Your search keyword '"Barbara Fazekas"' showing total 325 results

1. MHCII restriction demonstrates B cells have very limited capacity to activate tumour-specific CD4+ T cells in vivo

Author

Thomas V. Guy, Alexandra M. Terry, Helen M. McGuire, Elena Shklovskaya, and Barbara Fazekas de St Groth

Subjects

Antigen presentation, B cell, MHC restriction, T cell, tumour, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

There has been growing interest in the role of B cells in antitumour immunity and potential use in adoptive cellular therapies. To date, the success of such therapies is limited. The intrinsic capacity of B cells to specifically activate tumour-specific CD4+ T cells in vivo via TCR-dependent interactions remains poorly defined. We have developed an in vivo tumour model that utilizes MHCII I-E restriction which limits antigen presentation to tumour-specific CD4 T cells to either tumour-specific B cells or host myeloid antigen presenting cells (APCs) in lymphopenic RAG-/-mice. We have previously shown that these naive tumour-specific CD4+ T cells can successfully eradicate established tumours in this model when activated by host APCs. When naïve tumour-specific B cells are the only source of I-E+ APC, very limited proliferation of naïve CD4+ T cells is observed, whereas host I-E+ APCs are potent T cell activators. B cells pre-activated with an anti-CD40 agonistic antibody in vivo support increased T cell proliferation, although far less than host APCs. CD4+ T cells that have already differentiated to an effector/central memory phenotype proliferate more readily in response to naïve B cells, although still 100-fold less than in response to host APCs. This study demonstrates that even in a significantly lymphopenic environment, myeloid APCs are the dominant primary activators of tumour-specific T cells, in contrast to the very limited capacity of tumour-specific B cells. This suggests that future anti-tumour therapies that incorporate activated B cells should also include mechanisms that activate host APCs.

Published

2024

2. Immunoprofiling reveals cell subsets associated with the trajectory of cytomegalovirus reactivation post stem cell transplantation

Author

Lauren Stern, Helen M. McGuire, Selmir Avdic, Barbara Fazekas de St Groth, David Gottlieb, Allison Abendroth, Emily Blyth, and Barry Slobedman

Subjects

Science

Abstract

Human cytomegalovirus is a major cause of morbidity and mortality in transplant patients and multiple immune cells types are critical during infection and reactivation. Here the authors assess the immune cell compartments of haematopoietic stem cell recipients in the early period post transplantation and identify key features of effector memory CD4+ T cells and mucosal associated invariant T cells in this context.

Published

2022

3. Metabolite-based dietary supplementation in human type 1 diabetes is associated with microbiota and immune modulation

Author

Kirstine J. Bell, Sonia Saad, Bree J. Tillett, Helen M. McGuire, Sara Bordbar, Yu Anne Yap, Long T. Nguyen, Marc R. Wilkins, Susan Corley, Shannon Brodie, Sussan Duong, Courtney J. Wright, Stephen Twigg, Barbara Fazekas de St Groth, Leonard C. Harrison, Charles R. Mackay, Esteban N. Gurzov, Emma E. Hamilton-Williams, and Eliana Mariño

Subjects

Type 1 diabetes, SCFAs, Microbiota, Immune regulation, Dietary-metabolites, Autoimmunity, Microbial ecology, QR100-130

Abstract

Abstract Background Short-chain fatty acids (SCFAs) produced by the gut microbiota have beneficial anti-inflammatory and gut homeostasis effects and prevent type 1 diabetes (T1D) in mice. Reduced SCFA production indicates a loss of beneficial bacteria, commonly associated with chronic autoimmune and inflammatory diseases, including T1D and type 2 diabetes. Here, we addressed whether a metabolite-based dietary supplement has an impact on humans with T1D. We conducted a single-arm pilot-and-feasibility trial with high-amylose maize-resistant starch modified with acetate and butyrate (HAMSAB) to assess safety, while monitoring changes in the gut microbiota in alignment with modulation of the immune system status. Results HAMSAB supplement was administered for 6 weeks with follow-up at 12 weeks in adults with long-standing T1D. Increased concentrations of SCFA acetate, propionate, and butyrate in stools and plasma were in concert with a shift in the composition and function of the gut microbiota. While glucose control and insulin requirements did not change, subjects with the highest SCFA concentrations exhibited the best glycemic control. Bifidobacterium longum, Bifidobacterium adolescentis, and vitamin B7 production correlated with lower HbA1c and basal insulin requirements. Circulating B and T cells developed a more regulatory phenotype post-intervention. Conclusion Changes in gut microbiota composition, function, and immune profile following 6 weeks of HAMSAB supplementation were associated with increased SCFAs in stools and plasma. The persistence of these effects suggests that targeting dietary SCFAs may be a mechanism to alter immune profiles, promote immune tolerance, and improve glycemic control for the treatment of T1D. Trial registration ACTRN12618001391268. Registered 20 August 2018, https://www.anzctr.org.au/Trial/Registration/TrialReview.aspx?id=375792 Video Abstract

Published

2022

4. Mass cytometry analysis reveals altered immune profiles in patients with coronary artery disease

Author

Katharine A Kott, Adam S Chan, Stephen T Vernon, Thomas Hansen, Taiyun Kim, Macha deDreu, Bavani Gunasegaran, Andrew J Murphy, Ellis Patrick, Peter J Psaltis, Stuart M Grieve, Jean Y Yang, Barbara Fazekas de St Groth, Helen M McGuire, and Gemma A Figtree

Subjects

atherosclerosis, immune signature, inflammation, mass cytometry, T regulatory cells, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Objective The importance of inflammation in atherosclerosis is well accepted, but the role of the adaptive immune system is not yet fully understood. To further explore this, we assessed the circulating immune cell profile of patients with coronary artery disease (CAD) to identify discriminatory features by mass cytometry. Methods Mass cytometry was performed on patient samples from the BioHEART‐CT study, gated to detect 82 distinct cell subsets. CT coronary angiograms were analysed to categorise patients as having CAD (CAD+) or having normal coronary arteries (CAD−). Results The discovery cohort included 117 patients (mean age 61 ± 12 years, 49% female); 79 patients (68%) were CAD+. Mass cytometry identified changes in 15 T‐cell subsets, with higher numbers of proliferating, highly differentiated and cytotoxic cells and decreases in naïve T cells. Five T‐regulatory subsets were related to an age and gender‐independent increase in the odds of CAD incidence when expressing CCR2 (OR 1.12), CCR4 (OR 1.08), CD38 and CD45RO (OR 1.13), HLA‐DR (OR 1.06) and Ki67 (OR 1.22). Markers of proliferation and differentiation were also increased within B cells, while plasmacytoid dendritic cells were decreased. This combination of changes was assessed using SVM models in discovery and validation cohorts (area under the curve = 0.74 for both), confirming the robust nature of the immune signature detected. Conclusion We identified differences within immune subpopulations of CAD+ patients which are indicative of a systemic immune response to coronary atherosclerosis. This immune signature needs further study via incorporation into risk scoring tools for the precision diagnosis of CAD.

Published

2023

5. Investigation of type I interferon responses in ANCA-associated vasculitis

Author

Isabella Batten, Mark W. Robinson, Arthur White, Cathal Walsh, Barbara Fazekas, Jason Wyse, Antonia Buettner, Suzanne D’Arcy, Emily Greenan, Conor C. Murphy, Zoe Wigston, Joan Ní Gabhann-Dromgoole, Edward M. Vital, Mark A. Little, and Nollaig M. Bourke

Subjects

Medicine, Science

Abstract

Abstract Type I interferon (IFN) dysregulation is a major contributory factor in the development of several autoimmune diseases, termed type I interferonopathies, and is thought to be the pathogenic link with chronic inflammation in these conditions. Anti-neutrophil cytoplasmic antibody (ANCA)-Associated Vasculitis (AAV) is an autoimmune disease characterised by necrotising inflammation of small blood vessels. The underlying biology of AAV is not well understood, however several studies have noted abnormalities in type I IFN responses. We hypothesised that type I IFN responses are systemically dysregulated in AAV, consistent with features of a type I interferonopathy. To investigate this, we measured the expression of seven interferon regulated genes (IRGs) (ISG15, SIGLEC1, STAT1, RSAD2, IFI27, IFI44L and IFIT1) in peripheral blood samples, as well as three type I IFN regulated proteins (CXCL10, MCP-1 and CCL19) in serum samples from AAV patients, healthy controls and disease controls. We found no difference in type I IFN regulated gene or protein expression between AAV patients and healthy controls. Furthermore, IRG and IFN regulated protein expression did not correlate with clinical measurements of disease activity in AAV patients. Thus, we conclude that systemic type I IFN responses are not key drivers of AAV pathogenesis and AAV should not be considered a type I interferonopathy.

Published

2021

6. Brick plots: an intuitive platform for visualizing multiparametric immunophenotyped cell clusters

Author

Samuel E. Norton, Julia K. H. Leman, Tiffany Khong, Andrew Spencer, Barbara Fazekas de St Groth, Helen M. McGuire, and Roslyn A. Kemp

Subjects

Mass cytometry, Analysis, T cells, NK cells, Cancer, Clinical, Computer applications to medicine. Medical informatics, R858-859.7, Biology (General), QH301-705.5

Abstract

Abstract Background The advent of mass cytometry has dramatically increased the parameter limit for immunological analysis. New approaches to analysing high parameter cytometry data have been developed to ease analysis of these complex datasets. Many of these methods assign cells into population clusters based on protein expression similarity. Results Here we introduce an additional method, termed Brick plots, to visualize these cluster phenotypes in a simplified and intuitive manner. The Brick plot method generates a two-dimensional barcode that displays the phenotype of each cluster in relation to the entire dataset. We show that Brick plots can be used to visualize complex mass cytometry data, both from fundamental research and clinical trials, as well as flow cytometry data. Conclusion Brick plots represent a new approach to visualize complex immunological data in an intuitive manner.

