Your search keyword '"F Troilo"' showing total 10 results

1. Folding and Misfolding of a PDZ Tandem Repeat.

Author

Visconti L, Malagrinò F, Troilo F, Pagano L, Toto A, and Gianni S

Subjects

Amino Acid Sequence genetics, Humans, Membrane Proteins ultrastructure, Protein Binding genetics, Protein Conformation, Membrane Proteins genetics, PDZ Domains genetics, Protein Folding, Tandem Repeat Sequences genetics

Abstract

Although the vast majority of the human proteome is represented by multi-domain proteins, the study of multi-domain folding and misfolding is a relatively poorly explored field. The protein Whirlin is a multi-domain scaffolding protein expressed in the inner ear. It is characterized by the presence of tandem repeats of PDZ domains. The first two PDZ domains of Whirlin (PDZ1 and PDZ2 - namely P1P2) are structurally close and separated by a disordered short linker. We recently described the folding mechanism of the P1P2 tandem. The difference in thermodynamic stability of the two domains allowed us to selectively unfold one or both PDZ domains and to pinpoint the accumulation of a misfolded intermediate, which we demonstrated to retain physiological binding activity. In this work, we provide an extensive characterization of the folding and unfolding of P1P2. Based on the observed data, we describe an integrated kinetic analysis that satisfactorily fits the experiments and provides a valuable model to interpret multi-domain folding. The experimental and analytical approaches described in this study may be of general interest for the interpretation of complex multi-domain protein folding kinetics., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

2. Understanding the Binding Induced Folding of Intrinsically Disordered Proteins by Protein Engineering: Caveats and Pitfalls.

Author

Malagrinò F, Visconti L, Pagano L, Toto A, Troilo F, and Gianni S

Subjects

Intrinsically Disordered Proteins genetics, Mutation genetics, Protein Binding, Intrinsically Disordered Proteins chemistry, Intrinsically Disordered Proteins metabolism, Protein Engineering, Protein Folding

Abstract

Many proteins lack a well-defined three-dimensional structure in isolation. These proteins, typically denoted as intrinsically disordered proteins (IDPs), may display a characteristic disorder-to-order transition when binding their physiological partner(s). From an experimental perspective, it is of great importance to establish the general grounds to understand how such folding processes may be explored. Here we discuss the caveats and the pitfalls arising when applying to IDPs one of the key techniques to characterize the folding of globular proteins, the Φ value analysis. This method is based on measurements of the free energy changes of transition and native states upon conservative, non-disrupting, mutations. On the basis of available data, we reinforce the validity of Φ value analysis in the study of IDPs and suggest future experiments to further validate this powerful experimental method.

Published

2020

3. Templated folding of intrinsically disordered proteins.

Author

Toto A, Malagrinò F, Visconti L, Troilo F, Pagano L, Brunori M, Jemth P, and Gianni S

Subjects

Intrinsically Disordered Proteins metabolism, Intrinsically Disordered Proteins chemistry, Models, Molecular, Protein Folding

Abstract

Much of our current knowledge of biological chemistry is founded in the structure-function relationship, whereby sequence determines structure that determines function. Thus, the discovery that a large fraction of the proteome is intrinsically disordered, while being functional, has revolutionized our understanding of proteins and raised new and interesting questions. Many intrinsically disordered proteins (IDPs) have been determined to undergo a disorder-to-order transition when recognizing their physiological partners, suggesting that their mechanisms of folding are intrinsically different from those observed in globular proteins. However, IDPs also follow some of the classic paradigms established for globular proteins, pointing to important similarities in their behavior. In this review, we compare and contrast the folding mechanisms of globular proteins with the emerging features of binding-induced folding of intrinsically disordered proteins. Specifically, whereas disorder-to-order transitions of intrinsically disordered proteins appear to follow rules of globular protein folding, such as the cooperative nature of the reaction, their folding pathways are remarkably more malleable, due to the heterogeneous nature of their folding nuclei, as probed by analysis of linear free-energy relationship plots. These insights have led to a new model for the disorder-to-order transition in IDPs termed "templated folding," whereby the binding partner dictates distinct structural transitions en route to product, while ensuring a cooperative folding., (© 2020 Toto et al.)

Published

2020

4. Understanding Binding-Induced Folding by Temperature Jump.

Author

Toto A, Troilo F, Malagrinò F, and Gianni S

Subjects

Artifacts, Buffers, Calibration, Electric Conductivity, Equipment Design, Intrinsically Disordered Proteins metabolism, Nucleocapsid Proteins metabolism, Osmolar Concentration, Protein Domains, Temperature, Tryptophan analogs & derivatives, Tryptophan analysis, Intrinsically Disordered Proteins chemistry, Nucleocapsid Proteins chemistry, Protein Binding, Protein Folding

Abstract

Temperature jump is a powerful technique for the characterization of fast kinetics and can be readily employed to understand both binding and folding reactions. Here we summarize briefly a temperature-jump prototypical experiment between an intrinsically disordered protein and its physiological partner. The model used is the N TAIL domain from Measles virus Nucleoprotein and its natural ligand, the globular P XD domain from Measles virus Phosphoprotein. We recapitulate how to set up the experiment and how to analyze data in order to extract the kinetic parameters of the reaction.

