Your search keyword '"Venetia Bigley"' showing total 69 results

1. Serum Flt3 ligand is a biomarker of progenitor cell mass and prognosis in acute myeloid leukemia

Author

Paul Milne, Charlotte Wilhelm-Benartzi, Michael R. Grunwald, Venetia Bigley, Richard Dillon, Sylvie D. Freeman, Kathleen Gallagher, Amy Publicover, Sarah Pagan, Helen Marr, Gail L. Jones, Anne M. Dickinson, Angela Grech, Alan K. Burnett, Nigel H. Russell, Mark Levis, Steven Knapper, and Matthew Collin

Subjects

Specialties of internal medicine, RC581-951

Abstract

Abstract: Fms-like tyrosine kinase 3 (Flt3) is expressed on progenitor cells and acute myeloid leukemia (AML) blasts. Fms-like tyrosine kinase 3 ligand (Flt3L) is detectable during homeostasis and increases in hypoplasia due to genetic defects or treatment with cytoreductive agents. Conversely, Flt3+ AML is associated with depletion of Flt3L to undetectable levels. After induction chemotherapy, Flt3L is restored in patients entering complete remission (CR) but remains depressed in those with refractory disease. Weekly sampling reveals marked differences in the kinetics of Flt3L response during the first 6 weeks of treatment, proportionate to the clearance of blasts and cellularity of the bone marrow. In the UK NCRI AML17 trial, Flt3L was measured at day 26 in a subgroup of 140 patients with Flt3 mutation randomized to the tyrosine kinase inhibitor lestaurtinib or placebo. In these patients, attainment of CR was associated with higher Flt3L at day 26 (Mann-Whitney UP < .0001). Day 26 Flt3L was also associated with survival; Flt3L ≤291 pg/mL was associated with inferior event-free survival (EFS), and Flt3L >1185 pg/mL was associated with higher overall survival (OS; P = .0119). The separation of EFS and OS curves increased when minimal residual disease (MRD) status was combined with Flt3L measurement, and Flt3L retained a near-significant association with survival after adjusting for MRD in a proportional hazards model. Serial measurement of Flt3L in patients who had received a hematopoietic stem cell transplant for AML illustrates the potential value of monitoring Flt3L to identify relapse. Measurement of Flt3L is a noninvasive test with the potential to inform clinical decisions in patients with AML.

Published

2019

2. Subsets of CD1c+ DCs: Dendritic Cell Versus Monocyte Lineage

Author

Lukas Heger, Thomas P. Hofer, Venetia Bigley, I. Jolanda M. de Vries, Marc Dalod, Diana Dudziak, and Loems Ziegler-Heitbrock

Subjects

DC2, CD1c, CD172, CD301, CD14, dendritic cells, Immunologic diseases. Allergy, RC581-607

Abstract

Currently three bona fide dendritic cell (DC) types are distinguished in human blood. Herein we focus on type 2 DCs (DC2s) and compare the three defining markers CD1c, CD172, and CD301. When using CD1c to define DC2s, a CD14+ and a CD14− subset can be detected. The CD14+ subset shares features with monocytes, and this includes substantially higher expression levels for CD64, CD115, CD163, and S100A8/9. We review the current knowledge of these CD1c+CD14+ cells as compared to the CD1c+CD14− cells with respect to phenotype, function, transcriptomics, and ontogeny. Here, we discuss informative mutations, which suggest that two populations have different developmental requirements. In addition, we cover subsets of CD11c+CD8− DC2s in the mouse, where CLEC12A+ESAMlow cells, as compared to the CLEC12A−ESAMhigh subset, also express higher levels of monocyte-associated markers CD14, CD3, and CD115. Finally, we summarize, for both man and mouse, the data on lower antigen presentation and higher cytokine production in the monocyte-marker expressing DC2 subset, which demonstrate that the DC2 subsets are also functionally distinct.

Published

2020

3. Ikaros family zinc finger 1 regulates dendritic cell development and function in humans

Author

Urszula Cytlak, Anastasia Resteu, Delfien Bogaert, Hye Sun Kuehn, Thomas Altmann, Andrew Gennery, Graham Jackson, Attila Kumanovics, Karl V. Voelkerding, Seraina Prader, Melissa Dullaers, Janine Reichenbach, Harry Hill, Filomeen Haerynck, Sergio D. Rosenzweig, Matthew Collin, and Venetia Bigley

Subjects

Science

Abstract

IKZF1 is a transcription factor known to regulate mammalian B-cell development. Here the authors show that IKZF1 is required for human pDC development and regulation of DC cytokine production in patients with IKZF1 haploinsufficiency, findings which are recapitulated in lenalidomide-induced IKZF1 deficiency.

