Your search keyword '"Gabriella T. Heller"' showing total 8 results

1. A rationally designed bicyclic peptide remodels Aβ42 aggregation in vitro and reduces its toxicity in a worm model of Alzheimer’s disease

Author

Francesco Simone Ruggeri, Michele Perni, Michele Vendruscolo, Christian P. Haas, Francesco A. Aprile, Christopher M. Dobson, Thomas C. T. Michaels, Gabriella T. Heller, Tatsuya Ikenoue, Tuomas P. J. Knowles, Benedetta Mannini, Pietro Sormanni, Ryan Limbocker, Christoph Middel, Sormanni, Pietro [0000-0002-6228-2221], Ruggeri, Francesco [0000-0002-1232-1907], Knowles, Tuomas [0000-0002-7879-0140], Vendruscolo, Michele [0000-0002-3616-1610], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Amyloid, In silico, lcsh:Medicine, Plaque, Amyloid, Peptide, 010402 general chemistry, Protein Aggregation, Pathological, 01 natural sciences, Epitope, Article, 03 medical and health sciences, Alzheimer Disease, Animals, 631/92, Life Science, Caenorhabditis elegans, lcsh:Science, Binding selectivity, chemistry.chemical_classification, Amyloid beta-Peptides, Multidisciplinary, Bicyclic molecule, Drug discovery, lcsh:R, Rational design, 631/154, Small molecule, Chemical biology, Peptide Fragments, In vitro, 0104 chemical sciences, Disease Models, Animal, 030104 developmental biology, chemistry, Biochemistry, lcsh:Q

Abstract

Funder: Centre for Misfolding Diseases, Bicyclic peptides have great therapeutic potential since they can bridge the gap between small molecules and antibodies by combining a low molecular weight of about 2 kDa with an antibody-like binding specificity. Here we apply a recently developed in silico rational design strategy to produce a bicyclic peptide to target the C-terminal region (residues 31–42) of the 42-residue form of the amyloid β peptide (Aβ42), a protein fragment whose aggregation into amyloid plaques is linked with Alzheimer’s disease. We show that this bicyclic peptide is able to remodel the aggregation process of Aβ42 in vitro and to reduce its associated toxicity in vivo in a C. elegans worm model expressing Aβ42. These results provide an initial example of a computational approach to design bicyclic peptides to target specific epitopes on disordered proteins.

