Your search keyword '"Carl Goodyear"' showing total 12 results

1. Optimising psoriatic arthritis therapy with immunological methods to increase standard evaluation: the protocol of an open-label multicentre, parallel-group, two-arm randomised controlled study evaluation precision medicine approach in the treatment of psoriatic arthritis

Author

Iain B McInnes, Stefan Siebert, Paul Bowness, Laura C Coates, Anne Francis, Bruce W Kirkham, Alexander Ooms, Hussein Al-Mossawi, Louise Bennett, Nicole Yager, Duncan Richards, Mimi Bogale, Carl Goodyear, Sylvine Lalnunhlimi, Leonie S Taams, and Aysin Tulunay Virlan

Subjects

Medicine

Abstract

Introduction Psoriatic arthritis (PsA) affects around 150 000 people in the UK of whom around 50% require treatment with biologics. The most used biologics for PsA target tumour necrosis factor (TNF) or interleukin-17A (IL-17A). About 50% of patients respond to each, but it is not currently possible to predict response for individual patients, necessitating sequential treatment steps. A recent proof of concept study in PsA suggested that using peripheral immunophenotype to choose therapy could improve time to treatment response.This study will test the hypothesis, within an open-label parallel-group biomarker-stratified multicentre randomised controlled trial, which the baseline proportion of CD4+T cells with an activated type 17 immunophenotype (Th17 levels) predicts response to IL-17A or TNF inhibitors in PsA. Additional analyses will identify if the model can be refined by combining additional clinical and immunophenotypic factors. Statistical modelling will be used to predict the likely effectiveness of these approaches compared with standard care.Methods and analysis Patients with PsA eligible to start their first biologic as part of standard care are recruited and baseline blood tests are taken for immunophenotyping. Participants are stratified equally by Th17 levels and randomised 1:1 to receive either TNF (adalimumab) or IL-17A (secukinumab) inhibitors. The primary analysis will establish the interaction between baseline immunophenotype and treatment on the primary outcome (achievement of minimal disease activity criteria at week 24). In secondary analysis, modelling will identify if this prediction model can be optimised further by incorporating clinical phenotypes and additional immunophenotyping techniques.Ethics and dissemination Ethical approval for the study was granted by the North West Preston Research Ethics Committee (ref 21/NW/0016). Dissemination will be via conference presentations and peer-reviewed publications, aiming to impact on treatment guidelines.Trial registration number ISRCTN17228602.

Published

2023

2. P1350: M2-LIKE MONOCYTE-DERIVED MACROPHAGES PROTECT AML CELL LINES AND PRIMARY AML CELLS AGAINST THERAPY-INDUCED APOPTOSIS

Author

Katerina Miari, Athanasia Papadopoulou, Leandro Martinez, Victoria Campbell, Carl Goodyear, Helen Wheadon, Monica Guzman, and Mark Williams

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2023

3. No evidence for differential gene expression in major depressive disorder PBMCs, but robust evidence of elevated biological ageing

Author

John J. Cole, Alison McColl, Robin Shaw, Mary-Ellen Lynall, Philip J. Cowen, Peter de Boer, Wayne C. Drevets, Neil Harrison, Carmine Pariante, Linda Pointon, NIMA consortium, Carl Goodyear, Edward Bullmore, and Jonathan Cavanagh

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Abstract The increasingly compelling data supporting the involvement of immunobiological mechanisms in Major Depressive Disorder (MDD) might provide some explanation forthe variance in this heterogeneous condition. Peripheral blood measures of cytokines and chemokines constitute the bulk of evidence, with consistent meta-analytic data implicating raised proinflammatory cytokines such as IL6, IL1β and TNF. Among the potential mechanisms linking immunobiological changes to affective neurobiology is the accelerated biological ageing seen in MDD, particularly via the senescence associated secretory phenotype (SASP). However, the cellular source of immunobiological markers remains unclear. Pre-clinical evidence suggests a role for peripheral blood mononuclear cells (PBMC), thus here we aimed to explore the transcriptomic profile using RNA sequencing in PBMCs in a clinical sample of people with various levels of depression and treatment response comparing it with that in healthy controls (HCs). There were three groups with major depressive disorder (MDD): treatment-resistant (n = 94), treatment-responsive (n = 47) and untreated (n = 46). Healthy controls numbered 44. Using PBMCs gene expression analysis was conducted using RNAseq to a depth of 54.5 million reads. Differential gene expression analysis was performed using DESeq2. The data showed no robust signal differentiating MDD and HCs. There was, however, significant evidence of elevated biological ageing in MDD vs HC. Biological ageing was evident in these data as a transcriptional signature of 888 age-associated genes (adjusted p 0.6) that also correlated strongly with chronological age (spearman correlation coefficient of 0.72). Future work should expand clinical sample sizes and reduce clinical heterogeneity. Exploration of RNA-seq signatures in other leukocyte populations and single cell RNA sequencing may help uncover more subtle differences. However, currently the subtlety of any PBMC signature mitigates against its convincing use as a diagnostic or predictive biomarker.

