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142 results on '"Boyle, Louise H."'

25. TAPBPR bridges UDP-glucose: glycoprotein glucosyltransferase 1 onto MHC class I to provide quality control in the antigen presentation pathway

Author

Neerincx, Andreas, Hermann, Clemens, Antrobus, Robin, Van Hateren, Andrew, Cao, Huan, Trautwein, Nico, Stevanović, Stefan, Elliott, Tim, Deane, Janet E., and Boyle, Louise H.

Abstract

Recently, we revealed that TAPBPR is a peptide exchange catalyst that is important for optimal peptide selection by MHC class I molecules. Here, we asked whether any other co-factors associate with TAPBPR, which would explain its effect on peptide selection. We identify an interaction between TAPBPR and UDP-glucose:glycoprotein glucosyltransferase 1 (UGT1), a folding sensor in the calnexin/calreticulin quality control cycle that is known to regenerate the Glc1Man9GlcNAc2 moiety on glycoproteins. Our results suggest the formation of a multimeric complex, dependent on a conserved cysteine at position 94 in TAPBPR, in which TAPBPR promotes the association of UGT1 with peptide-receptive MHC class I molecules. We reveal that the interaction between TAPBPR and UGT1 facilities the reglucosylation of the glycan on MHC class I molecules, promoting their recognition by calreticulin. Our results suggest that in addition to being a peptide editor, TAPBPR improves peptide optimisation by promoting peptide-receptive MHC class I molecules to associate with the peptide-loading complex.

Published
2017

30. Author response: TAPBPR bridges UDP-glucose:glycoprotein glucosyltransferase 1 onto MHC class I to provide quality control in the antigen presentation pathway

Author

Neerincx, Andreas, primary, Hermann, Clemens, additional, Antrobus, Robin, additional, van Hateren, Andy, additional, Cao, Huan, additional, Trautwein, Nico, additional, Stevanović, Stefan, additional, Elliott, Tim, additional, Deane, Janet E, additional, and Boyle, Louise H, additional

Published
2017
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31. F pocket flexibility influences the tapasin dependence of two differentially disease-associated MHC Class I proteins

Author

Abualrous, Esam T, Fritzsche, Susanne, Hein, Zeynep, Al-Balushi, Mohammed S, Reinink, Peter, Boyle, Louise H, Wellbrock, Ursula, Antoniou, Antony N, Springer, Sebastian, Infection & Immunity, Risk Assessment, dI&I RA-I&I I&I, and LS Immunologie

Subjects
Models, Molecular, Protein Folding, Protein Conformation, Immunology, Peptide binding, Peptide, Molecular Dynamics Simulation, Major histocompatibility complex, Cell Line, Mice, Tapasin, MHC class I, Animals, Humans, Immunology and Allergy, Spondylitis, Ankylosing, Amino Acid Sequence, Binding site, HLA-B27 Antigen, chemistry.chemical_classification, Binding Sites, Base Sequence, biology, Membrane Transport Proteins, Sequence Analysis, DNA, Amino acid, chemistry, Biochemistry, biology.protein, Biophysics, Protein folding, Molecular Chaperones, Protein Binding
Abstract

The human major histocompatibility complex (MHC) class I protein HLA-B*27:05 is statistically associated with ankylosing spondylitis (AS), unlike HLA-B*27:09, which differs in a single amino acid in the F pocket of the peptide binding groove. To understand how this unique amino acid difference leads to a different behavior of the proteins in the cell, we have investigated the conformational stability of both proteins using a combination of in silico and experimental approaches. Here, we show that the binding site of B*27:05 is conformationally disordered in the absence of peptide due to a charge repulsion at the bottom of the F pocket. In agreement with this, B*27:05 requires the chaperone protein tapasin to a greater extent than the conformationally stable B*27:09 in order to remain structured and to bind peptide. Taken together, our data demonstrate a method to predict tapasin dependence and physiological behavior from the sequence and crystal structure of a particular class I allotype. This article is protected by copyright. All rights reserved.