Published

2018

4. Dendritic cell, monocyte, B and NK lymphoid deficiency defines the lost lineages of a new GATA-2 dependent myelodysplastic syndrome

Author

Venetia Bigley and Matthew Collin

Subjects

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

Published

2011

5. Epigenetic regulator genes direct lineage switching in MLL/AF4 leukemia

Author

Paul Milne, Helen J. Blair, Cornelia Eckert, Zoya Kingsbury, Matthew Collin, Anetta Ptasinska, Alex Elder, Roderick Skinner, Janine Stutterheim, Jennifer Becq, Elena Zerkalenkova, Constanze Bonifer, Denis M. Schewe, Peter N. Cockerill, N Martinez-Soria, Oskar A. Haas, Peter Carey, Katarzyna Szoltysek, Deepali Pal, Hesta McNeill, Claus Meyer, Maria Rosaria Imperato, James C. Mulloy, Mark Wunderlich, Catherine Cargo, Paul Evans, Sarah E. Fordham, Shan Lin, Pierre Cauchy, Y Shi, Simon Bailey, Salam A. Assi, Rolf Marschalek, Josef Vormoor, Olaf Heidenreich, A Komkov, Michael J. Thirman, Simon Bomken, Ricky Tirtakusuma, Sirintra Nakjang, Fotini Vogiatzi, James M. Allan, Lisa J. Russell, Jayne Y. Hehir-Kwa, Muzlifah Haniffa, Yulia Olshanskaya, Vasily V. Grinev, Christine J. Harrison, Venetia Bigley, Daniel Williamson, Alex Smith, and Natalia Miakova

Subjects

Myeloid, Lineage (genetic), Oncogene Proteins, Fusion, Immunology, Gene regulatory network, Biology, Biochemistry, Epigenesis, Genetic, hemic and lymphatic diseases, Genes, Regulator, medicine, Humans, Epigenetics, Alternative splicing, C100, Cell Biology, Hematology, Precursor Cell Lymphoblastic Leukemia-Lymphoma, A300, Chromatin, medicine.anatomical_structure, Cancer research, Oncogene Fusion, Reprogramming, Myeloid-Lymphoid Leukemia Protein

Abstract

The fusion gene MLL-AF4 defines a high-risk subtype of pro-B acute lymphoblastic leukaemia. However, relapse can be associated with a switch from acute lymphoblastic to acute myeloid leukaemia. Here we show that these myeloid relapses share oncogene fusion breakpoints with their matched lymphoid presentations and can originate in either early, multipotent progenitors or committed B-cell precursors. Lineage switching is linked to substantial changes in chromatin accessibility and rewiring of transcriptional programmes indicating that the execution and maintenance of lymphoid lineage differentiation is impaired. We show that this subversion is recurrently associated with the dysregulation of repressive chromatin modifiers, notably the nucleosome remodelling and deacetylation complex, NuRD. In addition to mutations, we show differential expression or alternative splicing of NuRD members and other genes is able to reprogram the B lymphoid into a myeloid gene regulatory network. Lineage switching in MLL-AF4 leukaemia is therefore driven and maintained by defunct epigenetic regulation.Statement of SignificanceWe demonstrate diverse cellular origins of lineage switched relapse within MLL-AF4 pro-B acute leukaemia. Irrespective of the developmental origin of relapse, dysregulation of NuRD and/or other epigenetic machinery underpins fundamental lineage reprogramming with profound implications for the increasing use of epitope directed therapies in this high-risk leukaemia.

Published

2022

6. Hematopoietic stem cell transplantation for adolescents and adults with inborn errors of immunity: an EBMT IEWP study

Author

Michael H. Albert, Tiarlan Sirait, Dirk-Jan Eikema, Katerina Bakunina, Claudia Wehr, Felipe Suarez, Maria Laura Fox, Nizar Mahlaoui, Andrew R. Gennery, Arjan C. Lankester, Rita Beier, Maria Ester Bernardo, Venetia Bigley, Caroline A. Lindemans, Siobhan O. Burns, Ben Carpenter, Jaroslaw Dybko, Tayfun Güngör, Fabian Hauck, Su Han Lum, Dmitry Balashov, Roland Meisel, Despina Moshous, Ansgar Schulz, Carsten Speckmann, Mary A. Slatter, Brigitte Strahm, Duygu Uckan-Cetinkaya, Isabelle Meyts, Tanja C. Vallée, Robert Wynn, Bénédicte Neven, Emma C. Morris, Alessandro Aiuti, Alexei Maschan, Mahmoud Aljurf, Tobias Gedde-Dahl, Gunhan Gurman, Victoria Bordon, Gergely Kriván, Franco Locatelli, Fulvio Porta, David Valcárcel, Yves Beguin, Maura Faraci, Nicolaus Kröger, Aleksandr Kulagin, Peter J. Shaw, Joan Hendrik Veelken, Cristina Diaz de Heredia, Franca Fagioli, Matthias Felber, Bernd Gruhn, Wolfgang Holter, Claudia Rössig, Petr Sedlacek, Jane Apperley, Mouhab Ayas, Ivana Bodova, Goda Choi, J.J. Cornelissen, Anne Sirvent, Anjum Khan, Alphan Kupesiz, Stig Lenhoff, Hakan Ozdogu, Nicolas von der Weid, Montserrat Rovira, Rik Schots, Donald C. Vinh, Clinical sciences, and Hematology

