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182 results on '"Jamieson, Andrew G"'

4. Hydroxamic Acid-Modified Peptide Library Provides Insights into the Molecular Basis for the Substrate Selectivity of HDAC Corepressor Complexes

Author

Archibald, Lewis J., Brown, Edward A., Millard, Christopher J., Watson, Peter J., Robertson, Naomi S., Wang, Siyu, Schwabe, John W. R., Jamieson, Andrew G., Jamieson, Andrew G [0000-0003-1726-7353], and Apollo - University of Cambridge Repository

Subjects
Histone Deacetylase Inhibitors, Histones, Peptide Library, Lysine, Humans, Molecular Medicine, General Medicine, Hydroxamic Acids, Peptides, Co-Repressor Proteins, Biochemistry, Histone Deacetylases
Abstract

Targeting the lysine deacetylase activity of class I histone deacetylases (HDACs) is potentially beneficial for the treatment of several diseases including human immunodeficiency virus (HIV) infection, Alzheimer's disease, and various cancers. It is therefore important to understand the function and mechanism of action of these enzymes. Class I HDACs act as catalytic components of seven large, multiprotein corepressor complexes. Different HDAC corepressor complexes have specific, nonredundant roles in the cell. It is likely that their specific functions are at least partly influenced by the substrate specificity of the complexes. To address this, we developed chemical tools to probe the specificity of HDAC complexes. We assessed a library of acetyl-lysine-containing substrate peptides and hydroxamic acid-containing inhibitor peptides against the full range of class I HDAC corepressor complexes. The results suggest that site-specific HDAC corepressor complex activity is driven in part by the recognition of the primary amino acid sequence surrounding a particular lysine position in the histone tail.

Published
2022
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5. Investigation of a new substrate directed aza-Claisen rearrangement for natural product synthesis

Author

Jamieson, Andrew G.

Subjects
547.2
Abstract

A novel substrate directed, palladium(II)-catalyst aza-Claisen rearrangement has been developed. Aza-Claisen rearrangement of a series of delta-ether substituted allylic trichloroacetimidates demonstrated that the oxygen atom in this position can effectively direct facial coordination of the palladium(II)-catalyst, with the MOM-ether substrate giving the most selective rearrangement reaction. An optimisation study was carried out using different catalysts and reaction conditions. The results from this study showed that bis(acetonitrile)palladium(II) chloride catalyst and non-coordinating solvents such as toluene give the most selective rearrangement resulting in the isolation of the anti-compound in up to 88% diastereomeric excess. This methodology was used as the key step in the novel diastereoselective synthesis of beta-hydroxy alpha-amino acids from enantiopure alpha-hydroxy acids. During the rearrangement step, a competing [1,3] pathway catalysed by palladium(O) was suppressed using p-benzoquinone as an in-situ oxidant in the reaction mixture. A series of compounds based on the structure of the piperidine alkaloid (+)-alpha-conhydrine were synthesised using this newly developed ether-directed, palladium(II)-catalysed aza-Claisen rearrangement and a ring closing metathesis reaction as the key steps.

Published
2006

12. Investigating the Structure–Activity Relationship of 1,2,4-Triazine G-Protein-Coupled Receptor 84 (GPR84) Antagonists

Author

Mahindra, Amit, primary, Jenkins, Laura, additional, Marsango, Sara, additional, Huggett, Mark, additional, Huggett, Margaret, additional, Robinson, Lindsay, additional, Gillespie, Jonathan, additional, Rajamanickam, Muralikrishnan, additional, Morrison, Angus, additional, McElroy, Stuart, additional, Tikhonova, Irina G., additional, Milligan, Graeme, additional, and Jamieson, Andrew G., additional

Published
2022
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14. Stapled ACE2 peptidomimetics designed to target the SARS-CoV-2 spike protein do not prevent virus internalisation

Author

Morgan, Danielle C., Morris, Caroline, Mahindra, Amit, Blair, Connor M., Tejeda, Gonzalo, Herbert, Imogen, Turnbull, Matthew L., Lieber, Gauthier, Willett, Brian J., Logan, Nicola, Smith, Brian, Tobin, Andrew B., Bhella, David, Baillie, George S., and Jamieson, Andrew G.