Published
2015

32. F pocket flexibility influences the tapasin dependence of two differentially disease-associated MHC Class I proteins

Author

Infection & Immunity, Risk Assessment, dI&I RA-I&I I&I, LS Immunologie, Abualrous, Esam T, Fritzsche, Susanne, Hein, Zeynep, Al-Balushi, Mohammed S, Reinink, Peter|info:eu-repo/dai/nl/413319520, Boyle, Louise H, Wellbrock, Ursula, Antoniou, Antony N, Springer, Sebastian, Infection & Immunity, Risk Assessment, dI&I RA-I&I I&I, LS Immunologie, Abualrous, Esam T, Fritzsche, Susanne, Hein, Zeynep, Al-Balushi, Mohammed S, Reinink, Peter|info:eu-repo/dai/nl/413319520, Boyle, Louise H, Wellbrock, Ursula, Antoniou, Antony N, and Springer, Sebastian

Published
2015

36. Tapasin dependence of major histocompatibility complex class I molecules correlates with their conformational flexibility

Author

Garstka, Malgorzata Anna, primary, Fritzsche, Susanne, additional, Lenart, Izabela, additional, Hein, Zeynep, additional, Jankevicius, Gytis, additional, Boyle, Louise H., additional, Elliott, Tim, additional, Trowsdale, John, additional, Antoniou, Antony N., additional, Zacharias, Martin, additional, and Springer, Sebastian, additional

Published
2011
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39. Correction: Cellular Expression, Trafficking, and Function of Two Isoforms of Human ULBP5/RAET1G

Author

Eagle, Robert A., primary, Flack, Gillian, additional, Warford, Anthony, additional, Martínez-Borra, Jesús, additional, Jafferji, Insiya, additional, Traherne, James A., additional, Ohashi, Maki, additional, Boyle, Louise H., additional, Barrow, Alexander D., additional, Caillat-Zucman, Sophie, additional, Young, Neil T., additional, and Trowsdale, John, additional

Published
2009
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40. Cellular Expression, Trafficking, and Function of Two Isoforms of Human ULBP5/RAET1G

Author

Eagle, Robert A., primary, Flack, Gillian, additional, Warford, Anthony, additional, Martínez-Borra, Jesús, additional, Jafferji, Insiya, additional, Traherne, James A., additional, Ohashi, Maki, additional, Boyle, Louise H., additional, Barrow, Alexander D., additional, Caillat-Zucman, Sophie, additional, Young, Neil T., additional, and Trowsdale, John, additional

Published
2009
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43. Conventional protein kinase C and atypical protein kinase Cζ differentially regulate macrophage production of tumour necrosis factor-α and interleukin-10.

Author

Boyle, Louise H., Goodall, Jane C., and Hill Gaston, J. S.

Subjects
*CYTOKINES, *MACROPHAGES, *PROTEIN kinase C, *RHEUMATOID arthritis, *ANTI-inflammatory agents, *TUMOR necrosis factors
Abstract

In chronic inflammatory diseases such as rheumatoid arthritis, joint macrophages/monocytes are the major source of pro- and anti-inflammatory cytokines. Little is understood regarding the signalling pathways which determine the production of the pro-inflammatory cytokine, tumour necrosis factor-α (TNF-α) and the anti-inflammatory cytokine, interleukin-10 (IL-10). Two pathways integral to macrophage function are the protein kinase C (PKC)- and the cAMP- dependent pathways. In this report, we have investigated the involvement of PKC and cAMP in the production of TNF-α and IL-10 by peripheral blood monocyte-derived macrophages. The utilization of the PKC inhibitors Go6983, Go6976 and RO-32–0432 demonstrated a role for conventional PKCs (α and β) in the production of TNF-α in response to stimulation by lipopolysaccharide and phorbol 12-myristate 13-acetate (PMA)/ionomycin. PKC stimulation resulted in the downstream activation of the p42/44 mitogen-activated protein kinase (MAPK) pathway which differentially regulates TNF-α and IL-10. The addition of cAMP however, suppressed activation of this MAPK and TNF-a production. Cyclic-AMP augmented IL-10 production and cAMP response element binding protein activation upon stimulation by PMA/ ionomycin. In addition, cAMP activated PKCζ; inhibition of which, by a dominant negative adenovirus construct, selectively suppressed IL-10 production. These observations suggest that pro-inflammatory and anti-inflammatory cytokines are differentially regulated by PKC isoforms; TNF-α being dependent on conventional PKCs (α and β) whereas IL-10 is regulated by the cAMP-regulated atypical PKCf. [ABSTRACT FROM AUTHOR]