Published

2020

5. The Effect of Proline cis - trans Isomerization on the Folding of the C-Terminal SH2 Domain from p85.

Author

Troilo F, Malagrinò F, Visconti L, Toto A, and Gianni S

Subjects

Class Ia Phosphatidylinositol 3-Kinase genetics, Humans, src Homology Domains, Class Ia Phosphatidylinositol 3-Kinase chemistry, Protein Folding

Abstract

SH2 domains are protein domains that modulate protein-protein interactions through a specific interaction with sequences containing phosphorylated tyrosines. In this work, we analyze the folding pathway of the C-terminal SH2 domain of the p85 regulatory subunit of the protein PI3K, which presents a proline residue in a cis configuration in the loop between the βE and βF strands. By employing single and double jump folding and unfolding experiments, we demonstrate the presence of an on-pathway intermediate that transiently accumulates during (un)folding. By comparing the kinetics of folding of the wild-type protein to that of a site-directed variant of C-SH2 in which the proline was replaced with an alanine, we demonstrate that this intermediate is dictated by the peptidyl prolyl cis-trans isomerization. The results are discussed in the light of previous work on the effect of peptidyl prolyl cis-trans isomerization on folding events., Competing Interests: The authors declare no conflicts of interest.

Published

2019

6. Binding induced folding: Lessons from the kinetics of interaction between N TAIL and XD.

Author

Toto A, Troilo F, Visconti L, Malagrinò F, Bignon C, Longhi S, and Gianni S

Subjects

Intrinsically Disordered Proteins chemistry, Kinetics, Protein Binding, Protein Domains, Viral Proteins chemistry, Intrinsically Disordered Proteins metabolism, Measles virus chemistry, Protein Folding, Viral Proteins metabolism

Abstract

Intrinsically Disordered Proteins (IDPs) are a class of protein that exert their function despite lacking a well-defined three-dimensional structure, which is sometimes achieved only upon binding to their natural ligands. This feature implies the folding of IDPs to be generally coupled with a binding event, representing an interesting challenge for kinetic studies. In this review, we recapitulate some of the most important findings of IDPs binding-induced folding mechanisms obtained by analyzing their binding kinetics. Furthermore, by focusing on the interaction between the Measles virus N TAIL protein, a prototypical IDP, and its physiological partner, the X domain, we recapitulate the major theoretical and experimental approaches that were used to describe binding induced folding., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

7. Mechanism of Folding and Binding of the N-Terminal SH2 Domain from SHP2.

Author

Bonetti D, Troilo F, Toto A, Travaglini-Allocatelli C, Brunori M, and Gianni S

Subjects

Humans, Protein Binding, Protein Tyrosine Phosphatase, Non-Receptor Type 11 isolation & purification, Protein Tyrosine Phosphatase, Non-Receptor Type 11 metabolism, Protein Folding, Protein Tyrosine Phosphatase, Non-Receptor Type 11 chemistry, src Homology Domains

Abstract

SHP2 is a phosphatase protein, involved in many cellular pathways, comprising two SH2 domains (namely N-SH2 and C-SH2) and a phosphatase domain. Among others, the interaction between SHP2 and Gab2 (Grb2 associated binder) is critical in cell death and differentiation. SHP2 binds to Gab2 through its SH2 domains, which recognize specific regions of Gab2 characterized by the presence of a phosphorylated tyrosine. In order to shed light on the dynamic and functional properties of this protein-protein interaction, we studied the mechanism of folding of N-SH2 and the binding process to a peptide mimicking a region of Gab2. The data presented represent the first description by stopped-flow of the kinetics of binding of an SH2 domain in solution. By performing experiments at different ionic strengths, we elucidate the electrostatic nature of the interaction, highlighting a key role of the negative charge of the phosphotyrosine in the recognition event of the reaction. Furthermore, by analyzing the equilibrium and kinetics of folding of N-SH2 folding we demonstrate the presence of an intermediate along the folding pathway. These results are discussed in the light of previous works on another SH2 domain.