Subjects
viruses, hormones, hormone substitutes, and hormone antagonists
Abstract

COVID‐19 is caused by a novel coronavirus called severe acute respiratory syndrome‐coronavirus 2 (SARS‐CoV‐2). Virus cell entry is mediated through a protein‐protein interaction (PPI) between the SARS‐CoV‐2 spike protein and angiotensin‐converting enzyme 2 (ACE2). A series of stapled peptide ACE2 peptidomimetics based on the ACE2 interaction motif were designed to bind the coronavirus S‐protein RBD and inhibit binding to the human ACE2 receptor. The peptidomimetics were assessed for antiviral activity in an array of assays including a neutralization pseudovirus assay, immunofluorescence (IF) assay and in‐vitro fluorescence polarization (FP) assay. However, none of the peptidomimetics showed activity in these assays, suggesting that an enhanced binding interface is required to outcompete ACE2 for S‐protein RBD binding and prevent virus internalization.

Published
2021

15. Peptides derived from the SARS-CoV-2 receptor binding motif bind to ACE2 but do not block ACE2-mediated host cell entry or pro-inflammatory cytokine induction

Author

Mahindra, Amit, primary, Tejeda, Gonzalo, additional, Rossi, Mario, additional, Janha, Omar, additional, Herbert, Imogen, additional, Morris, Caroline, additional, Morgan, Danielle C., additional, Beattie, Wendy, additional, Montezano, Augusto C., additional, Hudson, Brian, additional, Tobin, Andrew B., additional, Bhella, David, additional, Touyz, Rhian M., additional, Jamieson, Andrew G., additional, Baillie, George S., additional, and Blair, Connor M., additional

Published
2021
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24. Synthesis of HDAC substrate peptidomimetic inhibitors (SPIs) using Fmoc amino acids incorporating zinc-binding groups

Author

Mahindra, Amit, Millard, Christopher J., Black, Iona, Archibald, Lewis J., Schwabe, John W.R., and Jamieson, Andrew G.

Abstract

Syntheses of Fmoc amino acids having zinc-binding groups were prepared and incorporated into substrate inhibitor H3K27 peptides using Fmoc/tBu solid-phase peptide synthesis (SPPS). Peptide 11, prepared using Fmoc-Asu(NHOtBu)-OH, is a potent inhibitor (IC50 = 390 nM) of the core NuRD corepressor complex (HDAC1–MTA1–RBBP4). The Fmoc amino acids have the potential to facilitate the rapid preparation of substrate peptidomimetic inhibitor (SPI) libraries in the search for selective HDAC inhibitors.

Published
2019

25. Validation of the protein kinase Pf CLK3 as a multistage cross-species malarial drug target

Author

Alam, Mahmood M., primary, Sanchez-Azqueta, Ana, additional, Janha, Omar, additional, Flannery, Erika L., additional, Mahindra, Amit, additional, Mapesa, Kopano, additional, Char, Aditya B., additional, Sriranganadane, Dev, additional, Brancucci, Nicolas M. B., additional, Antonova-Koch, Yevgeniya, additional, Crouch, Kathryn, additional, Simwela, Nelson Victor, additional, Millar, Scott B., additional, Akinwale, Jude, additional, Mitcheson, Deborah, additional, Solyakov, Lev, additional, Dudek, Kate, additional, Jones, Carolyn, additional, Zapatero, Cleofé, additional, Doerig, Christian, additional, Nwakanma, Davis C., additional, Vázquez, Maria Jesús, additional, Colmenarejo, Gonzalo, additional, Lafuente-Monasterio, Maria Jose, additional, Leon, Maria Luisa, additional, Godoi, Paulo H. C., additional, Elkins, Jon M., additional, Waters, Andrew P., additional, Jamieson, Andrew G., additional, Álvaro, Elena Fernández, additional, Ranford-Cartwright, Lisa C., additional, Marti, Matthias, additional, Winzeler, Elizabeth A., additional, Gamo, Francisco Javier, additional, and Tobin, Andrew B., additional

Published
2019
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30. μ‐Conotoxin KIIIA peptidomimetics that block human voltage‐gated sodium channels.

