non-assembled species originate from induction of inherently chiral conformation and restriction of conformational freedom that leads to amplification of ECD signals during self-assembly of discrete species.


2021 ◽  
Vol 31 (45) ◽  
pp. 2170334
Author(s):  
Chenxi Zhai ◽  
Shangchao Lin ◽  
Mingchao Wang ◽  
Huanhuan Zhou ◽  
Eugenia Stanisauskis ◽  
...  

2021 ◽  
pp. 2104414
Author(s):  
Chenxi Zhai ◽  
Shangchao Lin ◽  
Mingchao Wang ◽  
Huanhuan Zhou ◽  
Eugenia Stanisauskis ◽  
...  

2021 ◽  
Author(s):  
Michael Gecht ◽  
Sören von Bülow ◽  
Camille Penet ◽  
Gerhard Hummer ◽  
Cyril Hanus ◽  
...  

More than 75% of surface and secreted proteins are modified by covalent addition of complex sugars through N- and O-glycosylation. Unlike proteins, glycans do not typically adopt specific secondary structures and remain very mobile, influencing protein dynamics and interactions with other molecules. Glycan conformational freedom impairs complete structural elucidation of glycoproteins. Computer simulations may be used to model glycan structure and dynamics. However, such simulations typically require thousands of computing hours on specialized supercomputers, thus limiting routine use. Here, we describe a reductionist method that can be implemented on personal computers to graft ensembles of realistic glycan conformers onto static protein structures in a matter of minutes. Using this open-source pipeline, we reconstructed the full glycan cover of SARS-CoV-2 Spike protein (S-protein) and a human GABAA receptor. Focusing on S-protein, we show that GlycoSHIELD recapitulates key features of extended simulations of the glycosylated protein, including epitope masking, and provides new mechanistic insights on N-glycan impact on protein structural dynamics.


2021 ◽  
Vol 9 ◽  
Author(s):  
Andrés E. Martín Díaz ◽  
James E. M. Lewis

Metal-organic cages (MOCs) have emerged as a diverse class of molecular hosts with potential utility across a vast spectrum of applications. With advances in single-crystal X-ray diffraction and economic methods of computational structure optimisation, cavity sizes can be readily determined. In combination with a chemist’s intuition, educated guesses about the likelihood of particular guests being bound within these porous structures can be made. Whilst practically very useful, simple rules-of-thumb, such as Rebek’s 55% rule, fail to take into account structural flexibility inherent to MOCs that can allow hosts to significantly adapt their internal cavity. An often unappreciated facet of MOC structures is that, even though relatively rigid building blocks may be employed, conformational freedom can enable large structural changes. If it could be exploited, this flexibility might lead to behavior analogous to the induced-fit of substrates within the active sites of enzymes. To this end, in-roads have already been made to prepare MOCs incorporating ligands with large degrees of conformational freedom. Whilst this may make the constitution of MOCs harder to predict, it has the potential to lead to highly sophisticated and functional synthetic hosts.


2021 ◽  
Author(s):  
Alexander Kotter ◽  
Henning D. Mootz ◽  
Andreas Heuer

SUMO targeted ubiqutin ligases (STUbLs) like RNF4 or Arkadia/RNF111 recognize SUMO chains through multiple SUMO interacting motifs (SIMs). Typically, these are contained in disordered regions of these enzymes and also the individual SUMO domains of SUMO chains move relatively freely. It is assumed that binding the SIM region significantly restricts the conformational freedom of SUMO chains. Here, we present the results of extensive molecular dynamics simulations on the complex formed by the SIM2-SIM3 region of RNF4 and diSUMO3. Though our simulations highlight the importance of typical SIM-SUMO interfaces also in the multivalent situation, we observe that frequently other regions of the peptide than the canonical SIMs establish this interface. This variability regarding the individual interfaces leads to a conformationally highly flexible complex. Even though this is in contrast to previous models of the RNF4 SUMO chain interaction, we demonstrate that our simulations are clearly consistent with previous experimental results.


Author(s):  
Yuhui Yang ◽  
Zhe He ◽  
Junzhao He ◽  
Yuqing Li ◽  
Yilong Chen ◽  
...  

Efficient isomerization of photochromic molecules requires conformational freedom and is often limited to the solution or polymer matrix. Thus, developing a new method to improve photochromism in the solid state...


Author(s):  
Junzhao He ◽  
Huimin Zhao ◽  
Han Wu ◽  
Yuhui Yang ◽  
Zhaohui Wang ◽  
...  

For photochromic molecules, effective isomerization usually requires conformational freedom,which is usually unavailable in solvent-free conditions. In this work, we report a new method, which can realize the reversible switching of...


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