Published

2021

4. Omics and Multi-Omics Analysis for the Early Identification and Improved Outcome of Patients with Psoriatic Arthritis

Author

Robert Gurke, Annika Bendes, John Bowes, Michaela Koehm, Richard M. Twyman, Anne Barton, Dirk Elewaut, Carl Goodyear, Lisa Hahnefeld, Rainer Hillenbrand, Ewan Hunter, Mark Ibberson, Vassilios Ioannidis, Sabine Kugler, Rik J. Lories, Eduard Resch, Stefan Rüping, Klaus Scholich, Jochen M. Schwenk, James C. Waddington, Phil Whitfield, Gerd Geisslinger, Oliver FitzGerald, Frank Behrens, and Stephen R. Pennington

Subjects

psoriatic diseases, psoriatic arthritis, psoriasis, multi-omics, data integration, Biology (General), QH301-705.5

Abstract

The definitive diagnosis and early treatment of many immune-mediated inflammatory diseases (IMIDs) is hindered by variable and overlapping clinical manifestations. Psoriatic arthritis (PsA), which develops in ~30% of people with psoriasis, is a key example. This mixed-pattern IMID is apparent in entheseal and synovial musculoskeletal structures, but a definitive diagnosis often can only be made by clinical experts or when an extensive progressive disease state is apparent. As with other IMIDs, the detection of multimodal molecular biomarkers offers some hope for the early diagnosis of PsA and the initiation of effective management and treatment strategies. However, specific biomarkers are not yet available for PsA. The assessment of new markers by genomic and epigenomic profiling, or the analysis of blood and synovial fluid/tissue samples using proteomics, metabolomics and lipidomics, provides hope that complex molecular biomarker profiles could be developed to diagnose PsA. Importantly, the integration of these markers with high-throughput histology, imaging and standardized clinical assessment data provides an important opportunity to develop molecular profiles that could improve the diagnosis of PsA, predict its occurrence in cohorts of individuals with psoriasis, differentiate PsA from other IMIDs, and improve therapeutic responses. In this review, we consider the technologies that are currently deployed in the EU IMI2 project HIPPOCRATES to define biomarker profiles specific for PsA and discuss the advantages of combining multi-omics data to improve the outcome of PsA patients.

Published

2022

5. In Human Autoimmunity, a Substantial Component of the B Cell Repertoire Consists of Polyclonal, Barely Mutated IgG+ve B Cells

Author

Graeme J. M. Cowan, Katherine Miles, Lorenzo Capitani, Sophie S. B. Giguere, Hanna Johnsson, Carl Goodyear, Iain B. McInnes, Steffen Breusch, David Gray, and Mohini Gray

Subjects

B cells, BCR, autoimmunity, TNF, rheumatoid arthritis, Immunologic diseases. Allergy, RC581-607

Abstract

B cells are critical for promoting autoimmunity and the success of B cell depletion therapy in rheumatoid arthritis (RA) confirms their importance in driving chronic inflammation. Whilst disease specific autoantibodies are useful diagnostically, our understanding of the pathogenic B cell repertoire remains unclear. Defining it would lead to novel insights and curative treatments. To address this, we have undertaken the largest study to date of over 150 RA patients, utilizing next generation sequencing (NGS) to analyze up to 200,000 BCR sequences per patient. The full-length antigen-binding variable region of the heavy chain (IgGHV) of the IgG B cell receptor (BCR) were sequenced. Surprisingly, RA patients do not express particular clonal expansions of B cells at diagnosis. Rather they express a polyclonal IgG repertoire with a significant increase in BCRs that have barely mutated away from the germline sequence. This pattern remains even after commencing disease modifying therapy. These hypomutated BCRs are expressed by TNF-alpha secreting IgG+veCD27−ve B cells, that are expanded in RA peripheral blood and enriched in the rheumatoid synovium. A similar B cell repertoire is expressed by patients with Sjögren's syndrome. A rate limiting step in the initiation of autoimmunity is the activation of B cells and this data reveals that a sizeable component of the human autoimmune B cell repertoire consists of polyclonal, hypomutated IgG+ve B cells, that may play a critical role in driving chronic inflammation.