Published

2020

2. Small-molecule sequestration of amyloid-β as a drug discovery strategy for Alzheimer's disease

Author

Benedetta Mannini, Roberta Pierattelli, Thomas Löhr, Massimiliano Bonomi, Carlo Camilloni, Thomas C. T. Michaels, Francesco Simone Ruggeri, Gabriella T. Heller, Alfonso De Simone, Michele Vendruscolo, Francesco A. Aprile, Christopher M. Dobson, Ryan Limbocker, Michele Perni, Isabella C. Felli, Tuomas P. J. Knowles, Heller, Gabriella T [0000-0002-5672-0467], Aprile, Francesco A [0000-0002-5040-4420], Perni, Michele [0000-0001-7593-8376], Ruggeri, Francesco Simone [0000-0002-1232-1907], Mannini, Benedetta [0000-0001-6812-7348], Löhr, Thomas [0000-0003-2969-810X], Bonomi, Massimiliano [0000-0002-7321-0004], Camilloni, Carlo [0000-0002-9923-8590], De Simone, Alfonso [0000-0001-8789-9546], Felli, Isabella C [0000-0002-6018-9090], Pierattelli, Roberta [0000-0001-7755-0885], Knowles, Tuomas PJ [0000-0002-7879-0140], Dobson, Christopher M [0000-0002-5445-680X], Vendruscolo, Michele [0000-0002-3616-1610], Apollo - University of Cambridge Repository, Heller, G. T., Aprile, F. A., Michaels, T. C. T., Limbocker, R., Perni, M., Ruggeri, F. S., Mannini, B., Lohr, T., Bonomi, M., Camilloni, C., de Simone, A., Felli, I. C., Pierattelli, R., Knowles, T. P. J., Dobson, C. M., Vendruscolo, M., University of Cambridge [UK] (CAM), Imperial College London, Harvard University, Bioinformatique structurale - Structural Bioinformatics, Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS), Università degli Studi di Milano = University of Milan (UNIMI), University of Naples Federico II = Università degli studi di Napoli Federico II, Università degli Studi di Firenze = University of Florence (UniFI), Funding: G.T.H. is supported by the Gates Cambridge Trust and the Rosalind Franklin Research Fellowship at Newnham College, Cambridge, F.A.A. is supported by UK Research and Innovation (Future Leaders Fellowship MR/S033947/1) and the Alzheimer’s Society, UK (317, 511), R.L. is supported by the Gates Cambridge Trust, TCTM by Peterhouse, Cambridge and the Swiss National Science Foundation, and F.S.R. is supported by Darwin College and the Swiss National Foundation (grant numbers P300P2_171219 and P2ELP2_162116, respectively). We acknowledge ARCHER UK National Supercomputing Service under ARCHER Leadership project (grant number e510) and PRACE for awarding us access to MareNostrum at Barcelona Supercomputing Center (BSC), Spain for metadynamic metainference simulations. Parameterization of 10074-G5 was performed using resources provided by the Cambridge Service for Data Driven Discovery (CSD3) operated by the University of Cambridge Research Computing Service (www.csd3.cam.ac.uk), provided by Dell EMC and Intel using Tier-2 funding from the Engineering and Physical Sciences Research Council (capital grant EP/P020259/1), and DiRAC funding from the Science and Technology Facilities Council (www.dirac.ac.uk). MALDI mass spectrometry measurements were performed by L. Packman at the Protein and Nucleic Acid Chemistry Facility (PNAC) at the Department of Biochemistry, University of Cambridge. The NMR measurements were supported by the iNEXT H2020 Programme (EC contract no. 653706). OW450 C. elegans were donated by E. Nollen. BLI measurements were performed in the Biophysics facility at the Department of Biochemistry, University of Cambridge. The work was also supported by the Centre for Misfolding Diseases and the INCEPTION project ANR-16-CONV-0005., ANR-16-CONV-0005,INCEPTION,Institut Convergences pour l'étude de l'Emergence des Pathologies au Travers des Individus et des populatiONs(2016), Harvard University [Cambridge], Institut Pasteur [Paris]-Centre National de la Recherche Scientifique (CNRS), Università degli Studi di Milano [Milano] (UNIMI), University of Naples Federico II, and Università degli Studi di Firenze = University of Florence [Firenze] (UNIFI)

Subjects

Amyloid beta, In silico, Biophysics, Intrinsically disordered proteins, 03 medical and health sciences, 0302 clinical medicine, Alzheimer Disease, Drug Discovery, medicine, Humans, Life Science, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biochemistry [q-bio.BM], Molecular Biology, Research Articles, 030304 developmental biology, 0303 health sciences, Multidisciplinary, Amyloid beta-Peptides, biology, Drug discovery, Chemistry, SciAdv r-articles, Conformational entropy, Small molecule, Peptide Fragments, 3. Good health, Mechanism of action, biology.protein, Small molecule binding, medicine.symptom, Hydrophobic and Hydrophilic Interactions, 030217 neurology & neurosurgery, Research Article

Abstract

A small molecule binds to a disordered protein in its monomeric form, preventing its aggregation linked to Alzheimer’s disease., Disordered proteins are challenging therapeutic targets, and no drug is currently in clinical use that modifies the properties of their monomeric states. Here, we identify a small molecule (10074-G5) capable of binding and sequestering the intrinsically disordered amyloid-β (Aβ) peptide in its monomeric, soluble state. Our analysis reveals that this compound interacts with Aβ and inhibits both the primary and secondary nucleation pathways in its aggregation process. We characterize this interaction using biophysical experiments and integrative structural ensemble determination methods. We observe that this molecule increases the conformational entropy of monomeric Aβ while decreasing its hydrophobic surface area. We also show that it rescues a Caenorhabditis elegans model of Aβ-associated toxicity, consistent with the mechanism of action identified from the in silico and in vitro studies. These results illustrate the strategy of stabilizing the monomeric states of disordered proteins with small molecules to alter their behavior for therapeutic purposes.

Published

2020

3. Small molecule sequestration of amyloid-β as a drug discovery strategy for Alzheimer’s disease

Author

Francesco Simone Ruggeri, Michele Vendruscolo, Ryan Limbocker, Thomas C. T. Michaels, Isabella C. Felli, Thomas Löhr, Massimiliano Bonomi, Gabriella T. Heller, Roberta Pierattelli, Alfonso De Simone, Michele Perni, Christopher M. Dobson, Francesco A. Aprile, Tuomas P. J. Knowles, Carlo Camilloni, and Benedetta Mannini