Published

2020

7. Expansion and activation of distinct central memory T lymphocyte subsets in complex regional pain syndrome

Author

Marc A. Russo, Nathan T. Fiore, Caryn van Vreden, Dominic Bailey, Danielle M. Santarelli, Helen M. McGuire, Barbara Fazekas de St Groth, and Paul J. Austin

Subjects

Complex regional pain syndrome, Central memory T lymphocytes, Myeloid dendritic cells, Mass cytometry, NFkB, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Complex regional pain syndrome (CRPS) is a debilitating condition where trauma to a limb results in devastating persistent pain that is disproportionate to the initial injury. The pathophysiology of CRPS remains unknown; however, accumulating evidence suggests it is an immunoneurological disorder, especially in light of evidence of auto-antibodies in ~ 30% of patients. Despite this, a systematic assessment of all circulating leukocyte populations in CRPS has never been performed. Methods We characterised 14 participants as meeting the Budapest clinical criteria for CRPS and assessed their pain ratings and psychological state using a series of questionnaires. Next, we performed immunophenotyping on blood samples from the 14 CRPS participants as well as 14 healthy pain-free controls using mass cytometry. Using a panel of 38 phenotypic and activation markers, we characterised the numbers and intracellular activation status of all major leukocyte populations using manual gating strategies and unsupervised cluster analysis. Results We have shown expansion and activation of several distinct populations of central memory T lymphocytes in CRPS. The number of central memory CD8+ T cells was increased 2.15-fold; furthermore, this cell group had increased phosphorylation of NFkB and STAT1 compared to controls. Regarding central memory CD4+ T lymphocytes, the number of Th1 and Treg cells was increased 4.98-fold and 2.18-fold respectively, with increased phosphorylation of NFkB in both populations. We also found decreased numbers of CD1c+ myeloid dendritic cells, although with increased p38 phosphorylation. These changes could indicate dendritic cell tissue trafficking, as well as their involvement in lymphocyte activation. Conclusions These findings represent the first mass cytometry immunophenotyping study in any chronic pain state and provide preliminary evidence of an antigen-mediated T lymphocyte response in CRPS. In particular, the presence of increased numbers of long-lived central memory CD4+ and CD8+ T lymphocytes with increased activation of pro-inflammatory signalling pathways may indicate ongoing inflammation and cellular damage in CRPS.

Published

2019

8. T lymphocyte and monocyte subsets are dysregulated in type 1 diabetes patients with peripheral neuropathic pain

Author

Jayden A. O'Brien, Helen M. McGuire, Diana Shinko, Barbara Fazekas de St Groth, Marc A. Russo, Dominic Bailey, Danielle M. Santarelli, Katie Wynne, and Paul J. Austin

Subjects

CD27, Chronic pain, Diabetic neuropathy, FlowSOM, Immunophenotyping, MAPKAPK2, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Diabetic neuropathic pain is a common and devastating complication of type 1 diabetes, but the mechanism by which it develops and persists is yet to be fully elucidated. This study utilised high-dimensional suspension mass cytometry in a pilot cohort to investigate differences in peripheral blood immunophenotypes between type 1 diabetes patients with (n ​= ​9) and without (n ​= ​9) peripheral neuropathic pain. The abundance and activation of several leukocyte subsets were investigated with unsupervised clustering approaches FlowSOM and SPADE, as well as by manual gating. Major findings included a proportional increase in CD4+ central memory T cells and an absolute increase in classical monocytes, non-classical monocytes, and mature natural killer cells in type 1 diabetes patients with pain compared to those without pain. The expression of CD27, CD127, and CD39 was upregulated on select T cell populations, and the phosphorylated form of pro-inflammatory transcription factor MK2 was upregulated across most populations. These results provide evidence that distinct immunological signatures are associated with painful neuropathy in type 1 diabetes patients. Further research may link these changes to mechanisms by which pain in type 1 diabetes is initiated and maintained, paving the way for much needed targeted treatments.

Published

2021

9. Autonomous Non Antioxidant Roles for Fasciola hepatica Secreted Thioredoxin-1 and Peroxiredoxin-1

Author

Amber Dorey, Krystyna Cwiklinski, James Rooney, Carolina De Marco Verissimo, Jesús López Corrales, Heather Jewhurst, Barbara Fazekas, Nichola Eliza Davies Calvani, Siobhán Hamon, Siobhán Gaughan, John P. Dalton, and Richard Lalor

Subjects

Fasciola, helminth, antioxidants, thioredoxin, thioredoxin peroxidase, peroxiredoxin, Microbiology, QR1-502

Abstract

Trematode parasites of the genus Fasciola are the cause of liver fluke disease (fasciolosis) in humans and their livestock. Infection of the host involves invasion through the intestinal wall followed by migration in the liver that results in extensive damage, before the parasite settles as a mature egg-laying adult in the bile ducts. Genomic and transcriptomic studies revealed that increased metabolic stress during the rapid growth and development of F. hepatica is balanced with the up-regulation of the thiol-independent antioxidant system. In this cascade system thioredoxin/glutathione reductase (TGR) reduces thioredoxin (Trx), which then reduces and activates peroxiredoxin (Prx), whose major function is to protect cells against the damaging hydrogen peroxide free radicals. F. hepatica expresses a single TGR, three Trx and three Prx genes; however, the transcriptional expression of Trx1 and Prx1 far out-weighs (>50-fold) other members of their family, and both are major components of the parasite secretome. While Prx1 possesses a leader signal peptide that directs its secretion through the classical pathway and explains why this enzyme is found freely soluble in the secretome, Trx1 lacks a leader peptide and is secreted via an alternative pathway that packages the majority of this enzyme into extracellular vesicles (EVs). Here we propose that F. hepatica Prx1 and Trx1 do not function as part of the parasite’s stress-inducible thiol-dependant cascade, but play autonomous roles in defence against the general anti-pathogen oxidative burst by innate immune cells, in the modulation of host immune responses and regulation of inflammation.

Published

2021

10. Single‐Cell Immune Profiling in Coronary Artery Disease: The Role of State‐of‐the‐Art Immunophenotyping With Mass Cytometry in the Diagnosis of Atherosclerosis

Author

Katharine A. Kott, Stephen T. Vernon, Thomas Hansen, Macha de Dreu, Souvik K. Das, Joseph Powell, Barbara Fazekas de St Groth, Belinda A. Di Bartolo, Helen M. McGuire, and Gemma A. Figtree

Subjects

atherosclerosis, coronary artery disease, immune system, inflammation, mass cytometry, Diseases of the circulatory (Cardiovascular) system, RC666-701

Abstract

Abstract Coronary artery disease remains the leading cause of death globally and is a major burden to every health system in the world. There have been significant improvements in risk modification, treatments, and mortality; however, our ability to detect asymptomatic disease for early intervention remains limited. Recent discoveries regarding the inflammatory nature of atherosclerosis have prompted investigation into new methods of diagnosis and treatment of coronary artery disease. This article reviews some of the highlights of the important developments in cardioimmunology and summarizes the clinical evidence linking the immune system and atherosclerosis. It provides an overview of the major serological biomarkers that have been associated with atherosclerosis, noting the limitations of these markers attributable to low specificity, and then contrasts these serological markers with the circulating immune cell subtypes that have been found to be altered in coronary artery disease. This review then outlines the technique of mass cytometry and its ability to provide high‐dimensional single‐cell data and explores how this high‐resolution quantification of specific immune cell subpopulations may assist in the diagnosis of early atherosclerosis in combination with other complimentary techniques such as single‐cell RNA sequencing. We propose that this improved specificity has the potential to transform the detection of coronary artery disease in its early phases, facilitating targeted preventative approaches in the precision medicine era.

Published

2020

11. Corrigendum: Pediatric Burn Survivors Have Long-Term Immune Dysfunction With Diminished Vaccine Response

Author

Blair Z. Johnson, Sonia McAlister, Helen M. McGuire, Vetrichevvel Palanivelu, Andrew Stevenson, Peter Richmond, Debra J. Palmer, Jessica Metcalfe, Susan L. Prescott, Fiona M. Wood, Barbara Fazekas de St Groth, Matthew D. Linden, Mark W. Fear, and Vanessa S. Fear

Subjects

non-severe burn injury, immunity, vaccination, mass cytometry, acute trauma, systemic, Immunologic diseases. Allergy, RC581-607

Published

2020

12. Pediatric Burn Survivors Have Long-Term Immune Dysfunction With Diminished Vaccine Response

Author

Blair Z. Johnson, Sonia McAlister, Helen M. McGuire, Vetrichevvel Palanivelu, Andrew Stevenson, Peter Richmond, Debra J. Palmer, Jessica Metcalfe, Susan L. Prescott, Fiona M. Wood, Barbara Fazekas de St Groth, Matthew D. Linden, Mark W. Fear, and Vanessa S. Fear

Subjects

non-severe burn injury, immunity, vaccination, mass cytometry, acute trauma, systemic, Immunologic diseases. Allergy, RC581-607

Abstract

Epidemiological studies have demonstrated that survivors of acute burn trauma are at long-term increased risk of developing a range of morbidities. The mechanisms underlying this increased risk remain unknown. This study aimed to determine whether burn injury leads to sustained immune dysfunction that may underpin long-term morbidity. Plasma and peripheral blood mononuclear cells were collected from 36 pediatric burn survivors >3 years after a non-severe burn injury (