Subjects

Adult, Adolescent, adolescenti, Trapianto, Immunology, Graft vs Host Disease, Biochemistry, Bronchiectasis/etiology, Humans, Transplantation, Homologous, Hematopoietic Stem Cell Transplantation/adverse effects, Child, Retrospective Studies, cellule staminali ematopoietiche, Hematopoietic Stem Cell Transplantation, Infant, Trapianto, cellule staminali ematopoietiche, adolescenti, Inborn errors of immunity, Cell Biology, Hematology, Middle Aged, Bronchiectasis, surgical procedures, operative, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, HSCT, young adult

Abstract

Allogeneic hematopoietic stem cell transplantation (HSCT) is the gold standard curative therapy for infants and children with many inborn errors of immunity (IEI), but adolescents and adults with IEI are rarely referred for transplant. Lack of published HSCT outcome data outside small, single-center studies and perceived high risk of transplant-related mortality have delayed the adoption of HSCT for IEI patients presenting or developing significant organ damage later in life. This large retrospective, multicenter HSCT outcome study reports on 329 IEI patients (age range, 15-62.5 years at HSCT). Patients underwent first HSCT between 2000 and 2019. Primary endpoints were overall survival (OS) and event-free survival (EFS). We also evaluated the influence of IEI-subgroup and IEI-specific risk factors at HSCT, including infections, bronchiectasis, colitis, malignancy, inflammatory lung disease, splenectomy, hepatic dysfunction, and systemic immunosuppression. At a median follow-up of 44.3 months, the estimated OS at 1 and 5 years post-HSCT for all patients was 78% and 71%, and EFS was 65% and 62%, respectively, with low rates of severe acute (8%) or extensive chronic (7%) graft-versus-host disease. On univariate analysis, OS and EFS were inferior in patients with primary antibody deficiency, bronchiectasis, prior splenectomy, hepatic comorbidity, and higher hematopoietic cell transplant comorbidity index scores. On multivariable analysis, EFS was inferior in those with a higher number of IEI-associated complications. Neither age nor donor had a significant effect on OS or EFS. We have identified age-independent risk factors for adverse outcome, providing much needed evidence to identify which patients are most likely to benefit from HSCT. ispartof: BLOOD vol:140 issue:14 pages:1635-1649 ispartof: location:United States status: published

Published

2022

7. Host versus graft HLA-DP1 mismatching promotes graft versus host disease

Author

Callum Wright, Ginette Reid, Beverley Clare Lendrem, Erin Hurst, Amy Publicover, Rachel Luke, Louise Duncan, Venetia Bigley, and Matthew Collin

Subjects

Transplantation, Hematology

Published

2023

8. Modeling the Effects of IL-1β-mediated Inflammation During Ex Vivo Lung Perfusion Using a Split Human Donor Model

Author

Thomas Pither, Lu Wang, Lucy Bates, Morvern Morrison, Catriona Charlton, Chelsea Griffiths, Jamie Macdonald, Venetia Bigley, Maria Mavridou, Joseph Barsby, Lee Borthwick, John Dark, William Scott, Simi Ali, and Andrew J. Fisher

Subjects

Transplantation

Published

2023

9. PAMI Syndrome: Two Cases of an Autoinflammatory Disease with an ALPS-Like Phenotype

Author

Fionnuala Cox, Venetia Bigley, Alan Irvine, Ronan Leahy, and Niall Conlon

Subjects

Immunology, Immunology and Allergy

Published

2022

10. GATA2 deficiency phenotype associated with tandem duplication of GATA2 and overexpression of GATA2-AS1

Author

Benedicte Neven, Preeti Singh, Rachel E. Dickinson, Mojgan Reza, Aneta Mikulasova, Laetitia Largeaud, Venetia Bigley, Anastasia Resteu, Eric Delabesse, Jacinta Bustamante, Matthew Collin, Maninder Heer, Daniel Rico, Marlène Pasquet, Stephanie Dufrechou, and Naïs Prade

Subjects

GATA2 Deficiency, DNA Copy Number Variations, Hematology, Biology, Molecular biology, Monocytes, Frameshift mutation, GATA2 Transcription Factor, Phenotype, Transcription (biology), Chimeric RNA, Child, Preschool, Gene duplication, Humans, Exceptional Case Report, Female, Tandem exon duplication, Copy-number variation, Allele, Alleles