Subjects

chemistry.chemical_classification, 0303 health sciences, biology, Drug discovery, In silico, Peptide, biology.organism_classification, Small molecule, In vitro, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Monomer, Mechanism of action, chemistry, medicine, Biophysics, medicine.symptom, 030217 neurology & neurosurgery, Caenorhabditis elegans, 030304 developmental biology

Abstract

Disordered proteins are challenging therapeutic targets, and no drug is currently in clinical use that has been shown to modify the properties of their monomeric states. Here, we identify a small molecule capable of binding and sequestering the amyloid-β peptide (Aβ) in its monomeric, soluble state. Our analysis reveals that this compound interacts with Aβ and inhibits both the primary and secondary nucleation pathways in its aggregation process. We characterise this interaction using biophysical experiments and integrative structural ensemble determination methods. We thus observe that this small molecule has the remarkable effect of increasing the conformational entropy of monomeric Aβ while decreasing its hydrophobic surface area. We then show that this small molecule rescues a Caenorhabditis elegans model of Aβ-associated toxicity in a manner consistent with the mechanism of action identified from the in silico and in vitro studies. These results provide an illustration of the strategy of targeting the monomeric states of disordered proteins with small molecules to alter their behaviour for therapeutic purposes.

Published

2019

4. Structural Ensemble Modulation upon Small-Molecule Binding to Disordered Proteins

Author

Gabriella T. Heller, Massimiliano Bonomi, Michele Vendruscolo, University of Cambridge [UK] (CAM), Heller, Gabrielle [0000-0002-5672-0467], Bonomi, Massimilano [0000-0002-7321-0004], Vendruscolo, Michele [0000-0002-3616-1610], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Models, Molecular, Protein Conformation, Entropy, structural ensembles, Computational biology, 010402 general chemistry, 01 natural sciences, drug discovery, 03 medical and health sciences, Structural Biology, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Molecular Biology, ComputingMilieux_MISCELLANEOUS, Physics, food and beverages, Proteins, Small molecule, 0104 chemical sciences, Intrinsically Disordered Proteins, Molecular Weight, small molecules, 030104 developmental biology, Small molecule binding, disordered proteins, Protein Binding

Abstract

Over the past decade, there has been a growing interest in investigating whether disordered proteins can be targeted for clinical purposes using small molecules [1] , [2] , [3] , [4] , [5] , [6] , [7] , [8] . While small-molecule binding to disordered proteins can be seen as unorthodox, examples of this phenomenon have been reported. In order to rationalize these observations, a variety of models are emerging, sometimes in apparent contradiction. Here, we offer a “structural ensemble modulation” view as an attempt to clarify the language, organize concepts, and facilitate the comparison of different studies. In doing so, we hope to promote the understanding of the general principles underlying this phenomenon toward the development of novel therapeutic compounds targeting disordered proteins, which are prevalent in a wide range of human diseases [1] , [2] , [3] , [4] , [5] , [6] , [7] , [8] .

Published

2017

5. Methods of probing the interactions between small molecules and disordered proteins

Author

Michele Vendruscolo, Francesco A. Aprile, Gabriella T. Heller, Heller, Gabrielle [0000-0002-5672-0467], Aprile, Francesco [0000-0002-5040-4420], Vendruscolo, Michele [0000-0002-3616-1610], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, binding, Fluorescence Polarization, 010402 general chemistry, 01 natural sciences, drugs, Small Molecule Libraries, 03 medical and health sciences, Cellular and Molecular Neuroscience, Multi-author Review, Two-Hybrid System Techniques, Scattering, Small Angle, Human proteome project, Fluorescence Resonance Energy Transfer, Humans, Molecular Biology, Pharmacology, Molecular interactions, Drug discovery, Chemistry, Circular Dichroism, Cell Biology, Surface Plasmon Resonance, Small molecule, 0104 chemical sciences, Intrinsically Disordered Proteins, small molecules, 030104 developmental biology, Order (biology), Biophysics, Molecular Medicine, disordered proteins, Protein Binding, molecular interactions

Abstract

It is generally recognized that a large fraction of the human proteome is made up of proteins that remain disordered in their native states. Despite the fact that such proteins play key biological roles and are involved in many major human diseases, they still represent challenging targets for drug discovery. A major bottleneck for the identification of compounds capable of interacting with these proteins and modulating their disease-promoting behaviour is the development of effective techniques to probe such interactions. The difficulties in carrying out binding measurements have resulted in a poor understanding of the mechanisms underlying these interactions. In order to facilitate further methodological advances, here we review the most commonly used techniques to probe three types of interactions involving small molecules: (1) those that disrupt functional interactions between disordered proteins; (2) those that inhibit the aberrant aggregation of disordered proteins, and (3) those that lead to binding disordered proteins in their monomeric states. In discussing these techniques, we also point out directions for future developments.