Published
2004

44. The Recognition of Abnormal Forms of HLA-B27 by CD4+ T Cells

Author

Boyle, Louise H., Goodall, Jane C., and Gaston, J. S. Hill

Abstract

The MHC class I molecule, HLA-B27 can be expressed as a number of non-conventional forms, in addition to conventional HLA-B27 heterodimers presenting peptide. This has lead to new avenues of research to explain the association of this molecule with SpA. Surprisingly, HLA-B27 transgenic animal models implicated CD4+ T cells, which conventionally interact with MHC class II molecules, not MHC class I molecules, in the pathogenesis of SpA. One hypothesis to explain these finding is that non-conventional forms of HLA-B27, specifically HLA-B27 homodimers, might mimic MHC class II molecules and be recognised by CD4+ T cells. We investigated whether CD4+ T cells from AS patients can interact with HLA-B27, discovering that indeed CD4+ T cells can interact with various forms of HLA-B27. Here we discuss how such interactions between HLA-B27 and CD4+ T cells could occur in vivo and potential contributions of such interactions to the pathogenesis of SpA.

Published
2004

45. Rethinking assessment for interprofessional learning during the COVID-19 era: steering a middle course

Author

McLarnon, Nichola, Hutchings, Maggie, O'Carroll, Veronica, Wetzlmair, Lisa-Christin, Blumenthal, Sharron, Boyle, Louise H., El-Awaisi, Alla, Greaves, Jane, Park, Vikki, and Power, Alison

Subjects
B900, X900, B700
Abstract

This, the sixth article in a series exploring interprofessional education during the COVID-19 pandemic, will focus upon the considerations and adaptations aligned to the assessment of interprofessional education, including examples of the alternative assessment strategies employed by faculty, the modality of assessment and the tools utilised, the student and faculty experience of remote/online assessment and the challenges faced by both during the rapid pivot to remote learning and assessment.

46. TAPBPR mediates peptide dissociation from MHC class I using a leucine lever

Author

Ilca, F Tudor, Neerincx, Andreas, Hermann, Clemens, Marcu, Ana, Stevanović, Stefan, Deane, Janet E, and Boyle, Louise H

Subjects
Antigen Presentation, Binding Sites, HLA-A Antigens, Histocompatibility Antigens Class I, Immunoglobulins, Membrane Proteins, major histocompatibility complex, 3. Good health, immunology, Molecular Docking Simulation, Protein Domains, inflammation, Leucine, Mutation, TAPBPR/TAPBPL, antigen processing, Humans, human, Amino Acid Sequence, Peptides, HeLa Cells, Protein Binding
Abstract

Tapasin and TAPBPR are known to perform peptide editing on major histocompatibility complex class I (MHC I) molecules; however, the precise molecular mechanism(s) involved in this process remain largely enigmatic. Here, using immunopeptidomics in combination with novel cell-based assays that assess TAPBPR-mediated peptide exchange, we reveal a critical role for the K22-D35 loop of TAPBPR in mediating peptide exchange on MHC I. We identify a specific leucine within this loop that enables TAPBPR to facilitate peptide dissociation from MHC I. Moreover, we delineate the molecular features of the MHC I F pocket required for TAPBPR to promote peptide dissociation in a loop-dependent manner. These data reveal that chaperone-mediated peptide editing on MHC I can occur by different mechanisms dependent on the C-terminal residue that the MHC I accommodates in its F pocket and provide novel insights that may inform the therapeutic potential of TAPBPR manipulation to increase tumour immunogenicity.