Published

2020

13. Inflammation and Oral Contraceptive Use in Female Athletes Before the Rio Olympic Games

Author

Brianna Larsen, Amanda Cox, Candice Colbey, Michael Drew, Helen McGuire, Barbara Fazekas de St Groth, David Hughes, Nicole Vlahovich, Gordon Waddington, Louise Burke, Bronwen Lundy, Nicholas West, and Clare Minahan

Subjects

C-reactive protein, cytokines, contraception, athletes, sex hormones, Physiology, QP1-981

Abstract

This study investigated the association between synthetic ovarian hormone use [i.e., the oral contraceptive (OC) pill] and basal C-reactive protein (CRP), peripheral blood immune cell subsets, and circulating pro- and anti-inflammatory cytokine concentrations in elite female athletes. Elite female athletes (n = 53) selected in Rio Summer Olympic squads participated in this study; 25 were taking an OC (AthletesOC) and 28 were naturally hormonally cycling (AthletesNC). Venous blood samples were collected at rest for the determination of sex hormones, cortisol, CRP, peripheral blood mononuclear memory and naïve CD4+ T-cells, CD8+ T-cells and natural killer cells, as well as pro- and anti-inflammatory cytokine concentrations. C-reactive protein concentrations were elevated (p < 0.001) in AthletesOC (median = 2.02, IQR = 3.15) compared to AthletesNC (median = 0.57, IQR = 1.07). No differences were reported for cortisol, cytokines, or PBMC immune cell subsets, although there was a trend (p = 0.062) for higher IL-6 concentrations in AthletesNC. Female Olympians had substantially higher CRP concentrations, a marker of inflammation and tissue damage, before the Rio Olympic Games if they used an OC. Future research should examine the potential consequences for athlete performance/recovery so that, if necessary, practitioners can implement prevention programs.

Published

2020

14. Pretreatment Innate Cell Populations and CD4 T Cells in Blood Are Associated With Response to Immune Checkpoint Blockade in Melanoma Patients

Author

Mehdi R. Pirozyan, Helen M. McGuire, Abdullah Al Emran, Hsin-Yi Tseng, Jessamy C. Tiffen, Jenny H. Lee, Matteo S. Carlino, Alexander M. Menzies, Georgina V. Long, Richard A. Scolyer, Barbara Fazekas de St Groth, and Peter Hersey

Subjects

melanoma, cancer immunotherapy, NK cells, CyTOF, T cell exhaustion, CD4 T cells, Immunologic diseases. Allergy, RC581-607

Abstract

The development of changes in T cells, referred to as T cell exhaustion, has been suggested as a cause of primary or acquired resistance to immunotherapy by immune checkpoint blockade (ICB). A limited number of studies, largely performed on tumor infiltrating lymphocytes (TILs), has provided evidence in support of this hypothesis, but whether similar changes occur in circulating blood lymphocytes has received little attention. In the present study, a comprehensive analysis of peripheral blood leukocytes from 42 patients taken over the course of treatment with anti-PD-1 was undertaken. The patients included those grouped as responders (who did not progress), primary non-responders (primary resistance) and those with acquired resistance (who initially responded then subsequently progressed). Analysis included surface markers of exhaustion, production of cytokines following in vitro stimulation, and assessment of transcription factor levels associated with T cell exhaustion. There were differences in innate cell populations between responders and non-responders at baseline and maintained throughout therapy. Frequencies of total and classical CD14+CD16− monocytes were higher and the major subset of NK cells (CD16hiCD56+) was significantly smaller in the primary resistance group compared with responders. However, differences in peripheral blood expression of exhaustion markers were not evident between the treatment groups. T cell exhaustion markers were expressed in practically all patients and the major observation was an increase in CD39 on CD4 T cells during treatment. The results confirm the association of Eomes transcription factor with T cell exhaustion but levels of expression and the ratio with T-bet over Eomes did not differ between the patient groups. Thus, peripheral blood expression of T cell exhaustion markers does not distinguish between responders and non-responders to anti-PD-1 therapy. CD4 T cell expression of IFNγ also differed in pre-treatment samples, indicating that predictors of response unrelated to exhaustion may be present in peripheral blood. The association of response with innate cell populations and CD4 T cell responses requires further study.

Published

2020

15. Mass cytometry reveals immune signatures associated with cytomegalovirus (CMV) control in recipients of allogeneic haemopoietic stem cell transplant and CMV‐specific T cells

Author

Helen M McGuire, Simone Rizzetto, Barbara P Withers, Leighton E Clancy, Selmir Avdic, Lauren Stern, Ellis Patrick, Barbara Fazekas de St Groth, Barry Slobedman, David J Gottlieb, Fabio Luciani, and Emily Blyth

Subjects

adoptive T‐cell therapy, CyTOF, haemopoietic stem cell transplant, immune reconstitution, immunotherapy, mass cytometry, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Objectives Cytomegalovirus (CMV) is known to have a significant impact on immune recovery post‐allogeneic haemopoietic stem cell transplant (HSCT). Adoptive therapy with donor‐derived or third‐party virus‐specific T cells (VST) can restore CMV immunity leading to clinical benefit in prevention and treatment of post‐HSCT infection. We developed a mass cytometry approach to study natural immune recovery post‐HSCT and assess the mechanisms underlying the clinical benefits observed in recipients of VST. Methods A mass cytometry panel of 38 antibodies was utilised for global immune assessment (72 canonical innate and adaptive immune subsets) in HSCT recipients undergoing natural post‐HSCT recovery (n = 13) and HSCT recipients who received third‐party donor‐derived CMV‐VST as salvage for unresponsive CMV reactivation (n = 8). Results Mass cytometry identified distinct immune signatures associated with CMV characterised by a predominance of innate cells (monocytes and NK) seen early and an adaptive signature with activated CD8+ T cells seen later. All CMV‐VST recipients had failed standard antiviral pharmacotherapy as a criterion for trial involvement; 5/8 had failed to develop the adaptive immune signature by study enrolment despite significant CMV antigen exposure. Of these, VST administration resulted in development of the adaptive signature in association with CMV control in three patients. Failure to respond to CMV‐VST in one patient was associated with persistent absence of the adaptive immune signature. Conclusion The clinical benefit of CMV‐VST may be mediated by the recovery of an adaptive immune signature characterised by activated CD8+ T cells.

Published

2020

16. Mass Cytometry Discovers Two Discrete Subsets of CD39−Treg Which Discriminate MGUS From Multiple Myeloma

Author

Felix Marsh-Wakefield, Annabel Kruzins, Helen M. McGuire, Shihong Yang, Christian Bryant, Barbara Fazekas de St. Groth, Najah Nassif, Scott N. Byrne, John Gibson, Christina Brown, Stephen Larsen, Derek McCulloch, Richard Boyle, Georgina Clark, Douglas Joshua, Phoebe Joy Ho, and Slavica Vuckovic

Subjects

MGUS, multiple myeloma, mass cytometry, FlowSom, Treg, Immunologic diseases. Allergy, RC581-607

Abstract

Multiple Myeloma (MM) is preceded by the clinically stable condition monoclonal gammopathy of undetermined significance (MGUS). Critical immune events that discriminate MGUS from newly diagnosed MM (ND)MM patients remain unknown, but may involve changes in the regulatory T cell (Treg) compartment that favor myeloma growth. To address this possibility, we used mass cytometry and the unsupervised clustering algorithm Flow self-organizing map (FlowSOM) to interrogate the distribution of multiple subsets within CD25+CD127low/negTreg in matched bone marrow (BM) and peripheral blood (PB) of MGUS and NDMM patients. Both mass cytometry and flow cytometry confirmed a trend toward prevalence of CD39−Treg within the Treg compartment in BM and PB of NDMM patients compared to CD39−Treg in MGUS patients. FlowSOM clustering displayed a phenotypic organization of Treg into 25 metaclusters that confirmed Treg heterogeneity. It identified two subsets which emerged within CD39−Treg of NDMM patients that were negligible or absent in CD39−Treg of MGUS patients. One subset was found in both BM and PB which phenotypically resembled activated Treg based on CD45RO, CD49d, and CD62L expression; another subset resembled BM-resident Treg based on its tissue-resident CD69+CD62L−CD49d− phenotype and restricted location within the BM. Both subsets co-expressed PD-1 and TIGIT, but PD-1 was expressed at higher levels on BM-resident Treg than on activated Treg. Within BM, both subsets had limited Perforin and Granzyme B production, whilst activated Treg in PB acquired high Perforin and Granzyme B production. In conclusion, the use of mass cytometry and FlowSOM clustering discovered two discrete subsets of CD39−Treg which are discordant in MGUS and NDMM patients and may be permissive of myeloma growth which warrants further study. Understanding the regulatory properties of these subsets may also advance MGUS and MM diagnosis, prognosis, and therapeutic implications for MM patients.

Published

2019

17. Mass Cytometry for the Assessment of Immune Reconstitution After Hematopoietic Stem Cell Transplantation

Author

Lauren Stern, Helen McGuire, Selmir Avdic, Simone Rizzetto, Barbara Fazekas de St Groth, Fabio Luciani, Barry Slobedman, and Emily Blyth

Subjects

mass cytometry, cytometry by time-of-flight, hematopoietic stem cell transplantation, immune reconstitution, CyTOF, HSCT, Immunologic diseases. Allergy, RC581-607

Abstract

Mass cytometry, or Cytometry by Time-Of-Flight, is a powerful new platform for high-dimensional single-cell analysis of the immune system. It enables the simultaneous measurement of over 40 markers on individual cells through the use of monoclonal antibodies conjugated to rare-earth heavy-metal isotopes. In contrast to the fluorochromes used in conventional flow cytometry, metal isotopes display minimal signal overlap when resolved by single-cell mass spectrometry. This review focuses on the potential of mass cytometry as a novel technology for studying immune reconstitution in allogeneic hematopoietic stem cell transplant (HSCT) recipients. Reconstitution of a healthy donor-derived immune system after HSCT involves the coordinated regeneration of innate and adaptive immune cell subsets in the recipient. Mass cytometry presents an opportunity to investigate immune reconstitution post-HSCT from a systems-level perspective, by allowing the phenotypic and functional features of multiple cell populations to be assessed simultaneously. This review explores the current knowledge of immune reconstitution in HSCT recipients and highlights recent mass cytometry studies contributing to the field.