Published

2017

6. Sequence Specificity in the Entropy-Driven Binding of a Small Molecule and a Disordered Peptide

Author

Gabriella T. Heller, Carlo Camilloni, Alfonso De Simone, Massimiliano Bonomi, Francesco A. Aprile, Michele Vendruscolo, University of Cambridge [UK] (CAM), Università degli Studi di Milano [Milano] (UNIMI), Imperial College London, Heller, Gabrielle [0000-0002-5672-0467], Aprile, Francesco [0000-0002-5040-4420], Bonomi, Massimilano [0000-0002-7321-0004], Vendruscolo, Michele [0000-0002-3616-1610], Apollo - University of Cambridge Repository, Heller, G. T., Aprile, F. A., Bonomi, M., Camilloni, C., De Simone, A., and Vendruscolo, M.

Subjects

0301 basic medicine, Magnetic Resonance Spectroscopy, Entropy, Statistics as Topic, small molecule, specificity, Peptide, Plasma protein binding, 010402 general chemistry, 01 natural sciences, Molecular Docking Simulation, Biophysical Phenomena, Proto-Oncogene Proteins c-myc, 03 medical and health sciences, drug binding, Structural Biology, disordered protein, Human proteome project, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Molecular Biology, ComputingMilieux_MISCELLANEOUS, chemistry.chemical_classification, Intermolecular force, Nuclear magnetic resonance spectroscopy, Small molecule, 3. Good health, 0104 chemical sciences, small molecules, Thiazoles, 030104 developmental biology, Biochemistry, chemistry, Biophysics, Thiazole, disordered proteins, Human, Protein Binding

Abstract

Approximately one-third of the human proteome is made up of proteins that are entirely disordered or that contain extended disordered regions. Although these disordered proteins are closely linked with many major diseases, their binding mechanisms with small molecules remain poorly understood, and a major concern is whether their specificity can be sufficient for drug development. Here, by studying the interaction of a small molecule and a disordered peptide from the oncogene protein c-Myc, we describe a “specific-diffuse” binding mechanism that exhibits sequence specificity despite being of entropic nature. By combining NMR spectroscopy, biophysical measurements, statistical inference, and molecular simulations, we provide a quantitative measure of such sequence specificity and compare it to the case of the interaction of urea, which is diffuse but not specific. To investigate whether this type of binding can generally modify intermolecular interactions, we show that it leads to an inhibition of the aggregation of the peptide. These results suggest that the binding mechanism that we report may create novel opportunities to discover drugs that target disordered proteins in their monomeric states in a specific manner.

Published

2017

7. Probing Specificity in Disordered Protein Interactions with Small Molecules using Integrative Methods

Author

Massimiliano Bonomi, Alfonso De Simone, Francesco A. Aprile, Michele Vendruscolo, Gabriella T. Heller, and Carlo Camilloni

Subjects

Chemistry, Biophysics, Small molecule, Protein–protein interaction

Published

2019

8. Targeting disordered proteins with small molecules using entropy

Author

Michele Vendruscolo, Gabriella T. Heller, Pietro Sormanni, Heller, Gabrielle [0000-0002-5672-0467], Sormanni, Pietro [0000-0002-6228-2221], Vendruscolo, Michele [0000-0002-3616-1610], and Apollo - University of Cambridge Repository

Subjects

binding, Protein Conformation, Entropy, Intermolecular force, small molecule, Proteins, Plasma protein binding, Biochemistry, Small molecule, chemistry.chemical_compound, Monomer, Protein structure, chemistry, Computational chemistry, entropic expansion, Biophysics, Human proteome project, Thermodynamics, Molecular Biology, disordered proteins, Entropy (order and disorder), Protein Binding

Abstract

The human proteome includes many disordered proteins. Although these proteins are closely linked with a range of human diseases, no clinically approved drug targets them in their monomeric forms. This situation arises, at least in part, from the current lack of understanding of the mechanisms by which small molecules bind proteins that do not fold into well-defined conformations. To explore possible solutions to this problem, we discuss quite generally how an overall decrease in the free energy associated with intermolecular binding can originate from different combinations of enthalpic and entropic contributions. We then consider more specifically a mechanism of binding by which small molecules can affect the conformational space of a disordered protein by creating an entropic expansion in which more conformations of the protein become populated.

Published

2015