47. TAPBPR alters MHC class I peptide presentation by functioning as a peptide exchange catalyst

Author

Hermann, Clemens, Van Hateren, Andy, Trautwein, Nico, Neerincx, Andreas, Duriez, Patrick J, Stevanović, Stefan, Trowsdale, John, Deane, Janet E, Elliott, Tim, and Boyle, Louise H

Subjects
peptide repertoire, Antigen Presentation, Histocompatibility Antigens Class I, Immunoglobulins, Membrane Proteins, chemical and pharmacologic phenomena, 3. Good health, Cell Line, immunology, cell biology, Humans, antigen processing and presentation, human, MHC, Antigens, Peptides, Protein Binding
Abstract

Our understanding of the antigen presentation pathway has recently been enhanced with the identification that the tapasin-related protein TAPBPR is a second major histocompatibility complex (MHC) class I-specific chaperone. We sought to determine whether, like tapasin, TAPBPR can also influence MHC class I peptide selection by functioning as a peptide exchange catalyst. We show that TAPBPR can catalyse the dissociation of peptides from peptide-MHC I complexes, enhance the loading of peptide-receptive MHC I molecules, and discriminate between peptides based on affinity in vitro. In cells, the depletion of TAPBPR increased the diversity of peptides presented on MHC I molecules, suggesting that TAPBPR is involved in restricting peptide presentation. Our results suggest TAPBPR binds to MHC I in a peptide-receptive state and, like tapasin, works to enhance peptide optimisation. It is now clear there are two MHC class I specific peptide editors, tapasin and TAPBPR, intimately involved in controlling peptide presentation to the immune system.

48. Distinct Polymorphisms in HLA Class I Molecules Govern Their Susceptibility to Peptide Editing by TAPBPR

Author

Ilca, F Tudor, Drexhage, Linnea Z, Brewin, Gemma, Peacock, Sarah, and Boyle, Louise H

Subjects
Antigen Presentation, Polymorphism, Genetic, HLA-A Antigens, Histocompatibility Antigens Class I, HLA-A24 Antigen, Immunoglobulins, Membrane Proteins, Membrane Transport Proteins, HLA-C Antigens, 3. Good health, polymorphism, HLA, HEK293 Cells, Protein Domains, HLA-B Antigens, HLA-A2 Antigen, TAPBPR/TAPBPL, Humans, antigen processing and presentation, MHC, Immunoglobulin Allotypes, Peptides, HeLa Cells, Molecular Chaperones, Protein Binding
Abstract

Understanding how peptide selection is controlled on different major histocompatibility complex class I (MHC I) molecules is pivotal for determining how variations in these proteins influence our predisposition to infectious diseases, cancer, and autoinflammatory conditions. Although the intracellular chaperone TAPBPR edits MHC I peptides, it is unclear which allotypes are subjected to TAPBPR-mediated peptide editing. Here, we examine the ability of 97 different human leukocyte antigen (HLA) class I allotypes to interact with TAPBPR. We reveal a striking preference of TAPBPR for HLA-A, particularly for supertypes A2 and A24, over HLA-B and -C molecules. We demonstrate that the increased propensity of these HLA-A molecules to undergo TAPBPR-mediated peptide editing is determined by molecular features of the HLA-A F pocket, specifically residues H114 and Y116. This work reveals that specific polymorphisms in MHC I strongly influence their susceptibility to chaperone-mediated peptide editing, which may play a significant role in disease predisposition.