Published

2018

18. Circulating Endothelial Progenitor Cells Present an Inflammatory Phenotype and Function in Patients With Alcoholic Liver Cirrhosis

Author

Savneet Kaur, Rashi Sehgal, Saggere M. Shastry, Geoffrey McCaughan, Helen M. McGuire, Barbara Fazekas St de Groth, Shiv Sarin, Nirupma Trehanpati, and Devanshi Seth

Subjects

angiogenesis, alcoholic liver cirrhosis, endothelial progenitor cells, inflammation, mass cytometry CyTOF, CD45, Physiology, QP1-981

Abstract

Background and Aim: Endothelial progenitor cells (EPCs) have been implicated in liver injury and repair. However, the phenotype and potential of these heterogenous EPCs remain elusive. In particular, their involvement in the pathogenesis of alcoholic liver cirrhosis (ALC) remains unclear. The current study extensively characterized the phenotype and functions of EPCs to understand their role in ALC pathogenesis.Methods: Circulating EPCs were identified as CD34+CD133+CD31+ cells by flow cytometer in ALC patients (n = 7) and healthy controls (HC, n = 7). A comprehensive characterization of circulating EPCs using more than 30 phenotype markers was performed by mass cytometer time of flight (CyTOF) in an independent cohort of age and gender matched ALC patients (n = 4) and controls (n = 5). Ex vivo cultures of circulating EPCs from ALC patients (n = 20) and controls (n = 18) were also tested for their functions, including colony formation, LDL uptake, lectin binding and cytokine secretion (ELISA).Results: Three distinct populations of circulating EPCs (CD34+CD133+CD31+) were identified, classified on their CD45 expression (negative: CD45−; intermediate: CD45int; high: CD45hi). CD45int and CD45hi EPCs significantly increased in ALC patients compared to controls (p-val = 0.006). CyTOF data showed that CD45hi EPCs were distinct from CD45− and CD45int EPCs, with higher expression of T cell and myeloid markers, including CD3, CD4, HLA-DR, and chemokine receptors, CCR2, CCR5, CCR7, and CX3CR1. Similar to circulating EPCs, percentage of CD45hiCD34+CD31+ EPCs in ex-vivo cultures from patients, were significantly higher compared to controls (p < 0.05). Cultured EPCs from patients also showed increased LDL uptake, lectin binding and release of TNF-alpha, RANTES, FGF-2, and VEGF.Conclusions: We report the first extensive characterization of circulating human EPCs with distinct EPC subtypes. Increase in CD45hi EPC subtype in ALC patients with enhanced functions, inflammatory cytokines and angiogenic mediators in patients suggests an inflammatory role for these cells in ALC.

Published

2018

19. A blood dendritic cell vaccine for acute myeloid leukemia expands anti-tumor T cell responses at remission

Author

Jennifer L. Hsu, Christian E. Bryant, Michael S. Papadimitrious, Benjamin Kong, Robin E. Gasiorowski, Daniel Orellana, Helen M. McGuire, Barbara Fazekas de St Groth, Douglas E. Joshua, P. Joy Ho, Stephen Larsen, Harry J. Iland, John Gibson, Georgina J. Clark, Phillip D. Fromm, and Derek NJ Hart

Subjects

acute myeloid leukemia, blood dendritic cell, immunotherapy, allogeneic haematopoietic stem cell transplantation, chemotherapy, t cell landscape, checkpoint inhibitor, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Only modest advances in AML therapy have occurred in the past decade and relapse due to residual disease remains the major challenge. The potential of the immune system to address this is evident in the success of allogeneic transplantation, however this leads to considerable morbidity. Dendritic cell (DC) vaccination can generate leukemia-specific autologous immunity with little toxicity. Promising results have been achieved with vaccines developed in vitro from purified monocytes (Mo-DC). We now demonstrate that blood DC (BDC) have superior function to Mo-DC. Whilst BDC are reduced at diagnosis in AML, they recover following chemotherapy and allogeneic transplantation, can be purified using CMRF-56 antibody technology, and can stimulate functional T cell responses. While most AML patients in remission had a relatively normal T cell landscape, those who had received fludarabine as salvage therapy have persistent T cell abnormalities including reduced number, altered subset distribution, failure to expand, and increased activation-induced cell death. Furthermore, PD-1 and TIM-3 are increased on CD4T cells in AML patients in remission and their blockade enhances the expansion of leukemia-specific T cells. This confirms the feasibility of a BDC vaccine to consolidate remission in AML and suggests it should be tested in conjunction with checkpoint blockade.

Published

2018

20. Correction to: Expansion and activation of distinct central memory T lymphocyte subsets in complex regional pain syndrome

Author

Marc A. Russo, Nathan T. Fiore, Caryn van Vreden, Dominic Bailey, Danielle M. Santarelli, Helen M. McGuire, Barbara Fazekas de St Groth, and Paul J. Austin

Subjects

Neurology. Diseases of the nervous system, RC346-429

Abstract

Following publication of the original article [1], the authors reported an error in Figure 4 as the wrong figure was used.

Published

2019

21. A systems biology approach to the analysis of subset-specific responses to lipopolysaccharide in dendritic cells.

Author

David G Hancock, Elena Shklovskaya, Thomas V Guy, Reza Falsafi, Chris D Fjell, William Ritchie, Robert E W Hancock, and Barbara Fazekas de St Groth

Subjects

Medicine, Science

Abstract

Dendritic cells (DCs) are critical for regulating CD4 and CD8 T cell immunity, controlling Th1, Th2, and Th17 commitment, generating inducible Tregs, and mediating tolerance. It is believed that distinct DC subsets have evolved to control these different immune outcomes. However, how DC subsets mount different responses to inflammatory and/or tolerogenic signals in order to accomplish their divergent functions remains unclear. Lipopolysaccharide (LPS) provides an excellent model for investigating responses in closely related splenic DC subsets, as all subsets express the LPS receptor TLR4 and respond to LPS in vitro. However, previous studies of the LPS-induced DC transcriptome have been performed only on mixed DC populations. Moreover, comparisons of the in vivo response of two closely related DC subsets to LPS stimulation have not been reported in the literature to date. We compared the transcriptomes of murine splenic CD8 and CD11b DC subsets after in vivo LPS stimulation, using RNA-Seq and systems biology approaches. We identified subset-specific gene signatures, which included multiple functional immune mediators unique to each subset. To explain the observed subset-specific differences, we used a network analysis approach. While both DC subsets used a conserved set of transcription factors and major signalling pathways, the subsets showed differential regulation of sets of genes that 'fine-tune' the network Hubs expressed in common. We propose a model in which signalling through common pathway components is 'fine-tuned' by transcriptional control of subset-specific modulators, thus allowing for distinct functional outcomes in closely related DC subsets. We extend this analysis to comparable datasets from the literature and confirm that our model can account for cell subset-specific responses to LPS stimulation in multiple subpopulations in mouse and man.

Published

2014

22. The role of antigen-competitive dynamics in regulating the immune response

Author

Pooladvand, Pantea, Kim, Peter S., and Groth, Barbara Fazekas de St

Subjects

Mathematics - Dynamical Systems

Abstract

The clonal expansion of T cells during an infection is tightly regulated to ensure an appropriate immune response against invading pathogens. Although experiments have mapped the trajectory from expansion to contraction, the interplay between mechanisms that control this response are not fully understood. Based on experimental data, we propose a model in which the dynamics of CD4+ T cell expansion is controlled through the interactions between T cells and antigen-presenting cells, where T cell stimulation is proportional to antigen availability and antigen availability is regulated through downregulation of antigen by T cells. This antigen-dependent-feedback mechanism operates alongside an intrinsic reduction in cell proliferation rate that may also be responsible for slowing expansion. Our model can successfully predict T cell recruitment rates into division, expansion and clonal burst size per cell when initial precursors are varied or when T cells are introduced late into an ongoing immune response. Importantly, the findings demonstrate that a feedback mechanism between T cells and antigen presenting cells, along with a reduction in cell proliferation rate, can explain the ability of the immune system to adapt its response to variations in initial conditions or changes that occur later in the response, ensuring a robust yet controlled line of defence against pathogens., Comment: 19 pages, 14 figures, 1 table

Published

2021

23. Partial body cryotherapy exposure drives acute redistribution of circulating lymphocytes: preliminary findings

Author

Rose, Catriona L., McGuire, Helen, Graham, Kenneth, Siegler, Jason, de St Groth, Barbara Fazekas, Caillaud, Corinne, and Edwards, Kate M.

Published

2023

24. Inverse relationship between oligoclonal expanded CD69− TTE and CD69+ TTE cells in bone marrow of multiple myeloma patients

Author

Vuckovic, Slavica, Bryant, Christian E., Lau, Ka Hei Aleks, Yang, Shihong, Favaloro, James, McGuire, Helen M., Clark, Georgina, de St. Groth, Barbara Fazekas, Marsh-Wakefield, Felix, Nassif, Najah, Abadir, Edward, Vanguru, Vinay, McCulloch, Derek, Brown, Christina, Larsen, Stephen, Dunkley, Scott, Khoo, Liane, Gibson, John, Boyle, Richard, Joshua, Douglas, and Ho, P. Joy

Published

2020

25. Correction to: Partial body cryotherapy exposure drives acute redistribution of circulating lymphocytes: preliminary findings

Author

Rose, Catriona L., McGuire, Helen, Graham, Kenneth, Siegler, Jason, de St Groth, Barbara Fazekas, Caillaud, Corinne, and Edwards, Kate M.