Author

Knuhtsen, Astrid, Whiting, Rachel, McWhinnie, Fergus S., Whitmore, Charlotte, Smith, Brian O., Green, A. Christopher, Timperley, Christopher M., Kinnear, Kenneth I., and Jamieson, Andrew G.

Subjects
PEPTIDOMIMETICS, PYRETHROIDS, SODIUM channels, ANALGESICS, HUMAN beings
Abstract

Peptidomimetics designed to target voltage‐gated sodium channels have attracted significant attention as potential analgesics. However, voltage‐gated sodium channel (VGSC)‐blocking activity of these compounds has mainly been assessed using rat and/or mice homologs. In this study, we developed a novel series of conformationally constrained peptidomimetic analogues of the μ‐conotoxin KIIIA and assessed their activity against human VGSCs. Two of the mimetics block the currents of hNav1.4 and hNav1.6 channels. NMR derived structures of the mimetics provided excellent insight into the structural requirements for bioactivity. A lactam‐constrained analogue, previously reported to be active in mice, did not block the corresponding human VGSC. This work highlights important differences in VGSCs between species and validates the potential of peptidomimetics as human analgesics. [ABSTRACT FROM AUTHOR]

Published
2021
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31. A short peptide that preferentially binds c-MYC G-quadruplex DNA.

Author

Minard, Aisling, Morgan, Danielle, Raguseo, Federica, Di Porzio, Anna, Liano, Denise, Jamieson, Andrew G., and Di Antonio, Marco

Subjects
DNA, HUMAN genome, DNA structure, CRYSTAL structure
Abstract

G-quadruplexes (G4s) are non-canonical DNA secondary structures. The identification of selective tools to probe individual G4s over the ∼700 000 found in the human genome is key to unravel the biological significance of specific G4s. We took inspiration from a crystal structure of the bovine DHX36 helicase bound to the G4 formed in the promoter region of the oncogene c-MYC to identify a short peptide that preferentially binds MYC G4 with nM affinity over a small panel of parallel and non-parallel G4s tested. [ABSTRACT FROM AUTHOR]

Published
2020
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32. Validation of the protein kinase PfCLK3 as a multi-stage cross species malarial drug target

Author

Alam, Mahmood M, primary, Sanchez-Azqueta, Ana, additional, Janha, Omar, additional, Flannery, Erika L., additional, Mahindra, Amit, additional, Mapesa, Kopano, additional, Brancucci, Nicolas, additional, Antonova-Koch, Yevgeniya, additional, Crouch, Kathryn, additional, Simwela, Nelson Victor, additional, Akinwale, Jude, additional, Mitcheson, Deborah, additional, Solyakov, Lev, additional, Dudek, Kate, additional, Jones, Carolyn, additional, Zapatero, Cleofé, additional, Doerig, Christian, additional, Nwakanma, Davis C., additional, Jesús Vázquez, Maria, additional, Colmenarejo, Gonzalo, additional, Jesús Lafuente, Maria, additional, Leon, Maria Luisa, additional, Waters, Andrew P., additional, Jamieson, Andrew G., additional, Fernandez Alvaro, León Elena, additional, Marti, Matthias, additional, Winzeler, Elizabeth A., additional, Gamo, Francisco Javier, additional, and Tobin, Andrew B., additional

Published
2018
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35. Insights into the activation mechanism of class I HDAC complexes by inositol phosphates

Author

Watson, Peter J., Millard, Christopher J., Riley, Andrew M., Robertson, Naomi S., Wright, Lyndsey C., Godage, Himali Y., Cowley, Shaun M., Jamieson, Andrew G., Potter, Barry V. L., and Schwabe, John W. R.