49. Polymorphisms in MHC class I molecules influence their interactions with components of the antigen processing and presentation pathway

Author

Louise H. Boyle, Aure Aflalo, Aflalo, Aure [0000-0002-7158-6868], Boyle, Louise H [0000-0002-3105-6555], and Apollo - University of Cambridge Repository

Subjects
0301 basic medicine, Peptide, chemical and pharmacologic phenomena, Computational biology, Major histocompatibility complex, polymorphism, immunology, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, antigens, MHC class I, expression, Genetics, Humans, Molecular Biology, Genetics (clinical), chemistry.chemical_classification, function, Antigen Presentation, Polymorphism, Genetic, biology, Antigen processing, Histocompatibility Antigens Class I, Histocompatibility Antigens Class II, General Medicine, Folding (chemistry), 030104 developmental biology, chemistry, biology.protein, Peptides, Function (biology), 030215 immunology
Abstract

MHC class I (MHC-I) molecules undergo an intricate folding process in order to pick up antigenic peptide to present to the immune system. In recent years, the discovery of a new peptide editor for MHC-I has added an extra level of complexity in our understanding of how peptide presentation is regulated. On top of this, the incredible diversity in MHC-I molecules leads to significant variation in the interaction between MHC-I and components of the antigen processing and presentation pathway. Here, we review our current understanding regarding how polymorphisms in human leukocyte antigen class I molecules influence their interactions with key components of the antigen processing and presentation pathway. A deeper understanding of this may offer new insights regarding how apparently subtle variation in MHC-I can have a significant impact on susceptibility to disease.

Published
2021

50. TAPBPR mediates peptide dissociation from MHC class I using a leucine lever

Author

Clemens Hermann, Stefan Stevanovic, Janet E. Deane, Andreas Neerincx, Ana Marcu, Louise H. Boyle, F. Tudor Ilca, Ilca, F Tudor [0000-0002-6582-8007], Neerincx, Andreas [0000-0002-6902-5383], Hermann, Clemens [0000-0002-0009-9501], Marcu, Ana [0000-0003-0808-8097], Stevanović, Stefan [0000-0003-1954-7762], Deane, Janet E [0000-0002-4863-0330], Boyle, Louise H [0000-0002-3105-6555], and Apollo - University of Cambridge Repository

Subjects
Cell, Peptide, immunology, Immunology and Inflammation, 0302 clinical medicine, Tapasin, Biology (General), chemistry.chemical_classification, 0303 health sciences, biology, Chemistry, Immunogenicity, major histocompatibility complex, 3. Good health, Cell biology, Molecular Docking Simulation, medicine.anatomical_structure, Molecular mechanism, TAPBPR/TAPBPL, Medicine, Leucine, Research Article, Human, Protein Binding, QH301-705.5, Science, Immunoglobulins, Major histocompatibility complex, 03 medical and health sciences, Protein Domains, MHC class I, medicine, antigen processing, Humans, Amino Acid Sequence, 030304 developmental biology, Binding Sites, HLA-A Antigens, Histocompatibility Antigens Class I, Membrane Proteins, antigen presentation, inflammation, Mutation, biology.protein, Peptides, HeLa Cells, 030215 immunology
Abstract

Tapasin and TAPBPR are known to perform peptide editing on major histocompatibility complex class I (MHC I) molecules, however, the precise molecular mechanism(s) involved in this process remain largely enigmatic. Here, using immunopeptidomics in combination with novel cell-based assays that assess TAPBPR-mediate peptide exchange, we reveal a critical role for the K22-D35 loop of TAPBPR in mediating peptide exchange on MHC I. We identify a specific leucine within this loop that enables TAPBPR to facilitate peptide dissociation from MHC I. Moreover, we delineate the molecular features of the MHC I F pocket required for TAPBPR to promote peptide dissociation in a loop-dependent manner. These data reveal that chaperone-mediated peptide editing of MHC I can occur by different mechanisms dependent on the C-terminal residue that the MHC I accommodates in its F pocket and provide novel insights that may inform the therapeutic potential of TAPBPR manipulation to increase tumour immunogenicity.Impact StatementThis work demonstrates for the first time that the K22-D35 loop of TAPBPR is the essential region for mediating peptide exchange and peptide selection on major histocompatibility complex class I molecules.

Published
2018

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