Published

2020

6. Inflammation causes remodeling of mitochondrial cytochrome

Author

Sally A, Clayton, Kalbinder K, Daley, Lucy, MacDonald, Erika, Fernandez-Vizarra, Giovanni, Bottegoni, John D, O'Neil, Triin, Major, Daniel, Griffin, Qinqin, Zhuang, Adeolu B, Adewoye, Kieran, Woolcock, Simon W, Jones, Carl, Goodyear, Aziza, Elmesmari, Andrew, Filer, Daniel A, Tennant, Stefano, Alivernini, Christopher D, Buckley, Robert D S, Pitceathly, Mariola, Kurowska-Stolarska, and Andrew R, Clark

Subjects

Immunology, SciAdv r-articles, Diseases and Disorders, Biomedicine and Life Sciences, Research Article

Abstract

Description, Exchange of mitochondrial subunits C15ORF48 and NDUFA4 occurs during macrophage activation in vitro and in inflammatory disease., Dysregulated mitochondrial function is a hallmark of immune-mediated inflammatory diseases. Cytochrome c oxidase (CcO), which mediates the rate-limiting step in mitochondrial respiration, is remodeled during development and in response to changes of oxygen availability, but there has been little study of CcO remodeling during inflammation. Here, we describe an elegant molecular switch mediated by the bifunctional transcript C15orf48, which orchestrates the substitution of the CcO subunit NDUFA4 by its paralog C15ORF48 in primary macrophages. Expression of C15orf48 is a conserved response to inflammatory signals and occurs in many immune-related pathologies. In rheumatoid arthritis, C15orf48 mRNA is elevated in peripheral monocytes and proinflammatory synovial tissue macrophages, and its expression positively correlates with disease severity and declines in remission. C15orf48 is also expressed by pathogenic macrophages in severe coronavirus disease 2019 (COVID-19). Study of a rare metabolic disease syndrome provides evidence that loss of the NDUFA4 subunit supports proinflammatory macrophage functions.

Published

2021

7. T cell and humoral immune response to multiple SARS-CoV-2 variants including omicron (B1.1.529) after two doses of COVID-19 vaccine in patients with cirrhosis and liver diseases requiring immunosuppression: data from the EASL COVID-Hep network

Author

Sam Murray, Stephanie Longet, Tom Tipton, Maria Carlota Londoño, Elisa Pose, Stephen Laidlaw, Dung Nguyen, Georgina Meacham, Zixiang Lim, Stavros Dimitriadis, Sophie Irwin, Jonathan Cook, Massimo Iavarone, Pietro Lampertico, Virginia Hernandez-Gea, Juan Carlos Garcia Pagan, Julian Schulze zur Wiesch, Martina Sterneck, Francesco Paolo Russo, Jack Satsangi, Susanna Dunachie, Paul Klenerman, Carl Goodyear, Iain B. McInnes, Pere Ginès, Miles Carroll, Thomas Marjot, and Eleanor Barnes

Subjects

Hepatology

Published

2022

8. Intestinal-derived ILCs migrating in lymph increase IFNγ production in response to Salmonella Typhimurium infection

Author

Verena, Kästele, Johannes, Mayer, Edward S, Lee, Natalie, Papazian, John J, Cole, Vuk, Cerovic, Gabrielle, Belz, Michio, Tomura, Gerard, Eberl, Carl, Goodyear, Rose A, Maciewicz, Daniel, Wall, Tom, Cupedo, David R, Withers, and Simon, Milling

Subjects

Mice, Knockout, Salmonella typhimurium, Gene Expression Profiling, Nuclear Receptor Subfamily 1, Group F, Member 3, Immunity, Innate, Mice, Inbred C57BL, Disease Models, Animal, Interferon-gamma, Mice, Cell Movement, Salmonella Infections, Animals, Humans, Lymph, Lymph Nodes, Lymphocytes, Intestinal Mucosa