Subjects
Binding Sites, Science, Inositol Phosphates, Histone Deacetylase 1, Crystallography, X-Ray, Article, Histone Deacetylases, Enzyme Activation, Molecular Docking Simulation, QH345, HEK293 Cells, Allosteric Regulation, Protein Domains, Catalytic Domain, Multiprotein Complexes, Humans, QD, Protein Binding
Abstract

Histone deacetylases (HDACs) 1, 2 and 3 form the catalytic subunit of several large transcriptional repression complexes. Unexpectedly, the enzymatic activity of HDACs in these complexes has been shown to be regulated by inositol phosphates, which bind in a pocket sandwiched between the HDAC and co-repressor proteins. However, the actual mechanism of activation remains poorly understood. Here we have elucidated the stereochemical requirements for binding and activation by inositol phosphates, demonstrating that activation requires three adjacent phosphate groups and that other positions on the inositol ring can tolerate bulky substituents. We also demonstrate that there is allosteric communication between the inositol-binding site and the active site. The crystal structure of the HDAC1:MTA1 complex bound to a novel peptide-based inhibitor and to inositol hexaphosphate suggests a molecular basis of substrate recognition, and an entropically driven allosteric mechanism of activation., Class I histone deacetylase complexes can be activated by inositol phosphates. Here, the authors investigate the stereochemical requirements for activation; use the crystal structure to understand substrate recognition, and suggest an entropically driven mechanism of allostery.

Published
2016
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36. Positional scanning for peptide secondary structure by systematic solid-phase synthesis of amino lactam peptides

Author

Jamieson, Andrew G., Boutard, Nicolas, Beauregard, Kim, Bodas, Mandar S., Huy Ong, Quiniou, Christiane, Chemtob, Sylvain, and Lubell, William D.

Subjects
Allosteric enzymes -- Structure, Allosteric enzymes -- Chemical properties, Amines -- Chemical properties, Peptides -- Chemical properties, Peptides -- Structure, Chemistry
Abstract

A solid-phase method using a Fmoc-protection strategy is developed for preparing peptides containing configurationally defined [alpha]- [beta]-amino [gamma]-lactams. The method has proved useful for the rapid identification of the secondary structure required for peptide biological activity, by considering the potential for amino lactams to induce peptide turn conformations.

Published
2009

41. The ansamycin antibiotic, rifamycin SV, inhibits BCL6 transcriptional repression and forms a complex with the BCL6-BTB/POZ domain

Author

Evans, Sian E, Goult, Benjamin T, Fairall, Louise, Jamieson, Andrew G, Ko Ferrigno, Paul, Ford, Robert, Schwabe, John W R, Wagner, Simon D, Evans, Sian E, Goult, Benjamin T, Fairall, Louise, Jamieson, Andrew G, Ko Ferrigno, Paul, Ford, Robert, Schwabe, John W R, and Wagner, Simon D

Abstract

BCL6 is a transcriptional repressor that is over-expressed due to chromosomal translocations, or other abnormalities, in ~40% of diffuse large B-cell lymphoma. BCL6 interacts with co-repressor, SMRT, and this is essential for its role in lymphomas. Peptide or small molecule inhibitors, which prevent the association of SMRT with BCL6, inhibit transcriptional repression and cause apoptosis of lymphoma cells in vitro and in vivo. In order to discover compounds, which have the potential to be developed into BCL6 inhibitors, we screened a natural product library. The ansamycin antibiotic, rifamycin SV, inhibited BCL6 transcriptional repression and NMR spectroscopy confirmed a direct interaction between rifamycin SV and BCL6. To further determine the characteristics of compounds binding to BCL6-POZ we analyzed four other members of this family and showed that rifabutin, bound most strongly. An X-ray crystal structure of the rifabutin-BCL6 complex revealed that rifabutin occupies a partly non-polar pocket making interactions with tyrosine58, asparagine21 and arginine24 of the BCL6-POZ domain. Importantly these residues are also important for the interaction of BLC6 with SMRT. This work demonstrates a unique approach to developing a structure activity relationship for a compound that will form the basis of a therapeutically useful BCL6 inhibitor.

Published
2014

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