Published

2023

26. CD127 expression inversely correlates with FoxP3 and suppressive function of human CD4+ T reg cells

Author

Liu, Weihong, Putnam, Amy L, Xu-yu, Zhou, Szot, Gregory L, Lee, Michael R, Zhu, Shirley, Gottlieb, Peter A, Kapranov, Philipp, Gingeras, Thomas R, de St. Groth, Barbara Fazekas, Clayberger, Carol, Soper, David M, Ziegler, Steven F, and Bluestone, Jeffrey A

Subjects

Clinical Research, Aetiology, 2.1 Biological and endogenous factors, Adolescent, Adult, Biomarkers, CD4 Lymphocyte Count, Cells, Cultured, Diabetes Mellitus, Type 1, Forkhead Transcription Factors, Humans, Immunologic Memory, Middle Aged, Receptors, Interleukin-2, Receptors, Interleukin-7, T-Lymphocytes, Regulatory, Medical and Health Sciences, Immunology

Abstract

Regulatory T (T reg) cells are critical regulators of immune tolerance. Most T reg cells are defined based on expression of CD4, CD25, and the transcription factor, FoxP3. However, these markers have proven problematic for uniquely defining this specialized T cell subset in humans. We found that the IL-7 receptor (CD127) is down-regulated on a subset of CD4(+) T cells in peripheral blood. We demonstrate that the majority of these cells are FoxP3(+), including those that express low levels or no CD25. A combination of CD4, CD25, and CD127 resulted in a highly purified population of T reg cells accounting for significantly more cells that previously identified based on other cell surface markers. These cells were highly suppressive in functional suppressor assays. In fact, cells separated based solely on CD4 and CD127 expression were anergic and, although representing at least three times the number of cells (including both CD25(+)CD4(+) and CD25(-)CD4(+) T cell subsets), were as suppressive as the "classic" CD4(+)CD25(hi) T reg cell subset. Finally, we show that CD127 can be used to quantitate T reg cell subsets in individuals with type 1 diabetes supporting the use of CD127 as a biomarker for human T reg cells.

Published

2006

27. Mapping the extent of heterogeneity of human CCR5+ CD4+ T cells in peripheral blood and lymph nodes

Author

Zaunders, John, Munier, C. Mee Ling, McGuire, Helen M., Law, Hannah, Howe, Annett, Xu, Yin, de St Groth, Barbara Fazekas, Schofield, Peter, Christ, Daniel, Milner, Brad, Obeid, Solange, Dyer, Wayne B., Saksena, Nitin K., and Kelleher, Anthony D.

Published

2020

28. A High-Throughput Colorimetric Microplate Assay for Determination of Plasma Arginase Activity

Author

Natalie J. Smith, Mahnaz Maddahfar, Bavani Gunasegaran, Helen M. McGuire, and Barbara Fazekas de St Groth

Published

2023

29. Correction to: Partial body cryotherapy exposure drives acute redistribution of circulating lymphocytes: preliminary findings

Author

Rose, Catriona L., primary, McGuire, Helen, additional, Graham, Kenneth, additional, Siegler, Jason, additional, de St Groth, Barbara Fazekas, additional, Caillaud, Corinne, additional, and Edwards, Kate M., additional

Published

2022

30. Partial body cryotherapy exposure drives acute redistribution of circulating lymphocytes: preliminary findings

Author

Rose, Catriona L., primary, McGuire, Helen, additional, Graham, Kenneth, additional, Siegler, Jason, additional, de St Groth, Barbara Fazekas, additional, Caillaud, Corinne, additional, and Edwards, Kate M., additional

Published

2022

31. Selective Treg reconstitution during lymphopenia normalizes DC costimulation and prevents graft-versus-host disease

Author

Bolton, Holly A., Zhu, Erhua, Terry, Alexandra M., Guy, Thomas V., Koh, Woon-Puay, Tan, Sioh-Yang, Power, Carl A., Bertolino, Patrick, Lahl, Katharina, Sparwasser, Tim, Shklovskaya, Elena, and de St. Groth, Barbara Fazekas

Subjects

Prevention, Research, Risk factors, Health aspects, Lymphocytopenia -- Prevention -- Analysis -- Risk factors -- Research, Graft vs. host disease -- Prevention -- Research, Dendritic cells -- Health aspects, Lymphocytopenia, Dendritic cells, Graft versus host reaction

Abstract

Introduction Achieving satisfactory immune reconstitution in lymphopenic subjects remains a major problem in many clinical settings, including following autologous or allogeneic hematopoietic stem-cell transplantation (HSCT) and recovery from cancer chemotherapy. [...], Regulatory T cells (Tregs) have been shown to enhance Immune reconstitution and prevent graft-versus-host disease (GVHD) after hematopoietic stem cell transplantation; however, it is unclear how Tregs mediate these effects. Here, we developed a model to examine the mechanism of Treg-dependent regulation of immune reconstitution. Lymphopenic mice were selectively reconstituted with Tregs prior to transfer of conventional CD4* T cells. Full Treg reconstitution prevented the rapid oligoclonal proliferation that gives rise to pathogenic CD4 effector T cells, while preserving the slow homeostatic form of lymphopenia-induced peripheral expansion that repopulates a diverse peripheral T cell pool. Treg-mediated CTLA-4-dependent downregulation of CD80/CD86 on DCs was critical for inhibition of rapid proliferation and was a function of the Treg/DC ratio achieved by reconstitution. In an allogeneic BM transplant model, selective Treg reconstitution before T cell transfer also normalized DC costimulation and provided complete protection against GVHD. In contrast, cotransfer of Tregs was not protective. Our results indicate that achieving optimal recovery from lymphopenia should aim to improve early Treg reconstitution in order to increase the relative number of Tregs to DCs and thereby inhibit spontaneous oligoclonal T cell proliferation.

Published

2015

32. Langerhans cells are precommitted to immune tolerance induction

Author

Shklovskaya, Elena, O'Sullivan, Brendan J., Ng, Lai Guan, Roediger, Ben, Thomas, Ranjeny, Weninger, Wolfgang, and de St Groth, Barbara Fazekas

Published

2011

33. Bacterial antigen is directly delivered to the draining lymph nodes and activates CD8 + T cells during Staphylococcus aureus skin infection

Author

Ben Roediger, Neville Firth, Anthony J. Brzoska, Gyohei Egawa, Barbara Fazekas de, Lois L. Cavanagh, Thomas V. Guy, Wolfgang Weninger, and Szun S. Tay

Subjects

0301 basic medicine, T cell, Immunology, Cell Biology, Biology, Acquired immune system, medicine.disease_cause, Microbiology, 03 medical and health sciences, CTL, 030104 developmental biology, 0302 clinical medicine, Immune system, medicine.anatomical_structure, Staphylococcus aureus, medicine, Immunology and Allergy, Cytotoxic T cell, Bacterial antigen, CD8, 030215 immunology

Abstract

Staphylococcus aureus is one of the most common causes of community- and hospital-acquired bacterial infection worldwide. While neutrophils play an important role in anti-S. aureus immune defense, the role of adaptive immunity is less clear. In this study, we generated a model antigen-expressing S. aureus strain to investigate the dynamics and magnitude of T cell immune responses against this pathogen. We demonstrate that S. aureus is delivered to the draining lymph nodes (LNs) by lymphatic flow immediately after intradermal inoculation. There, the bacterium initiates CD8+ cytotoxic T lymphocyte (CTL) proliferation via activating LN-resident dendritic cells. Large numbers of neutrophils are recruited to the draining LNs to engulf bacteria; however, neutrophil depletion did not impact on CTL proliferation, despite increasing bacterial burden. Tissue-resident memory T cells were formed in the skin at bacteria-inoculated sites. Yet, blood and tissue-resident memory T cells failed to prevent secondary cutaneous S. aureus infection. Our study defines the delivery kinetics of S. aureus from the skin and suggests that CTLs are dispensable for protection against skin infections.

Published

2020

34. Rapidly expanded partially HLA DRB1–matched fungus-specific T cells mediate in vitro and in vivo antifungal activity

Author

Barbara Fazekas de St Groth, Leighton Clancy, Gloria Castellano-Gonzalez, Ziduo Li, Luigina Romani, David Gottlieb, Giorgia Renga, Fabio Luciani, Marina M. Bellet, Marilena Pariano, Brendan Hughes, Helen M. McGuire, Selmir Avdic, and Mandeep Singh

Subjects

Antifungal Agents, Immunobiology and Immunotherapy, Population, Antigen-Presenting Cells, Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Antigen, In vivo, Animals, Humans, education, 030304 developmental biology, 0303 health sciences, education.field_of_study, CD137, Fungi, Hematopoietic Stem Cell Transplantation, Hematology, Colony-stimulating factor, Acquired immune system, Fungal antigen, In vitro, 3. Good health, 030220 oncology & carcinogenesis, Immunology, HLA-DRB1 Chains

Abstract

Invasive fungal infections are a major cause of disease and death in immunocompromised hosts, including patients undergoing allogeneic hematopoietic stem cell transplant (HSCT). Recovery of adaptive immunity after HSCT correlates strongly with recovery from fungal infection. Using initial selection of lymphocytes expressing the activation marker CD137 after fungal stimulation, we rapidly expanded a population of mainly CD4+ T cells with potent antifungal characteristics, including production of tumor necrosis factor α, interferon γ, interleukin-17, and granulocyte-macrophage colony stimulating factor. Cells were manufactured using a fully good manufacturing practice–compliant process. In vitro, the T cells responded to fungal antigens presented on fully and partially HLA-DRB1 antigen–matched presenting cells, including when the single common DRB1 antigen was allelically mismatched. Administration of antifungal T cells lead to reduction in the severity of pulmonary and cerebral infection in an experimental mouse model of Aspergillus. These data support the establishment of a bank of cryopreserved fungus-specific T cells using normal donors with common HLA DRB1 molecules and testing of partially HLA-matched third-party donor fungus-specific T cells as a potential therapeutic in patients with invasive fungal infection after HSCT.

