Your search keyword '"Pomarici ND"' showing total 10 results

1. PEP-Patch: Electrostatics in Protein-Protein Recognition, Specificity, and Antibody Developability.

Author

Hoerschinger VJ, Waibl F, Pomarici ND, Loeffler JR, Deane CM, Georges G, Kettenberger H, Fernández-Quintero ML, and Liedl KR

Subjects

Static Electricity, Solubility, Viscosity, Proteins chemistry, Antibodies

Abstract

The electrostatic properties of proteins arise from the number and distribution of polar and charged residues. Electrostatic interactions in proteins play a critical role in numerous processes such as molecular recognition, protein solubility, viscosity, and antibody developability. Thus, characterizing and quantifying electrostatic properties of a protein are prerequisites for understanding these processes. Here, we present PEP-Patch, a tool to visualize and quantify the electrostatic potential on the protein surface in terms of surface patches, denoting separated areas of the surface with a common physical property. We highlight its applicability to elucidate protease substrate specificity and antibody-antigen recognition and predict heparin column retention times of antibodies as an indicator of pharmacokinetics.

Published

2023

2. Structure and Dynamics Guiding Design of Antibody Therapeutics and Vaccines.

Author

Fernández-Quintero ML, Pomarici ND, Fischer AM, Hoerschinger VJ, Kroell KB, Riccabona JR, Kamenik AS, Loeffler JR, Ferguson JA, Perrett HR, Liedl KR, Han J, and Ward AB

Abstract

Antibodies and other new antibody-like formats have emerged as one of the most rapidly growing classes of biotherapeutic proteins. Understanding the structural features that drive antibody function and, consequently, their molecular recognition is critical for engineering antibodies. Here, we present the structural architecture of conventional IgG antibodies alongside other formats. We emphasize the importance of considering antibodies as conformational ensembles in solution instead of focusing on single-static structures because their functions and properties are strongly governed by their dynamic nature. Thus, in this review, we provide an overview of the unique structural and dynamic characteristics of antibodies with respect to their antigen recognition, biophysical properties, and effector functions. We highlight the numerous technical advances in antibody structure prediction and design, enabled by the vast number of experimentally determined high-quality structures recorded with cryo-EM, NMR, and X-ray crystallography. Lastly, we assess antibody and vaccine design strategies in the context of structure and dynamics.

Published

2023

3. Evolution of the Immunoglobulin Isotypes-Variations of Biophysical Properties among Animal Classes.

Author

Pomarici ND, Cacciato R, Kokot J, Fernández-Quintero ML, and Liedl KR

Subjects

Animals, Antibodies, Vertebrates genetics, Fishes, Immunoglobulin Isotypes genetics, Evolution, Molecular

Abstract

The adaptive immune system arose around 500 million years ago in jawed fish, and, since then, it has mediated the immune defense against pathogens in all vertebrates. Antibodies play a central role in the immune reaction, recognizing and attacking external invaders. During the evolutionary process, several immunoglobulin isotypes emerged, each having a characteristic structural organization and dedicated function. In this work, we investigate the evolution of the immunoglobulin isotypes, in order to highlight the relevant features that were preserved over time and the parts that, instead, mutated. The residues that are coupled in the evolution process are often involved in intra- or interdomain interactions, meaning that they are fundamental to maintaining the immunoglobulin fold and to ensuring interactions with other domains. The explosive growth of available sequences allows us to point out the evolutionary conserved residues and compare the biophysical properties among different animal classes and isotypes. Our study offers a general overview of the evolution of immunoglobulin isotypes and advances the knowledge of their characteristic biophysical properties, as a first step in guiding protein design from evolution.

Published

2023

4. Structural mechanism of Fab domain dissociation as a measure of interface stability.

Author

Pomarici ND, Waibl F, Quoika PK, Bujotzek A, Georges G, Fernández-Quintero ML, and Liedl KR

Subjects

Immunoglobulin Fab Fragments chemistry, Immunoglobulin Fab Fragments metabolism, Antibodies

Abstract

Therapeutic antibodies should not only recognize antigens specifically, but also need to be free from developability issues, such as poor stability. Thus, the mechanistic understanding and characterization of stability are critical determinants for rational antibody design. In this study, we use molecular dynamics simulations to investigate the melting process of 16 antigen binding fragments (Fabs). We describe the Fab dissociation mechanisms, showing a separation in the V H -V L and in the C H 1-C L domains. We found that the depths of the minima in the free energy curve, corresponding to the bound states, correlate with the experimentally determined melting temperatures. Additionally, we provide a detailed structural description of the dissociation mechanism and identify key interactions in the CDR loops and in the C H 1-C L interface that contribute to stabilization. The dissociation of the V H -V L or C H 1-C L domains can be represented by conformational changes in the bend angles between the domains. Our findings elucidate the melting process of antigen binding fragments and highlight critical residues in both the variable and constant domains, which are also strongly germline dependent. Thus, our proposed mechanisms have broad implications in the development and design of new and more stable antigen binding fragments., (© 2023. The Author(s).)