Abstract

Innate lymphoid cells (ILCs) are enriched in mucosae and have been described as tissue-resident. Interestingly, ILCs are also present within lymph nodes (LNs), in the interfollicular regions, the destination for lymph-migratory cells. We have previously shown that LN ILCs are supplemented by peripheral tissue-derived ILCs. Using thoracic duct cannulations, we here enumerate the intestinal lymph ILCs that traffic from the intestine to the mesenteric LNs (MLNs). We provide, for the first time, a detailed characterisation of these lymph-migratory ILCs. We show that all ILC subsets migrate in lymph, and while global transcriptional analysis reveals a shared signature with tissue-resident ILCs, lymph ILCs express migration-associated genes including S1PRs, SELL (CD62L) and CCR7. Interestingly, we discovered that while Salmonella Typhimurium infections do not increase the numbers of migrating ILCs, infection changes their composition and cytokine profile. Infection increases the proportions of RORyt

Published

2020

9. Innovative Education and Engagement Tools for Rheumatology and Immunology Public Engagement with Augmented Reality

Author

Timea, Kosa, Louise, Bennett, Daniel, Livingstone, Carl, Goodyear, and Brian, Loranger

Subjects

Arthritis, Rheumatoid, Augmented Reality, Patient Education as Topic, Rheumatology, Allergy and Immunology, Humans, Learning

Abstract

Rheumatoid arthritis (RA) affects around 1% of the population, which places a heavy burden on society and has severe consequences for the individuals affected. The early diagnosis and implementation of disease-modifying anti-rheumatic drugs significantly increase the chance of achieving long-term sustained remission. Therefore, raising awareness of RA amongst the general public is important in order to decrease the time of diagnosis of the disease. Augmented reality (AR) can be tremendously valuable in a teaching and learning context, as the coexistence of real and virtual objects aids learners in understanding abstract ideas and complicated spatial relationships. It has also been suggested that it raises motivation in users through interactivity and novelty. In this chapter we explore the use AR in public engagement, and detail the design, development and evaluation of a blended learning experience utilising AR. A set of informative printed posters was produced, enhanced by an accompanying interactive AR application. The main user testing was conducted with 27 participants at a science outreach event at the Glasgow Science Centre. Findings report mean positive attitudes regarding all aspects of the study, highlighting the potential of AR for public engagement with topics such as RA.

Published

2020

10. OP0305 THE ALARMIN S100A9 HAMPERS OSTEOCLAST DIFFERENTIATION FROM CIRCULATING PRECURSORS BY REDUCING THE EXPRESSION OF RANK

Author

Martijn van den Bosch, Irene DI Ceglie, Arjen Blom, Robab Davar, Colin Logie, Ehsan Habibi, Johannes Roth, Thomas Vogl, Carl Goodyear, Peter van der Kraan, and Peter van Lent

Published

2019

11. O46. Proteinase-Activated Receptor-2 Critically Influences Osteophyte Formation in Experimental Osteoarthritis

Author

William R. Ferrell, Robin Plevin, Carl Goodyear, Andrew Rowan, John C. Lockhart, Carmen Huesa, Iain B. McInnes, Rob van 't Hof, and Laura McGavin

Subjects

Rheumatology, business.industry, Proteolytic enzymes, Medicine, Pharmacology (medical), Osteoarthritis, Experimental osteoarthritis, Pharmacology, Receptor, business, medicine.disease

Published

2014

12. A B-cell superantigen that targets B-1 lymphocytes

Author

Gj, Silverman, Cary S, Graille M, Ve, Curtiss, Wagenknecht R, Luo L, Dwyer D, Carl Goodyear, Al, Corper, Ea, Stura, and Jb, Charbonnier

Subjects

Staphylococcus aureus, T-Lymphocytes, B-Lymphocyte Subsets, Immunoglobulin Variable Region, Clonal Deletion, Receptors, Antigen, B-Cell, Mice, Transgenic, Crystallography, X-Ray, Antigen-Antibody Reactions, Evolution, Molecular, Immunoglobulin Fab Fragments, Mice, Structure-Activity Relationship, Xenopus laevis, Animals, Humans, Staphylococcal Protein A, Antigens, Bacterial, Binding Sites, Superantigens, Antibodies, Bacterial, Immunoglobulin Fc Fragments, Protein Structure, Tertiary, Animals, Newborn, Immunoglobulin G, Immunoglobulin Heavy Chains

Published

2000