Published

2020

35. Partial body cryotherapy exposure drives acute redistribution of circulating lymphocytes: preliminary findings

Author

Catriona L. Rose, Helen McGuire, Kenneth Graham, Jason Siegler, Barbara Fazekas de St Groth, Corinne Caillaud, and Kate M. Edwards

Subjects

Physiology, Physiology (medical), Public Health, Environmental and Occupational Health, Orthopedics and Sports Medicine, General Medicine

Abstract

Partial body cryotherapy (PBC) is proposed to alleviate symptoms of exercise-induced muscle damage (EIMD) by reducing associated inflammation. No studies have assessed acute PBC exposure on peripheral blood mononuclear cell mobilisation or compared these with cold water immersion (CWI), which may inform how PBC impacts inflammatory processes. This trial examined the impact of a single PBC exposure on circulating peripheral blood mononuclear cells compared to CWI or a control. 26 males were randomised into either PBC (3 min at − 110 to − 140 °C), CWI (3 min at 9 °C), or control (3 min at 24 °C), with blood samples, heart rate, and blood pressure taken before and after exposure. Cytometric analysis determined that CD8+ T-cell populations were significantly elevated after treatments, with PBC increasing CD8+ T cells to a greater degree than either CWI or CON. Natural killer cell counts were also elevated after PBC, with the increase attributed specifically to the CD56loCD16+ cytotoxic subset. This provides the first evidence for the effect of PBC exposure on redistribution of immune cells. An increase in circulating leukocyte subsets such as CD8+ T cells and CD56loCD16+ natural killer cells suggests that PBC may induce a transient mobilisation of lymphocytes. PBC may thus enable a more efficient trafficking of these cells from the circulation to the site of initial cellular insult from exercise, potentially accelerating the process of cellular recovery. This provides novel evidence on the use of PBC as a recovery treatment and may also have applicability in other clinical settings involving the recovery of damaged skeletal muscle.

Published

2022

36. 216.15: Natural History of CXCR5+ t Follicular-like Helper (TFH) Cells in Kidney Transplant Recipients With Rejection

Author

Brenda Rosales, Susan Wan, Nicole De La Mata, Bavani Gunasegaran, Angela C Webster, Helen Mcguire, Barbara Fazekas, and Kate Wyburn

Subjects

Transplantation

Published

2022

37. Role of Dendritic Cells in Induction of Tolerance and Immunity in Vivo

Author

de St. Groth, Barbara Fazekas, Cook, Matthew C., Smith, Adrian L., Wikstrom, Matthew E., Basten, Antony, and Ricciardi-Castagnoli, Paola, editor

Published

1997

38. Metabolite-based dietary supplementation in human type 1 diabetes is associated with microbiota and immune modulation

Author

Bell, Kirstine K.J., Saad, Sonia, Tillett, Bree B.J., McGuire, Helen H.M., Bordbar, Sara, Yap, Yu Anne, Nguyen, Long The, Wilkins, Marc M.R., Corley, Susan, Brodie, Shannon, Duong, Sussan, Wright, Courtney C.J., Twigg, Stephen, de St Groth, Barbara Fazekas, Harrison, Leonard L.C., Mackay, Charles R, Gurzov, Esteban Nicolas, Hamilton-Williams, Emma E.E., Mariño, Eliana, Bell, Kirstine K.J., Saad, Sonia, Tillett, Bree B.J., McGuire, Helen H.M., Bordbar, Sara, Yap, Yu Anne, Nguyen, Long The, Wilkins, Marc M.R., Corley, Susan, Brodie, Shannon, Duong, Sussan, Wright, Courtney C.J., Twigg, Stephen, de St Groth, Barbara Fazekas, Harrison, Leonard L.C., Mackay, Charles R, Gurzov, Esteban Nicolas, Hamilton-Williams, Emma E.E., and Mariño, Eliana

Abstract

Background: Short-chain fatty acids (SCFAs) produced by the gut microbiota have beneficial anti-inflammatory and gut homeostasis effects and prevent type 1 diabetes (T1D) in mice. Reduced SCFA production indicates a loss of beneficial bacteria, commonly associated with chronic autoimmune and inflammatory diseases, including T1D and type 2 diabetes. Here, we addressed whether a metabolite-based dietary supplement has an impact on humans with T1D. We conducted a single-arm pilot-and-feasibility trial with high-amylose maize-resistant starch modified with acetate and butyrate (HAMSAB) to assess safety, while monitoring changes in the gut microbiota in alignment with modulation of the immune system status. Results: HAMSAB supplement was administered for 6 weeks with follow-up at 12 weeks in adults with long-standing T1D. Increased concentrations of SCFA acetate, propionate, and butyrate in stools and plasma were in concert with a shift in the composition and function of the gut microbiota. While glucose control and insulin requirements did not change, subjects with the highest SCFA concentrations exhibited the best glycemic control. Bifidobacterium longum, Bifidobacterium adolescentis, and vitamin B7 production correlated with lower HbA1c and basal insulin requirements. Circulating B and T cells developed a more regulatory phenotype post-intervention. Conclusion: Changes in gut microbiota composition, function, and immune profile following 6 weeks of HAMSAB supplementation were associated with increased SCFAs in stools and plasma. The persistence of these effects suggests that targeting dietary SCFAs may be a mechanism to alter immune profiles, promote immune tolerance, and improve glycemic control for the treatment of T1D. Trial registration: ACTRN12618001391268. Registered 20 August 2018,https://www.anzctr.org.au/Trial/Registration/TrialReview.aspx?id=375792 [MediaObject not available: see fulltext.], SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2022

39. Additional file 1 of Metabolite-based dietary supplementation in human type 1 diabetes is associated with microbiota and immune modulation

Author

Bell, Kirstine J., Saad, Sonia, Tillett, Bree J., McGuire, Helen M., Bordbar, Sara, Yap, Yu Anne, Nguyen, Long T., Wilkins, Marc R., Corley, Susan, Brodie, Shannon, Duong, Sussan, Wright, Courtney J., Twigg, Stephen, de St Groth, Barbara Fazekas, Harrison, Leonard C., Mackay, Charles R., Gurzov, Esteban N., Hamilton-Williams, Emma E., and Mari��o, Eliana

Abstract

Additional file 1: Fig. S1. sPLS-DA plot loadings indicating the contribution of each taxa. Fig. S2. Gating Strategy for identification of immune cell phenotypes by CyTOF. Fig. S3. Immune cell phenotype changes following HAMSAB treatment. Fig. S4. Immune cell phenotype changes following HAMSAB treatment. Fig. S5. Circulating pro-inflammatory and anti-inflammatory cytokines measured in subjects at baseline, W6 and W12 following HAMSAB supplementation. Fig. S6. Correlations between concentration of SCFAs, clinical parameters, relative abundance of bacterial communities and significant changes in immune cell subsets. Table S1. Nutritional and gastrointestinal changes across time. Table S2. Functional pathways encoded by the gut microbiota changed after taking dietary supplement. Table S3. Upregulated KEGG pathway gene sets identified using the camera function of limma following 6-weeks of HAMSAB supplementation. Table S4. Results of differential gene expression testing with EdgeR and RUVseq comparing baseline and week 6. Table S5. Mass cytometry panel used for immunophenotyping.

Published

2022

40. Metabolite-based dietary supplementation in human type 1 diabetes is associated with microbiota and immune modulation

Author

Bell, Kirstine J., primary, Saad, Sonia, additional, Tillett, Bree J., additional, McGuire, Helen M., additional, Bordbar, Sara, additional, Yap, Yu Anne, additional, Nguyen, Long T., additional, Wilkins, Marc R., additional, Corley, Susan, additional, Brodie, Shannon, additional, Duong, Sussan, additional, Wright, Courtney J., additional, Twigg, Stephen, additional, de St Groth, Barbara Fazekas, additional, Harrison, Leonard C., additional, Mackay, Charles R., additional, Gurzov, Esteban N., additional, Hamilton-Williams, Emma E., additional, and Mariño, Eliana, additional

Published

2022

41. Metabolite-based dietary supplementation in human type 1 diabetes is associated with microbiota and immune modulation

Author

Sara Bordbar, Charles R. Mackay, Stephen M. Twigg, Eliana Mariño, Shannon Brodie, Sonia Saad, Marc R. Wilkins, Barbara Fazekas de St Groth, Long T. Nguyen, Emma E. Hamilton-Williams, Bree J. Tillett, Susan M. Corley, Courtney J. Wright, Helen M. McGuire, Yu Anne Yap, Kirstine J. Bell, Sussan Duong, Esteban Nicolas Gurzov, and Leonard C. Harrison

Subjects

medicine.medical_specialty, Type 1 diabetes, Bifidobacterium longum, food.ingredient, biology, business.industry, Insulin, medicine.medical_treatment, Type 2 diabetes, Butyrate, Gut flora, biology.organism_classification, medicine.disease, Immune system, Endocrinology, food, Internal medicine, medicine, Resistant starch, business