Abstract

Key Points Typical features of GATA2 deficiency were associated with a de novo tandem duplication of GATA2 and increased expression of GATA2-AS1.The duplication contained a maternally inherited deletion copy number polymorphism esv2725896/nsv513733., A 3-year-old girl of nonconsanguineous healthy parents presented with cervical and mediastinal lymphadenopathy due to Mycobacterium fortuitum infection. Routine blood analysis showed normal hemoglobin, neutrophils, and platelets but profound mononuclear cell deficiency (monocytes < 0.1 × 109/L; B cells 78/μL; NK cells 48/μL). A 548 902-bp region containing GATA2 was sequenced by targeted capture and deep sequencing. This revealed a de novo 187-kb duplication of the entire GATA2 locus, containing a maternally inherited copy number variation deletion of 25 kb (GRCh37: esv2725896 and nsv513733). Many GATA2-associated phenotypes have been attributed to amino acid substitution, frameshift/deletion, loss of intronic enhancer function, or aberrant splicing. Gene deletion has been described, but other structural variation has not been reported in the germline configuration. In this case, duplication of the GATA2 locus was paradoxically associated with skewed diminished expression of GATA2 messenger RNA and loss of GATA2 protein. Chimeric RNA fusion transcripts were not detected. A possible mechanism involves increased transcription of the anti-sense long noncoding RNA GATA2-AS1 (RP11-472.220), which was increased several fold. This case further highlights that evaluation of the allele count is essential in any case of suspected GATA2-related syndrome.

Published

2021

11. Guidelines for mouse and human DC generation

Author

Manfred B. Lutz, Shafaqat Ali, Cindy Audiger, Stella E. Autenrieth, Luciana Berod, Venetia Bigley, Laura Cyran, Marc Dalod, Jan Dörrie, Diana Dudziak, Georgina Flórez‐Grau, Lucila Giusiano, Gloria J. Godoy, Marion Heuer, Anne B. Krug, Christian H. K. Lehmann, Christian T. Mayer, Shalin H. Naik, Stefanie Scheu, Gerty Schreibelt, Elodie Segura, Kristin Seré, Tim Sparwasser, Jurjen Tel, Huaming Xu, Martin Zenke, University of Würzburg, Institute of Medical Microbiology and Hospital Hygiene (University of Düsseldorf), Heinrich Heine Universität Düsseldorf = Heinrich Heine University [Düsseldorf], The Walter and Eliza Hall Institute of Medical Research (WEHI), University of Melbourne, German Cancer Research Center - Deutsches Krebsforschungszentrum [Heidelberg] (DKFZ), University of Tübingen, University Medical Center of the Johannes Gutenberg-University Mainz, Newcastle University [Newcastle], Centre d'Immunologie de Marseille - Luminy (CIML), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Universitätsklinikum Erlangen [Erlangen], Friedrich-Alexander Universität Erlangen-Nürnberg (FAU), University Hospital Erlangen = Uniklinikum Erlangen, Radboud Institute for Molecular Life Sciences [Nijmegen, the Netherlands], Ludwig Maximilian University [Munich] (LMU), Universität Duisburg-Essen = University of Duisburg-Essen [Essen], Immunité et cancer (U932), Institut Curie [Paris]-Institut National de la Santé et de la Recherche Médicale (INSERM), Université Paris sciences et lettres (PSL), Universitätsklinikum RWTH Aachen - University Hospital Aachen [Aachen, Germany] (UKA), Rheinisch-Westfälische Technische Hochschule Aachen University (RWTH), Eindhoven University of Technology [Eindhoven] (TU/e), University of Duisburg-Essen, and Dalod, Marc

Subjects

In vitro, Immunology, Generation, Immunology and Allergy, endritic cells, [SDV.IMM.II] Life Sciences [q-bio]/Immunology/Innate immunity, [SDV.IMM.II]Life Sciences [q-bio]/Immunology/Innate immunity, Isolation

Abstract

European journal of immunology (2022). doi:10.1002/eji.202249816, Published by Wiley-VCH, Weinheim

Published

2022

12. Allogeneic haematopoietic stem cell transplantation for VEXAS syndrome: UK experience

Author

Adam Al‐Hakim, James A. Poulter, Dina Mahmoud, Ailsa M. S. Rose, Suzanne Elcombe, Helen Lachmann, Catherine Cargo, Christopher J. A. Duncan, Mark Bishton, Venetia Bigley, Anjum Khan, and Sinisa Savic

Subjects

Transplantation Conditioning, Hematopoietic Stem Cell Transplantation, Humans, Transplantation, Homologous, Hematology, United Kingdom

Published

2022

13. Lineage-switching of the cellular distribution of BRAFV600E in multisystem Langerhans cell histiocytosis

Author

Paul Milne, Simon Bomken, Olga Slater, Ashish Kumar, Adam Nelson, Somak Roy, Jessica Velazquez, Kshitij Mankad, James Nicholson, Dan Yeomanson, Richard Grundy, Ahmed Kamal, Anthony Penn, Jane Pears, Gerard Millen, Bruce Morland, James Hayden, Jason Lam, Maymoon Madkhali, Jamie MacDonald, Preeti Singh, Sarah Pagan, Carlos Rodriguez-Galindo, Milen Minkov, Jean Donadieu, Jennifer Picarsic, Carl Allen, Venetia Bigley, and Matthew Collin