Published

2018

8. How Robust Is the Mechanism of Folding-Upon-Binding for an Intrinsically Disordered Protein?

Author

Bonetti D, Troilo F, Brunori M, Longhi S, and Gianni S

Subjects

Models, Molecular, Nucleocapsid Proteins, Nucleoproteins chemistry, Nucleoproteins metabolism, Phosphoproteins chemistry, Phosphoproteins metabolism, Protein Binding, Protein Domains, Viral Proteins chemistry, Viral Proteins metabolism, Intrinsically Disordered Proteins chemistry, Intrinsically Disordered Proteins metabolism, Protein Folding

Abstract

The mechanism of interaction of an intrinsically disordered protein (IDP) with its physiological partner is characterized by a disorder-to-order transition in which a recognition and a binding step take place. Even if the mechanism is quite complex, IDPs tend to bind their partner in a cooperative manner such that it is generally possible to detect experimentally only the disordered unbound state and the structured complex. The interaction between the disordered C-terminal domain of the measles virus nucleoprotein (N TAIL ) and the X domain (XD) of the viral phosphoprotein allows us to detect and quantify the two distinct steps of the overall reaction. Here, we analyze the robustness of the folding of N TAIL upon binding to XD by measuring the effect on both the folding and binding steps of N TAIL when the structure of XD is modified. Because it has been shown that wild-type XD is structurally heterogeneous, populating an on-pathway intermediate under native conditions, we investigated the binding to 11 different site-directed variants of N TAIL of one particular variant of XD (I504A XD) that populates only the native state. Data reveal that the recognition and the folding steps are both affected by the structure of XD, indicating a highly malleable pathway. The experimental results are briefly discussed in the light of previous experiments on other IDPs., (Copyright © 2018 Biophysical Society. Published by Elsevier Inc. All rights reserved.)

Published

2018

9. Analyzing the Folding and Binding Steps of an Intrinsically Disordered Protein by Protein Engineering.

Author

Bonetti D, Troilo F, Toto A, Brunori M, Longhi S, and Gianni S

Subjects

Intrinsically Disordered Proteins genetics, Measles virus genetics, Nucleocapsid Proteins, Nucleoproteins genetics, Protein Domains, Viral Proteins genetics, Intrinsically Disordered Proteins chemistry, Measles virus chemistry, Nucleoproteins chemistry, Protein Engineering, Protein Folding, Viral Proteins chemistry

Abstract

Intrinsically disordered proteins (IDPs) are functionally active despite lacking a well-defined three-dimensional structure. Such proteins often undergo a disorder-to-order transition, or induced folding, when binding to their specific physiological partner. Because of cooperativity, the folding and binding steps typically appear as a single event, and therefore, induced folding is extremely difficult to characterize experimentally. In this perspective, the interaction between the disordered C-terminal domain of the measles virus nucleoprotein N TAIL and the folded X domain of the viral phosphoprotein (XD) is particularly interesting because the inherent complexity of the observed kinetics allows characterization of the binding and folding steps individually. Here we present a detailed structural description of the folding and binding events occurring in the recognition between N TAIL and XD. This result was achieved by measuring the effect of single-amino acid substitutions in N TAIL on the reaction mechanism. Analysis of the experimental data allowed us (i) to identify the key residues involved in the initial recognition between the two molecules and (ii) to depict the general features of the folding pathway of N TAIL . Furthermore, an analysis of the changes in stability obtained for the whole set of variants highlights how the sequence of this IDP has not been selected during evolution to fold efficiently. This feature might be a consequence of the weakly funneled nature of the energy landscape of IDPs in their unbound state and represents a plausible explanation of their highly dynamic nature even in the bound state, typically defined as "fuzziness".

Published

2017

10. The Folding Pathway of the KIX Domain.

Author

Troilo F, Bonetti D, Toto A, Visconti L, Brunori M, Longhi S, and Gianni S

Subjects

Binding Sites genetics, Humans, Mutagenesis, Site-Directed, Protein Denaturation, Protein Domains genetics, Protein Domains physiology, Proteostasis Deficiencies genetics, Metabolic Networks and Pathways, Protein Folding

Abstract

The KIX domain is an 89-residues globular domain with an important role in mediating protein-protein interactions. The presence of two distinct binding sites in such a small domain makes KIX a suitable candidate to investigate the effect of the potentially divergent demands between folding and function. Here, we report an extensive mutational analysis of the folding pathway of the KIX domain, based on 30 site-directed mutants, which allow us to assess the structures of both the transition and denatured states. Data reveal that, while the transition state presents mostly native-like interactions, the denatured state is somewhat misfolded. We mapped some of the non-native contacts in the denatured state using a second round of mutagenesis, based on double mutant cycles on 15 double mutants. Interestingly, such a misfolding arises from non-native interactions involving the residues critical for the function of the protein. The results described in this work appear to highlight the diverging demands between folding and function that may lead to misfolding, which may be observed in the early stages of folding.

Published

2017