Abstract

BackgroundShort-chain fatty acids (SCFAs) produced by the gut microbiota have beneficial anti-inflammatory and gut homeostasis effects and prevent type 1 diabetes (T1D) in mice. Reduced SCFA production indicates a loss of beneficial bacteria, commonly associated with chronic autoimmune and inflammatory diseases, including T1D and type 2 diabetes. Here we addressed whether a metabolite-based dietary supplement has an impact on humans with T1D. We conducted a single-arm pilot-and-feasibility trial with high-amylose maize resistant starch modified with acetate and butyrate (HAMSAB) to assess safety, while monitoring changes in the microbiota in alignment with modulation of the immune system status.ResultsHAMSAB supplement was administered for six weeks with follow-up at 12 weeks in adults with long-standing T1D. Increased concentrations of SCFA acetate, propionate, and butyrate in stools and plasma were in concert with a shift in the composition and function of the gut microbiota. While glucose control and insulin requirements did not change, subjects with the highest SCFA concentrations exhibited the best glycemic control. Bifidobacterium longum, Bifidobacterium adolescentis, and vitamin B7 production correlated with lower HbA1c and basal insulin requirements. Circulating B and T cells developed a more regulatory phenotype post-intervention.ConclusionChanges in gut microbiota composition, function, and immune profile following six weeks of HAMSAB supplementation were associated with increased SCFAs in stools and plasma. The persistence of these effects suggests that targeting dietary SCFAs may be a mechanism to alter immune profiles, promote immune tolerance and improve glycemic control for the treatment of T1D.Trial registrationACTRN12618001391268. Registered 20 August 2018, https://www.anzctr.org.au/Trial/Registration/TrialReview.aspx?id=375792

Published

2021

42. Distinguishing human peripheral blood CD16+ myeloid cells based on phenotypic characteristics

Author

Michael S. Papadimitrious, Christian E Bryant, Derek N.J. Hart, Tsun-Ho Lo, Pablo A. Silveira, Ahmed H. Mekkawy, Xinsheng Ju, Barbara Fazekas de St Groth, Phillip D. Fromm, John Gibson, Elizabeth Newman, Helen M. McGuire, Jennifer Hsu, Adelina Romano, Georgina J. Clark, Fiona Kupresanin, Ilona Cunningham, Benjamin Y. Kong, Wei-Hsun Hsu, P. Mark Hogarth, and Edward Abadir

Subjects

0301 basic medicine, Myeloid, CD14, Lineage markers, Immunology, virus diseases, CD11c, chemical and pharmacologic phenomena, hemic and immune systems, Cell Biology, CD16, Biology, Molecular biology, CD19, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, immune system diseases, 030220 oncology & carcinogenesis, medicine, biology.protein, Immunology and Allergy, Stem cell

Abstract

Myeloid lineage cells present in human peripheral blood include dendritic cells (DC) and monocytes. The DC are identified phenotypically as HLA-DR+ cells that lack major cell surface lineage markers for T cells (CD3), B cells (CD19, CD20), NK cells (CD56), red blood cells (CD235a), hematopoietic stem cells (CD34), and Mo that express CD14. Both DC and Mo can be phenotypically divided into subsets. DC are divided into plasmacytoid DC, which are CD11c−, CD304+, CD85g+, and myeloid DC that are CD11c+. The CD11c+ DC are readily classified as CD1c+DC and CD141+ DC. Monocytes are broadly divided into the CD14+CD16− (classical) and CD14dimCD16+ subsets (nonclassical). A population of myeloid-derived cells that have DC characteristics, that is, HLA-DR+ and lacking lineage markers including CD14, but express CD16 are generally clustered with CD14dimCD16+ monocytes. We used high-dimensional clustering analyses of fluorescence and mass cytometry data, to delineate CD14+ monocytes, CD14dimCD16+ monocytes (CD16+Mo), and CD14− CD16+DC (CD16+DC). We sought to identify the functional and kinetic relationship of CD16+DC to CD16+Mo. We demonstrate that differentiation of CD16+DC and CD16+Mo during activation with IFNγ in vitro and as a result of an allo-hematopoietic cell transplant (HCT) in vivo resulted in distinct populations. Recovery of blood CD16+DC in both auto- and allo-(HCT) patients after myeloablative conditioning showed similar reconstitution and activation kinetics to CD16+Mo. Finally, we show that expression of the cell surface markers CD300c, CCR5, and CLEC5a can distinguish the cell populations phenotypically paving the way for functional differentiation as new reagents become available.

Published

2019

43. High-Dimensional Mass Cytometric Analysis Reveals an Increase in Effector Regulatory T Cells as a Distinguishing Feature of Colorectal Tumors

Author

Kirsten A Ward-Hartstonge, Roslyn A. Kemp, John L. McCall, Fran Munro, Edward S Taylor, Samuel E Norton, Julia Kh Leman, Helen M. McGuire, Barbara Fazekas de St Groth, and Michael A. Black

Subjects

Male, Colorectal cancer, T cell, Immunology, Population, chemical and pharmacologic phenomena, Cell Separation, Lymphocyte Activation, T-Lymphocytes, Regulatory, 03 medical and health sciences, Lymphocytes, Tumor-Infiltrating, 0302 clinical medicine, Immune system, T-Lymphocyte Subsets, medicine, Humans, Immunology and Allergy, Mass cytometry, IL-2 receptor, education, Aged, education.field_of_study, Chemistry, FOXP3, hemic and immune systems, Middle Aged, medicine.disease, Phenotype, medicine.anatomical_structure, Cancer research, Female, Colorectal Neoplasms, 030215 immunology

Abstract

T cell infiltration of tumors plays an important role in determining colorectal cancer disease progression and has been incorporated into the Immunoscore prognostic tool. In this study, mass cytometry was used to demonstrate a significant increase in the frequency of both conventional CD25+FOXP3+CD127lo regulatory T cells (Tregs) as well as BLIMP-1+ Tregs in the tumor compared with nontumor bowel (NTB) of the same patients. Network cluster analyses using SCAFFoLD, VorteX, and CITRUS revealed that an increase in BLIMP-1+ Tregs was a single distinguishing feature of the tumor tissue compared with NTB. BLIMP-1+ Tregs represented the most significantly enriched T cell population in the tumor compared with NTB. The enrichment of ICOS, CD45RO, PD-1, PDL-1, LAG-3, CTLA-4, and TIM-3 on BLIMP-1+ Tregs suggests that BLIMP-1+ Tregs have a more activated phenotype than conventional Tregs and may play a role in antitumor immune responses.

Published

2019

44. Immunoprofiling reveals cell subsets associated with the trajectory of cytomegalovirus reactivation post stem cell transplantation

Author

Lauren Stern, Helen M. McGuire, Selmir Avdic, Barbara Fazekas de St Groth, David Gottlieb, Allison Abendroth, Emily Blyth, and Barry Slobedman

Subjects

Multidisciplinary, Cytomegalovirus Infections, Hematopoietic Stem Cell Transplantation, General Physics and Astronomy, Cytomegalovirus, Humans, General Chemistry, General Biochemistry, Genetics and Molecular Biology

Abstract

Human cytomegalovirus reactivation is a major opportunistic infection after allogeneic haematopoietic stem cell transplantation and has a complex relationship with post-transplant immune reconstitution. Here, we use mass cytometry to define patterns of innate and adaptive immune cell reconstitution at key phases of human cytomegalovirus reactivation in the first 100 days post haematopoietic stem cell transplantation. Human cytomegalovirus reactivation is associated with the development of activated, memory T-cell profiles, with faster effector-memory CD4+ T-cell recovery in patients with low-level versus high-level human cytomegalovirus DNAemia. Mucosal-associated invariant T cell levels at the initial detection of human cytomegalovirus DNAemia are significantly lower in patients who subsequently develop high-level versus low-level human cytomegalovirus reactivation. Our data describe distinct immune signatures that emerged with human cytomegalovirus reactivation after haematopoietic stem cell transplantation, and highlight Mucosal-associated invariant T cell levels at the first detection of reactivation as a marker that may be useful to anticipate the magnitude of human cytomegalovirus DNAemia.

Published

2021

45. Immune Cell Profiling Reveals MAIT and Effector Memory CD4+ T Cell Recovery Link to Control of Cytomegalovirus Reactivation after Stem Cell Transplant

Author

Emily Blyth, Selmir Avdic, David Gottlieb, Helen M. McGuire, Barry Slobedman, Lauren Stern, Allison Abendroth, and Barbara Fazekas de St Groth

Subjects

Human cytomegalovirus, Opportunistic infection, Cell, biochemical phenomena, metabolism, and nutrition, Biology, medicine.disease, Transplantation, Haematopoiesis, medicine.anatomical_structure, Immune system, Immunology, medicine, Mass cytometry, Stem cell

Abstract

SummaryHuman cytomegalovirus (HCMV) reactivation is a major opportunistic infection after allogeneic haematopoietic stem cell transplantation and has a complex relationship with post-transplant immune reconstitution. Here, we used mass cytometry to comprehensively define global patterns of innate and adaptive immune cell reconstitution at key phases of HCMV reactivation (before detection, initial detection, peak and near resolution) in the first 100 days post-transplant. In addition to identifying patterns of immune reconstitution in those with or without HCMV reactivation, we found mucosal-associated invariant T (MAIT) cell levels at the initial detection of HCMV DNAemia distinguished patients who subsequently developed low-level versus high-level HCMV reactivation. In addition, early recovery of effector-memory CD4+ T cells distinguished low-level and high-level reactivation. Our data describe distinct immune signatures that emerged with HCMV reactivation post-HSCT, and highlight MAIT cell levels at the initial detection of reactivation as a potential prognostic marker to guide clinical decisions regarding pre-emptive therapy.