Subjects

Hematology

Abstract

Most children with high-risk Langerhans cell histiocytosis (LCH) have BRAFV600E mutation. BRAFV600E alleles are detectable in myeloid mononuclear cells at diagnosis but it is not known if the cellular distribution of mutation evolves over time. Here, the profiles of 16 patients with high-risk disease were analyzed. Two received conventional salvage chemotherapy, 4 patients on inhibitors were tracked at intervals of 3 to 6 years, and 10 patients, also given inhibitors, were analyzed more than 2 years after diagnosis. In contrast to the patients responding to salvage chemotherapy who completely cleared BRAFV600E within 6 months, children who received inhibitors maintained high BRAFV600E alleles in their blood. At diagnosis, mutation was detected predominantly in monocytes and myeloid dendritic cells. With time, mutation switched to the T-cell compartment, which accounted for most of the mutational burden in peripheral blood mononuclear cells, more than 2 years from diagnosis (median, 85.4%; range, 44.5%-100%). The highest level of mutation occurred in naïve CD4+ T cells (median, 51.2%; range, 3.8%-93.5%). This study reveals an unexpected lineage switch of BRAFV600E mutation in high-risk LCH, which may influence monitoring strategies for the potential withdrawal of inhibitor treatment and has new implications for the pathogenesis of neurodegeneration, which occurred in 4 patients.

Published

2022

14. Author response for 'Guidelines for mouse and human DC generation'

Author

null Manfred B. Lutz, null Shafaqat Ali, null Cindy Audiger, null Stella E. Autenrieth, null Luciana Berod, null Venetia Bigley, null Laura Cyran, null Marc Dalod, null Jan Dörrie, null Diana Dudziak, null Georgina Flórez‐Grau, null Lucila Giusiano, null Gloria J. Godoy, null Marion Heuer, null Anne B. Krug, null Christian H. K. Lehmann, null Christian T. Mayer, null Shalin H. Naik, null Stefanie Scheu, null Gerty Schreibelt, null Elodie Segura, null Kristin Seré, null Tim Sparwasser, null Jurjen Tel, null Huaming Xu, and null Martin Zenke

Published

2022

15. Many Langerhans make light work of skin immunity

Author

Venetia Bigley and Matthew Collin

Subjects

Immunology, Functional specialization, biochemical phenomena, metabolism, and nutrition, Biology, Infectious Diseases, Immune system, Immunity, Langerhans Cells, Humans, Immunology and Allergy, Skin immunity, Epidermis, Neuroscience, Light Work, Skin

Abstract

The concept of functional specialization is fundamental to the immune system but has not been previously observed in human Langerhans cells. In this issue of Immunity, Liu et al. use single-cell approaches to define two distinct epidermal subsets converging on a common activation and migration pathway.

Published

2021

16. A Novel Case of Homozygous Interferon Alpha/Beta Receptor Alpha Chain (IFNAR1) Deficiency With Hemophagocytic Lymphohistiocytosis

Author

Zofia Klimova, Linh Truong, Martina Fejtkova, Venetia Bigley, Dusana Moravcikova, Catherine F Hatton, Dipayan Mitra, Angela Grainger, Florian Gothe, Veronika Kanderova, Sophie Hambleton, Ales Janda, Joanna E. Perthen, Christopher J A Duncan, and Eva Fronkova

Subjects

0301 basic medicine, Microbiology (medical), Alpha interferon, Antiviral Agents, 03 medical and health sciences, 0302 clinical medicine, inborn error of immunity, Immunity, Interferon, medicine, Humans, IFNAR1, Inflammation, business.industry, Brief Report, Phenotype, Immunity, Innate, Vaccination, 030104 developmental biology, Infectious Diseases, AcademicSubjects/MED00290, Immunology, Interferon Type I, type I interferon, business, 030217 neurology & neurosurgery, Alpha chain, medicine.drug, HLH

Abstract

We present a case of complete deficiency of the interferon alpha/beta receptor alpha chain (IFNAR1) in a child with fatal systemic hyperinflammation, apparently provoked by live-attenuated viral vaccination. Such pathologic hyperinflammation, fulfilling criteria for hemophagocytic lymphohistiocytosis, is an emerging phenotype accompanying inborn errors of type I interferon immunity.

Published

2020

17. Human dendritic cell immunodeficiencies

Author

Matthew Collin, Venetia Bigley, and Urszula Cytlak

Subjects

0301 basic medicine, Autoimmunity, Biology, medicine.disease_cause, Dendritic cells, IRF8, 03 medical and health sciences, 0302 clinical medicine, Immunity, GATA2, Immune Tolerance, medicine, Humans, Mutation, Primary immunodeficiency, Manchester Cancer Research Centre, ResearchInstitutes_Networks_Beacons/mcrc, Dendritic Cells, Syndrome, Cell Biology, Dendritic cell, IKZF1, medicine.disease, Phenotype, 030104 developmental biology, Immunology, 030217 neurology & neurosurgery, Developmental Biology

Abstract

The critical functions of dendritic cells (DCs) in immunity and tolerance have been demonstrated in many animal models but their non-redundant roles in humans are more difficult to probe. Human primary immunodeficiency (PID), resulting from single gene mutations, may result in DC deficiency or dysfunction. This relatively recent recognition illuminates the in vivo role of human DCs and the pathophysiology of the associated clinical syndromes. In this review, the development and function of DCs as established in murine models and human in vitro systems, discussed. This forms the basis of predicting the effects of DC deficiency in vivo and understanding the consequences of specific mutations on DC development and function. DC deficiency syndromes are associated with heterozygous GATA2 mutation, bi-allelic and heterozygous IRF8 mutation and heterozygous IKZF1 mutation. The intricate involvement of DCs in the balance between immunity and tolerance is leading to increased recognition of their involvement in a number of other immunodeficiencies and autoimmune conditions. Owing to the precise control of transcription factor gene expression by super-enhancer elements, phenotypic anomalies are relatively commonly caused by heterozygous mutations.

