The mechanism of coupled folding-upon-binding of an intrinsically disordered protein

Robustelli, Paul; Piana, Stefano; Shaw, David E.

doi:10.1101/2020.03.23.004283

Cited by 3 publications

(4 citation statements)

References 45 publications

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“…Simulations are performed in explicit water and ions at room temperature and physiological salt concentration using the a99SB-disp force field. [46] By computing the PMF as a function of the center-of-mass (COM) distance between one reference peptide, which we dissociate from the other peptides (see further details of these calculations in Supporting Information), we determine the binding free energy difference between the structured (kinked 𝛽-sheet motif; PDB code 5WHN) and the fully disordered state of a TDP-43 LARKS aggregate (Figure 1a).…”

Section: Larks Abundance In Low-complexity Domains Critically Modulat...mentioning

confidence: 99%

“…The chosen LARKS distribution across the low-complexity domains is in all cases symmetric and equispaced (as shown in Figure 1c for the "1-Center," "2-Equispaced," and "3-Equispaced" sequences) and the total length using the a99SB-disp force field. [46] Simulations are carried out at room conditions and physiological NaCl concentration. While the solid green curve denotes the interaction strength among peptides with a kinked 𝛽-sheet structure, the dashed red curve accounts for the interaction energy among the same segments when they are fully disordered.…”

Section: Larks Abundance In Low-complexity Domains Critically Modulat...mentioning

confidence: 99%

“…[41][42][43][44][45] In this work, we use multiscale simulations to investigate the impact of LARKS abundance and patterning in the progressive maturation of biomolecular condensates. Our multiscale approach bridges atomistic force fields [46,47] and coarse-grained models of proteins and nucleic acids. [48,49] Based on structured versus disordered peptide binding interactions predicted from free-energy atomistic calculations, we develop a coarse-grained model for LARKS-containing low-complexity domains that considers the accumulation of local structural transitions over time inside coarse-grained protein condensates.…”

Section: Introductionmentioning

confidence: 99%

“…Disorder-to-𝛽-sheet structural transitions augments protein binding, and their progressive accumulation within biomolecular condensates increases density. a) Atomistic potential of mean force (PMF) dissociation curves of a 6-amino acid segment (PDB code: 5WHN) of the TDP-43 lowcomplexity domain sequence from a 𝛽-sheet structure formed by six peptides (of the same sequence) as a function of the center-of-mass distance (COM)using the a99SB-disp force field [46]. Simulations are carried out at room conditions and physiological NaCl concentration.…”

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confidence: 99%

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Location and Concentration of Aromatic‐Rich Segments Dictates the Percolating Inter‐Molecular Network and Viscoelastic Properties of Ageing Condensates

et al. 2023

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Maturation of functional liquid‐like biomolecular condensates into solid‐like aggregates has been linked to the onset of several neurodegenerative disorders. Low‐complexity aromatic‐rich kinked segments (LARKS) contained in numerous RNA‐binding proteins can promote aggregation by forming inter‐protein β‐sheet fibrils that accumulate over time and ultimately drive the liquid‐to‐solid transition of the condensates. Here, atomistic molecular dynamics simulations are combined with sequence‐dependent coarse‐grained models of various resolutions to investigate the role of LARKS abundance and position within the amino acid sequence in the maturation of condensates. Remarkably, proteins with tail‐located LARKS display much higher viscosity over time than those in which the LARKS are placed toward the center. Yet, at very long timescales, proteins with a single LARKS—independently of its location—can still relax and form high viscous liquid condensates. However, phase‐separated condensates of proteins containing two or more LARKS become kinetically trapped due to the formation of percolated β‐sheet networks that display gel‐like behavior. Furthermore, as a work case example, they demonstrate how shifting the location of the LARKS‐containing low‐complexity domain of FUS protein toward its center effectively precludes the accumulation of β‐sheet fibrils in FUS‐RNA condensates, maintaining functional liquid‐like behavior without ageing.

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Section: Larks Abundance In Low-complexity Domains Critically Modulat...mentioning

confidence: 99%

Section: Larks Abundance In Low-complexity Domains Critically Modulat...mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

mentioning

confidence: 99%

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Location and Concentration of Aromatic‐Rich Segments Dictates the Percolating Inter‐Molecular Network and Viscoelastic Properties of Ageing Condensates

et al. 2023

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Transient exposure of a buried phosphorylation site in an autoinhibited protein

Orioli

Lindorff‐Larsen

2021

Preprint

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Autoinhibition is a mechanism used to regulate protein function, often by making functional sites inaccessible through the interaction with a cis-acting inhibitory domain. Such autoinhibitory domains often display a substantial degree of structural disorder when unbound, and only become structured in the inhibited state. This structural dynamics makes it difficult to study the structural origin of regulation, including effects of regulatory post-translational modifications. Here, we study the autoinhibition of the Dbl Homology domain in the protein Vav1 by the so-called acidic inhibitory domain. We use molecular simulations to study the process by which a mostly unstructured inhibitory domain folds upon binding and how transient exposure of a key buried tyrosine residue makes it accessible for phosphorylation. We show that the inhibitory domain, which forms a helix in the bound and inhibited stated, samples helical structures already before binding and that binding occurs via a molten-globule-like intermediate state. Together, our results shed light on key interactions that enable the inhibitory domain to sample a finely-tuned equilibrium between an inhibited and a kinase-accessible state.

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Deciphering the Role of Residues Involved in Disorder-To-Order Transition Regions in Archaeal tRNA Methyltransferase 5

Srivastava

Yesudhas

Ahmad

et al. 2021

Genes

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tRNA methyltransferase 5 (Trm5) enzyme is an S-adenosyl methionine (AdoMet)-dependent methyltransferase which methylates the G37 nucleotide at the N1 atom of the tRNA. The free form of Trm5 enzyme has three intrinsically disordered regions, which are highly flexible and lack stable three-dimensional structures. These regions gain ordered structures upon the complex formation with tRNA, also called disorder-to-order transition (DOT) regions. In this study, we performed molecular dynamics (MD) simulations of archaeal Trm5 in free and complex forms and observed that the DOT residues are highly flexible in free proteins and become stable in complex structures. The energetic contributions show that DOT residues are important for stabilising the complex. The DOT1 and DOT2 are mainly observed to be important for stabilising the complex, while DOT3 is present near the active site to coordinate the interactions between methyl-donating ligands and G37 nucleotides. In addition, mutational studies on the Trm5 complex showed that the wild type is more stable than the G37A tRNA mutant complex. The loss of productive interactions upon G37A mutation drives the AdoMet ligand away from the 37th nucleotide, and Arg145 in DOT3 plays a crucial role in stabilising the ligand, as well as the G37 nucleotide, in the wild-type complex. Further, the overall energetic contribution calculated using MMPBSA corroborates that the wild-type complex has a better affinity between Trm5 and tRNA. Overall, our study reveals that targeting DOT regions for binding could improve the inhibition of Trm5.

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The mechanism of coupled folding-upon-binding of an intrinsically disordered protein

Cited by 3 publications

References 45 publications

Location and Concentration of Aromatic‐Rich Segments Dictates the Percolating Inter‐Molecular Network and Viscoelastic Properties of Ageing Condensates

Location and Concentration of Aromatic‐Rich Segments Dictates the Percolating Inter‐Molecular Network and Viscoelastic Properties of Ageing Condensates

Transient exposure of a buried phosphorylation site in an autoinhibited protein

Deciphering the Role of Residues Involved in Disorder-To-Order Transition Regions in Archaeal tRNA Methyltransferase 5

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