Published

2023

5. Bispecific antibodies-effects of point mutations on CH3-CH3 interface stability.

Author

Pomarici ND, Fernández-Quintero ML, Quoika PK, Waibl F, Bujotzek A, Georges G, and Liedl KR

Subjects

Point Mutation, Immunoglobulin G genetics, Binding Sites, Antibodies, Bispecific chemistry

Abstract

A new format of therapeutic proteins is bispecific antibodies, in which two different heavy chains heterodimerize to obtain two different binding sites. Therefore, it is crucial to understand and optimize the third constant domain (CH3-CH3) interface to favor heterodimerization over homodimerization, and to preserve the physicochemical properties, as thermal stability. Here, we use molecular dynamics simulations to investigate the dissociation process of 19 CH3-CH3 crystal structures that differ from each other in few point mutations. We describe the dissociation of the dimeric interface as a two-steps mechanism. As confirmed by a Markov state model, apart from the bound and the dissociated state, we observe an additional intermediate state, which corresponds to an encounter complex. The analysis of the interdomain contacts reveals key residues that stabilize the interface. We expect that our results will improve the understanding of the CH3-CH3 interface interactions and thus advance the developability and design of new antibodies formats., (© The Author(s) 2022. Published by Oxford University Press.)

Published

2022

6. Corrigendum: Comparing Antibody Interfaces to Inform Rational Design of New Antibody Formats.

Author

Fernández-Quintero ML, Quoika PK, Wedl FS, Seidler CA, Kroell KB, Loeffler JR, Pomarici ND, Hoerschinger VJ, Bujotzek A, Georges G, Kettenberger H, and Liedl KR

Abstract

[This corrects the article DOI: 10.3389/fmolb.2022.812750.]., (Copyright © 2022 Fernández-Quintero, Quoika, Wedl, Seidler, Kroell, Loeffler, Pomarici, Hoerschinger, Bujotzek, Georges, Kettenberger and Liedl.)

Published

2022

7. Comparing Antibody Interfaces to Inform Rational Design of New Antibody Formats.

Author

Fernández-Quintero ML, Quoika PK, Wedl FS, Seidler CA, Kroell KB, Loeffler JR, Pomarici ND, Hoerschinger VJ, Bujotzek A, Georges G, Kettenberger H, and Liedl KR

Abstract

As the current biotherapeutic market is dominated by antibodies, the design of different antibody formats, like bispecific antibodies and other new formats, represent a key component in advancing antibody therapy. When designing new formats, a targeted modulation of pairing preferences is key. Several existing approaches are successful, but expanding the repertoire of design possibilities would be desirable. Cognate immunoglobulin G antibodies depend on homodimerization of the fragment crystallizable regions of two identical heavy chains. By modifying the dimeric interface of the third constant domain (C H 3-C H 3), with different mutations on each domain, the engineered Fc fragments form rather heterodimers than homodimers. The first constant domain (C H 1-C L ) shares a very similar fold and interdomain orientation with the C H 3-C H 3 dimer. Thus, numerous well-established design efforts for C H 3-C H 3 interfaces, have also been applied to C H 1-C L dimers to reduce the number of mispairings in the Fabs. Given the high structural similarity of the C H 3-C H 3 and C H 1-C L domains we want to identify additional opportunities in comparing the differences and overlapping interaction profiles. Our vision is to facilitate a toolkit that allows for the interchangeable usage of different design tools from crosslinking the knowledge between these two interface types. As a starting point, here, we use classical molecular dynamics simulations to identify differences of the C H 3-C H 3 and C H 1-C L interfaces and already find unexpected features of these interfaces shedding new light on possible design variations. Apart from identifying clear differences between the similar C H 3-C H 3 and C H 1-C L dimers, we structurally characterize the effects of point-mutations in the C H 3-C H 3 interface on the respective dynamics and interface interaction patterns. Thus, this study has broad implications in the field of antibody engineering as it provides a structural and mechanistical understanding of antibody interfaces and thereby presents a crucial aspect for the design of bispecific antibodies., Competing Interests: Authors AB, GG and HK were employed by the company Roche. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Fernández-Quintero, Quoika, Wedl, Seidler, Kroell, Loeffler, Pomarici, Hoerschinger, Bujotzek, Georges, Kettenberger and Liedl.)

Published

2022

8. Antibodies exhibit multiple paratope states influencing V H -V L domain orientations.

Author

Fernández-Quintero ML, Pomarici ND, Math BA, Kroell KB, Waibl F, Bujotzek A, Georges G, and Liedl KR

Subjects

Antibodies immunology, Immunoglobulin Fab Fragments chemistry, Immunoglobulin Fab Fragments immunology, Immunoglobulin Heavy Chains immunology, Immunoglobulin Light Chains immunology, Immunoglobulin Variable Region immunology, Molecular Docking Simulation, Molecular Dynamics Simulation, Protein Binding, Protein Conformation, Antibodies chemistry, Binding Sites, Antibody, Immunoglobulin Heavy Chains chemistry, Immunoglobulin Light Chains chemistry, Immunoglobulin Variable Region chemistry, Protein Interaction Domains and Motifs