Published

2019

18. Differential IRF8 Transcription Factor Requirement Defines Two Pathways of Dendritic Cell Development in Humans

Author

Rachel Queen, Venetia Bigley, Gina M. Doody, Sarah Pagan, Sheetal Maisuria, James Thaventhiran, Kile Green, Rosie Hague, Andrew Filby, Gillian Hulme, Benjamin C. Carpenter, David McDonald, Hana Lango Allen, Paul Milne, Urszula Cytlak, Matthew Collin, Anastasia Resteu, Sophie Hambleton, Lango Allen, Hana [0000-0002-7803-8688], Thaventhiran, James [0000-0001-8616-074X], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Myeloid, dendritic cell, Immunology, Interleukin-3 Receptor alpha Subunit, Lipopolysaccharide Receptors, BTLA, Antigens, CD34, Biology, CD8-Positive T-Lymphocytes, primary immunodeficiency, Article, single-cell RNA sequencing, Cell Line, IRF8, Antigens, CD1, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Immunology and Allergy, Compartment (development), Animals, Humans, Cell Lineage, Receptors, Immunologic, Transcription factor, transcription factor, Progenitor, Glycoproteins, Manchester Cancer Research Centre, ResearchInstitutes_Networks_Beacons/mcrc, Dendritic cell, Dendritic Cells, Hematopoietic Stem Cells, immunity, hematopoiesis, Cell biology, Haematopoiesis, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Interferon Regulatory Factors, CyTOF

Abstract

Summary The formation of mammalian dendritic cells (DCs) is controlled by multiple hematopoietic transcription factors, including IRF8. Loss of IRF8 exerts a differential effect on DC subsets, including plasmacytoid DCs (pDCs) and the classical DC lineages cDC1 and cDC2. In humans, cDC2-related subsets have been described including AXL+SIGLEC6+ pre-DC, DC2 and DC3. The origin of this heterogeneity is unknown. Using high-dimensional analysis, in vitro differentiation, and an allelic series of human IRF8 deficiency, we demonstrated that cDC2 (CD1c+DC) heterogeneity originates from two distinct pathways of development. The lymphoid-primed IRF8hi pathway, marked by CD123 and BTLA, carried pDC, cDC1, and DC2 trajectories, while the common myeloid IRF8lo pathway, expressing SIRPA, formed DC3s and monocytes. We traced distinct trajectories through the granulocyte-macrophage progenitor (GMP) compartment showing that AXL+SIGLEC6+ pre-DCs mapped exclusively to the DC2 pathway. In keeping with their lower requirement for IRF8, DC3s expand to replace DC2s in human partial IRF8 deficiency., Graphical Abstract, Highlights • Distinct development trajectories of DC2 and DC3 underpin human cDC2 heterogeneity • pDC, cDC1, and DC2 (classical DCs) develop from LMPPs along a CD123+ IRF8high pathway • DC3 and monocytes develop from CD33+ GMPs along an IRF8low SIRPA+ pathway • IRF8 deficiency causes gene dose-dependent loss of IRF8high then IRF8low pathway DCs, Heterogeneity of human CD1c+ dendritic cells (cDC2s) is described, but how this arises is unknown. Cytlak and colleagues demonstrate that the cDC2 subsets, DC2 and DC3, develop along distinct hematopoietic trajectories, defined by differential IRF8 expression. DC2s develop from LMPPs along an IRF8hi pathway, while DC3 differentiation follows an IRF8low trajectory.

Published

2020

19. Donor monocyte–derived macrophages promote human acute graft-versus-host disease

Author

A. J. Simpson, Gary Reynolds, Xiao-Nong Wang, Sarah Pagan, Laura Jardine, Graham H. Jackson, Urszula Cytlak, Smeera Nair, Merry Gunawan, Matthew Collin, Anna Long, Kile Green, Erin Hurst, Amy Publicover, Christopher A. Lamb, Muzlifah Haniffa, Venetia Bigley, and Maharani Paramitha

Subjects

0301 basic medicine, Bone marrow transplantation, CD14, Immunology, Antigen presentation, CD11c, Biology, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Antigen, medicine, Macrophage, Transplantation, Manchester Cancer Research Centre, Macrophages, Monocyte, ResearchInstitutes_Networks_Beacons/mcrc, Stem cell transplantation, General Medicine, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Myelopoiesis, Research Article