Published

2021

46. Comparison of Single and Repeated Dosing of Anti-Inflammatory Human Umbilical Cord Mesenchymal Stromal Cells in a Mouse Model of Polymicrobial Sepsis

Author

Senthilkumar Alagesan, Cristina Català, María Velasco-de Andrés, Stephen J. Elliman, Matthew D. Griffin, Francisco Lozano, Barbara Fazekas, Callum M. Conroy, Luke Watson, Neema Negi, Olivia Ng, and Jared Q. Gerlach

Subjects

Pathology, medicine.medical_specialty, Text mining, medicine.anatomical_structure, business.industry, medicine.drug_class, Mesenchymal stem cell, Repeated dosing, Medicine, business, Polymicrobial sepsis, Umbilical cord, Anti-inflammatory

Abstract

Background Mesenchymal stromal cells (MSCs) ameliorate pre-clinical sepsis and sepsis-associated acute kidney injury (SA-AKI) but clinical trials of single-dose MSCs have not indicated robust efficacy. This study investigated immunomodulatory effects of a novel MSC product (CD362-selected human umbilical cord-derived MSCs [hUC-MSCs]) in mouse endotoxemia and polymicrobial sepsis models. Methods Initially, mice received intra-peritoneal (i.p.) lipopolysaccharide (LPS) followed by single i.p. doses of hUC-MSCs or vehicle. Next, mice underwent cecal ligation and puncture (CLP) followed by intravenous (i.v.) doses of hUC-MSCs at 4 hours or 4 and 28 hours. Analyses included serum/plasma assays of biochemical indices, inflammatory mediators and the AKI biomarker NGAL; multi-color flow cytometry of peritoneal macrophages (LPS) and intra-renal immune cell subpopulations (CLP) and histology/immunohistochemistry of kidney (CLP). Results At 72 hours post-LPS injections, hUC-MSCs reduced serum inflammatory mediators and peritoneal macrophage M1/M2 ratio. Repeated, but not single, hUC-MSC doses administered at 48 hours post-CLP resulted in increased survival, lower serum concentrations of inflammatory mediators, lower plasma NGAL and reversal of sepsis-associated depletion of intra-renal T-cell and myeloid cell subpopulations. Hierarchical clustering analysis of all 48-hour serum/plasma analytes demonstrated partial co-clustering of repeated-dose hUC-MSC CLP animals with a Sham group but did not reveal a distinct signature of response to therapy. Conclusions It was concluded that repeated doses of CD362-selected hUC-MSCs are required to modulate systemic and local immune/inflammatory events in polymicrobial sepsis and SA-AKI. Inter-individual variability and lack of effect of single dose MSC administration in the CLP model are consistent with observations to date from early-phase clinical trials.

Published

2021

47. T lymphocyte and monocyte subsets are dysregulated in type 1 diabetes patients with peripheral neuropathic pain

Author

Katie Wynne, Diana Shinko, Paul J. Austin, Barbara Fazekas de St Groth, Helen M. McGuire, Danielle M. Santarelli, Jayden A. O’Brien, Dominic Bailey, and Marc Russo

Subjects

Diabetic neuropathy, T cell, Neurosciences. Biological psychiatry. Neuropsychiatry, Chronic pain, Immunophenotyping, MK2, Downregulation and upregulation, Full Length Article, Medicine, Interleukin-7 receptor, CD27, General Environmental Science, FlowSOM, Type 1 diabetes, business.industry, MAPKAPK2, medicine.disease, medicine.anatomical_structure, Neuropathic pain, Immunology, General Earth and Planetary Sciences, Mass cytometry, SPADE, business, RC321-571

Abstract

Diabetic neuropathic pain is a common and devastating complication of type 1 diabetes, but the mechanism by which it develops and persists is yet to be fully elucidated. This study utilised high-dimensional suspension mass cytometry in a pilot cohort to investigate differences in peripheral blood immunophenotypes between type 1 diabetes patients with (n ​= ​9) and without (n ​= ​9) peripheral neuropathic pain. The abundance and activation of several leukocyte subsets were investigated with unsupervised clustering approaches FlowSOM and SPADE, as well as by manual gating. Major findings included a proportional increase in CD4+ central memory T cells and an absolute increase in classical monocytes, non-classical monocytes, and mature natural killer cells in type 1 diabetes patients with pain compared to those without pain. The expression of CD27, CD127, and CD39 was upregulated on select T cell populations, and the phosphorylated form of pro-inflammatory transcription factor MK2 was upregulated across most populations. These results provide evidence that distinct immunological signatures are associated with painful neuropathy in type 1 diabetes patients. Further research may link these changes to mechanisms by which pain in type 1 diabetes is initiated and maintained, paving the way for much needed targeted treatments.

Published

2021

48. Visualizing dendritic cell migration within the skin

Author

Roediger, Ben, Ng, Lai Guan, Smith, Adrian L., de St Groth, Barbara Fazekas, and Weninger, Wolfgang

Published

2008

49. Effects of storage time and temperature on highly multiparametric flow analysis of peripheral blood samples; implications for clinical trial samples

Author

Amelia Jerram, Lucinda Beutler, Helen M. McGuire, Barbara Fazekas de St Groth, Bavani Gunasegaran, Thomas V. Guy, and Ronald Sluyter

Subjects

Adult, Male, 0301 basic medicine, Immunology & Inflammation, Blood processing, Biophysics, Pilot Projects, Receptors, Cell Surface, CXCR3, Biochemistry, Peripheral blood mononuclear cell, Specimen Handling, Flow cytometry, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Immunophenotyping, immunophenotyping, TIGIT, medicine, Humans, Mass cytometry, Lymphocytes, Molecular Biology, Diagnostics & Biomarkers, Research Articles, medicine.diagnostic_test, Chemistry, Temperature, neutrophil, hemic and immune systems, Cell Biology, Flow Cytometry, cytometry, Molecular biology, 030104 developmental biology, 030220 oncology & carcinogenesis, Female, Translational Science, Cytometry, CD8

Abstract

We sought to determine the effect of time and temperature of blood sample storage before preparation of human peripheral blood mononuclear cells (PBMCs) by Ficoll-hypaque density gradient centrifugation. Blood samples from healthy donors were stored at room temperature (RT) or refrigerated at 4°C before preparation of PBMCs. Cell yield and viability, and proportions of major cell populations within PBMCs, as determined by fluorescence flow cytometry, were assessed for both fresh and cryopreserved samples. Highly multiparametric mass cytometry was performed on cryopreserved PBMCs. We found that refrigeration had marked negative effects on subsequent PBMC yield. Storage at RT led to co-purification of low density neutrophils with PBMCs, but had no detectable effects on the proportions of multiple cell subsets including, but not limited to, monocytes, NK cells, B cells, Treg cells, and naïve, central memory and effector memory CD4+ and CD8+ T cells and CD45RA-positive terminal effector CD8+ T cells. Expression of a number of cell surface receptors, including CXCR5, CCR6, CXCR3 and TIGIT, but not CD247 was reduced after RT storage before PBMC preparation, and this effect correlated with the degree of low density neutrophil contamination. As such, when PBMC preparation cannot be undertaken immediately after blood draw, storage at RT is far superior to refrigeration. RT storage leads to neutrophil activation, but does not compromise measurement of PBMC subset distribution. However caution must be applied to interpretation of cytometric measurements of surface molecules such as chemokine receptors.

Published

2021

50. Investigation of type I interferon responses in ANCA-associated vasculitis

Author

Joan Ní Gabhann-Dromgoole, Edward M Vital, Cathal Walsh, Nollaig M. Bourke, Emily Greenan, Mark A. Little, Barbara Fazekas, Suzanne D’Arcy, Isabella Batten, Jason Wyse, Mark W. Robinson, Arthur White, Antonia Buettner, Zoe Wigston, and Conor Murphy

Subjects

0301 basic medicine, Immunopathogenesis, Sialic Acid Binding Ig-like Lectin 1, viruses, Science, Immunology, Gene Expression, Inflammation, Anti-Neutrophil Cytoplasmic Antibody-Associated Vasculitis, Article, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Interferon, CXCL10, Medicine, Humans, STAT1, IRGs, Ubiquitins, Chemokine CCL2, 030203 arthritis & rheumatology, Autoimmune disease, Innate immunity, Multidisciplinary, Kidney diseases, biology, business.industry, medicine.disease, 3. Good health, Chemokine CXCL10, 030104 developmental biology, Gene Expression Regulation, Interferon Type I, biology.protein, Cytokines, medicine.symptom, business, Vasculitis, Negative Results, Biomarkers, medicine.drug

Abstract

Type I interferon (IFN) dysregulation is a major contributory factor in the development of several autoimmune diseases, termed type I interferonopathies, and is thought to be the pathogenic link with chronic inflammation in these conditions. Anti-neutrophil cytoplasmic antibody (ANCA)-Associated Vasculitis (AAV) is an autoimmune disease characterised by necrotising inflammation of small blood vessels. The underlying biology of AAV is not well understood, however several studies have noted abnormalities in type I IFN responses. We hypothesised that type I IFN responses are systemically dysregulated in AAV, consistent with features of a type I interferonopathy. To investigate this, we measured the expression of seven interferon regulated genes (IRGs) (ISG15, SIGLEC1, STAT1, RSAD2, IFI27, IFI44L and IFIT1) in peripheral blood samples, as well as three type I IFN regulated proteins (CXCL10, MCP-1 and CCL19) in serum samples from AAV patients, healthy controls and disease controls. We found no difference in type I IFN regulated gene or protein expression between AAV patients and healthy controls. Furthermore, IRG and IFN regulated protein expression did not correlate with clinical measurements of disease activity in AAV patients. Thus, we conclude that systemic type I IFN responses are not key drivers of AAV pathogenesis and AAV should not be considered a type I interferonopathy.

Published

2021