Abstract

In the last decades, antibodies have emerged as one of the most important and successful classes of biopharmaceuticals. The highest variability and diversity of an antibody is concentrated on six hypervariable loops, also known as complementarity determining regions (CDRs) shaping the antigen-binding site, the paratope. Whereas it was assumed that certain sequences can only adopt a limited set of backbone conformations, in this study we present a kinetic classification of several paratope states in solution. Using molecular dynamics simulations in combination with experimental structural information we capture the involved conformational transitions between different canonical clusters and additional dominant solution structures occurring in the micro-to-millisecond timescale. Furthermore, we observe a strong correlation of CDR loop movements. Another important aspect when characterizing different paratope states is the relative V H /V L orientation and the influence of the distinct CDR loop states on the V H /V L interface. Conformational rearrangements of the CDR loops do not only have an effect on the relative V H /V L orientations, but also influence in some cases the elbow-angle dynamics and shift the respective distributions. Thus, our results show that antibodies exist as several interconverting paratope states, each contributing to the antibody's properties.

Published

2020

9. T-Cell Receptor CDR3 Loop Conformations in Solution Shift the Relative Vα-Vβ Domain Distributions.

Author

Fernández-Quintero ML, Pomarici ND, Loeffler JR, Seidler CA, and Liedl KR

Subjects

Adaptive Immunity, Animals, Antigens metabolism, Complementarity Determining Regions genetics, Complementarity Determining Regions metabolism, Crystallography, X-Ray, Histocompatibility Antigens metabolism, Humans, Molecular Dynamics Simulation, Peptides metabolism, Protein Binding, Protein Conformation, Protein Domains genetics, Receptors, Antigen, T-Cell, alpha-beta genetics, Receptors, Antigen, T-Cell, alpha-beta metabolism, Structure-Activity Relationship, T-Cell Antigen Receptor Specificity, Complementarity Determining Regions chemistry, Receptors, Antigen, T-Cell, alpha-beta chemistry

Abstract

T-cell receptors are an important part in the adaptive immune system as they are responsible for detecting foreign proteins presented by the major histocompatibility complex (MHC). The affinity is predominantly determined by structure and sequence of the complementarity determining regions (CDRs), of which the CDR3 loops are responsible for peptide recognition. We present a kinetic classification of T-cell receptor CDR3 loops with different loop lengths into canonical and non-canonical solution structures. Using molecular dynamics simulations, we do not only sample available X-ray structures, but we also observe a substantially broader CDR3 loop ensemble with various distinct kinetic minima in solution. Our results strongly imply, that for given CDR3 loop sequences several canonical structures have to be considered to characterize the conformational diversity of these loops. Our suggested dominant solution structures could extend the repertoire of available canonical clusters by including kinetic minimum structures present in solution. Thus, the CDR3 loops need to be characterized as conformational ensembles in solution. Furthermore, the conformational changes of the CDR3 loops follow the paradigm of conformational selection, because the experimentally determined binding competent state is present within this ensemble of pre-existing conformations without the presence of the antigen. We also identify strong correlations between the CDR3 loops and include combined state descriptions. Additionally, we observe a strong dependency of the CDR3 loop conformations on the relative Vα-Vβ interdomain orientations, revealing that certain CDR3 loop states favor specific interface orientations., (Copyright © 2020 Fernández-Quintero, Pomarici, Loeffler, Seidler and Liedl.)

Published

2020

10. Antibody CDR loops as ensembles in solution vs. canonical clusters from X-ray structures.

Author

Fernández-Quintero ML, Heiss MC, Pomarici ND, Math BA, and Liedl KR

Subjects

Animals, Crystallography, X-Ray methods, Humans, Molecular Dynamics Simulation, Complementarity Determining Regions chemistry, Protein Conformation

Abstract

In the past decade, the relevance of antibodies as therapeutics has increased substantially. Therefore, structural and functional characterization, in particular of the complementarity-determining regions (CDRs), is crucial to the design and engineering of antibodies with unique binding properties. Various studies have focused on classifying the CDR loops into a small set of main-chain conformations to facilitate antibody design by assuming that certain sequences can only adopt a limited number of conformations. Here, we present a kinetic classification of CDR loop structures as ensembles in solution. Using molecular dynamics simulations in combination with strong experimental structural information, we observe conformational transitions between canonical clusters and additional dominant solution structures in the micro-to-millisecond timescale for all CDR loops, independent of length and sequence composition. Besides identifying all relevant conformations in solution, our results revealed that various canonical cluster medians actually belong to the same kinetic minimum. Additionally, we reconstruct the kinetics and probabilities of the conformational transitions between canonical clusters, and thereby extend the model of static canonical structures to reveal a dynamic conformational ensemble in solution as a new paradigm in the field of antibody structure design. Abbreviations: CDR: Complementary-determining region; Fv: Antibody variable fragment; PCCA: Perron cluster analysis; tICA: Time-lagged independent component analysis; V H : Heavy chain variable region; V L : Light chain variable region.

Published

2020