Abstract

Myelopoiesis is invariably present and contributes to pathology in animal models of graft-versus-host disease (GVHD). In humans, a rich inflammatory infiltrate bearing macrophage markers has also been described in histological studies. In order to determine the origin, functional properties, and role in pathogenesis of these cells, we isolated single-cell suspensions from acute cutaneous GVHD and subjected them to genotype, transcriptome, and in vitro functional analysis. A donor-derived population of CD11c+CD14+ cells was the dominant population of all leukocytes in GVHD. Surface phenotype and NanoString gene expression profiling indicated the closest steady-state counterpart of these cells to be monocyte-derived macrophages. In GVHD, however, there was upregulation of monocyte antigens SIRPα and S100A8/9 transcripts associated with leukocyte trafficking, pattern recognition, antigen presentation, and costimulation. Isolated GVHD macrophages stimulated greater proliferation and activation of allogeneic T cells and secreted higher levels of inflammatory cytokines than their steady-state counterparts. In HLA-matched mixed leukocyte reactions, we also observed differentiation of activated macrophages with a similar phenotype. These exhibited cytopathicity to a keratinocyte cell line and mediated pathological damage to skin explants independently of T cells. Together, these results define the origin, functional properties, and potential pathogenic roles of human GVHD macrophages.

Published

2020

20. Subsets of CD1c

Author

Lukas, Heger, Thomas P, Hofer, Venetia, Bigley, I Jolanda M, de Vries, Marc, Dalod, Diana, Dudziak, and Loems, Ziegler-Heitbrock

Subjects

Immunity, Cellular, DC subsets, Immunology, Asialoglycoproteins, Membrane Proteins, Cell Differentiation, Dendritic Cells, Review, Antigens, Differentiation, CD1c, Monocytes, DC2, Antigens, CD1, Mice, CD301, Animals, Cytokines, Humans, Cell Lineage, Lectins, C-Type, dendritic cells, Receptors, Immunologic, CD14, Glycoproteins, CD172

Abstract

Currently three bona fide dendritic cell (DC) types are distinguished in human blood. Herein we focus on type 2 DCs (DC2s) and compare the three defining markers CD1c, CD172, and CD301. When using CD1c to define DC2s, a CD14+ and a CD14− subset can be detected. The CD14+ subset shares features with monocytes, and this includes substantially higher expression levels for CD64, CD115, CD163, and S100A8/9. We review the current knowledge of these CD1c+CD14+ cells as compared to the CD1c+CD14− cells with respect to phenotype, function, transcriptomics, and ontogeny. Here, we discuss informative mutations, which suggest that two populations have different developmental requirements. In addition, we cover subsets of CD11c+CD8− DC2s in the mouse, where CLEC12A+ESAMlow cells, as compared to the CLEC12A−ESAMhigh subset, also express higher levels of monocyte-associated markers CD14, CD3, and CD115. Finally, we summarize, for both man and mouse, the data on lower antigen presentation and higher cytokine production in the monocyte-marker expressing DC2 subset, which demonstrate that the DC2 subsets are also functionally distinct.

Published

2020

21. Insights from Patients with Dendritic Cell Immunodeficiency

Author

Matthew Collin and Venetia Bigley

Subjects

0301 basic medicine, Genetically modified mouse, medicine.medical_treatment, Immunology, GATA2, Immunotherapy, Dendritic cell, Biology, medicine.disease, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, 0302 clinical medicine, Immune system, medicine, Stem cell, Molecular Biology, Neuroscience, Immunodeficiency, 030215 immunology

Abstract

Dendritic Cells (DCs), derived from haematopoietic stem cells, are critical to the dynamic and balanced functioning of the intact immune system and are of great interest as vehicles of immunotherapy. Genetically modified mouse models have proved powerful tools to map DC development and function in vivo but human studies have previously relied heavily on in vitro systems. Human dendritic cell immunodeficiency, resulting from single gene mutations, offers new opportunities to dissect the role of human DCs in vivo, determine the genetic requirements for their development and map their haematopoietic differentiation pathways. This review will summarise the clinical phenotypes of mutations in GATA2, IRF8 and IKZF1 genes which result in global or subset specific dendritic cell deficiencies, discuss the functional consequences of these cytopenias and how these syndromes have informed our knowledge of DC differentiation and human haematopoiesis.

Published

2020

22. Subsets of CD1c+DCs: Dendritic cell versus monocyte lineage

Author

Lukas Heger, Thomas P. Hofer, Venetia Bigley, I. Jolanda M. de Vries, Marc Dalod, Diana Dudziak, Loems Ziegler-Heitbrock, DUMENIL, Anita, Department of Dermatology, University of Erlangen, Friedrich-Alexander Universität Erlangen-Nürnberg (FAU), Helmholtz Centre Munich, Newcastle University [Newcastle], Radboud Institute for Molecular Life Sciences [Nijmegen, the Netherlands], Centre d'Immunologie de Marseille - Luminy (CIML), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Deutsches Zentrum Immuntherapie [Erlangen] (DZI), Monocytomics Research, and Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Aix Marseille Université (AMU)

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, DC subsets, CD14, CD3, [SDV]Life Sciences [q-bio], Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Immunology, Antigen presentation, CD11c, CD1c, DC2, 03 medical and health sciences, 0302 clinical medicine, Medizinische Fakultät, medicine, Immunology and Allergy, ddc:610, dendritic cells, Dc2, Cd1c, Cd172, Cd301, Cd14, Dendritic Cells, Dc Subsets, CD172, biology, Monocyte, Dendritic cell, Phenotype, Cell biology, [SDV] Life Sciences [q-bio], 030104 developmental biology, medicine.anatomical_structure, CD301, biology.protein, lcsh:RC581-607, CD8, 030215 immunology

Abstract

Contains fulltext : 229325.pdf (Publisher’s version ) (Open Access) Currently three bona fide dendritic cell (DC) types are distinguished in human blood. Herein we focus on type 2 DCs (DC2s) and compare the three defining markers CD1c, CD172, and CD301. When using CD1c to define DC2s, a CD14(+) and a CD14(-) subset can be detected. The CD14(+) subset shares features with monocytes, and this includes substantially higher expression levels for CD64, CD115, CD163, and S100A8/9. We review the current knowledge of these CD1c(+)CD14(+) cells as compared to the CD1c(+)CD14(-) cells with respect to phenotype, function, transcriptomics, and ontogeny. Here, we discuss informative mutations, which suggest that two populations have different developmental requirements. In addition, we cover subsets of CD11c(+)CD8(-) DC2s in the mouse, where CLEC12A(+)ESAM(low) cells, as compared to the CLEC12A(-)ESAM(high) subset, also express higher levels of monocyte-associated markers CD14, CD3, and CD115. Finally, we summarize, for both man and mouse, the data on lower antigen presentation and higher cytokine production in the monocyte-marker expressing DC2 subset, which demonstrate that the DC2 subsets are also functionally distinct.

Published

2020

23. In vivo T-depleted reduced-intensity transplantation for GATA2-related immune dysfunction

Author

Rachel E. Dickinson, Venetia Bigley, Andrew R. Gennery, Mary Slatter, Graham Jackson, Andrew J. Cant, Matthew Collin, Sophie Hambleton, Katherine Sturgess, James Lordan, and Eleni Tholouli

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, GATA2 Deficiency, medicine.medical_treatment, Immunology, Hematopoietic stem cell transplantation, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Text mining, Germline mutation, In vivo, Internal medicine, medicine, Humans, Letter to Blood, Ponds, business.industry, GATA2, Hematopoietic Stem Cell Transplantation, Reduced intensity, Retrospective cohort study, Cell Biology, Hematology, GATA2 Transcription Factor, Clinical trial, 030104 developmental biology, Immune System Diseases, business, 030215 immunology

Abstract

Publisher's Note: There is a Blood Commentary on this article in this issue.

Published

2018

24. Early Molecular Stratification of High-risk Primary Biliary Cholangitis

Author

Sarah Pagan, L. Jopson, Claire Hardie, Dina Tiniakos, Muzlifah Haniffa, John G. Brain, Jessica K Dyson, Kile Green, Lucy J. Walker, Barbara A. Innes, Venetia Bigley, Ben Millar, and David Jones

Subjects

0301 basic medicine, Senescence, Oncology, Adult, Cyclin-Dependent Kinase Inhibitor p21, Male, Leukocyte migration, medicine.medical_specialty, Pathology, Cholangitis, medicine.medical_treatment, Biopsy, Disease, Liver transplantation, PBC, General Biochemistry, Genetics and Molecular Biology, UDCA, Gene product, 03 medical and health sciences, Internal medicine, medicine, Humans, Gene Regulatory Networks, RNA, Messenger, NanoString® nCounter PanCancer Immunity Panel, Aged, medicine.diagnostic_test, business.industry, Gene Expression Profiling, General Medicine, Middle Aged, Prognosis, Ursodeoxycholic acid, 3. Good health, Gene expression profiling, 030104 developmental biology, Gene Expression Regulation, Disease Progression, Female, Stratification, business, Transcriptome, Biomarkers, medicine.drug, Research Paper

Abstract

High-risk primary biliary cholangitis (PBC), defined by inadequate response at one year to Ursodeoxycholic acid (UDCA), is associated with disease progression and liver transplantation. Stratifying high-risk patients early would facilitate improved approaches to care. Using long-term follow-up data to define risk at presentation, 6 high-risk PBC patients and 8 low-risk patients were identified from biopsy, transplant and biochemical archival records. Formalin-fixed paraffin-embedded (FFPE) liver biopsies taken at presentation were graded (Scheuer and Nakanuma scoring) and gene expression analysed using the NanoString® nCounter PanCancer Immunity 770-gene panel. Principle component analysis (PCA) demonstrated discrete gene expression clustering between controls and high- and low-risk PBC. High-risk PBC was characterised by up-regulation of genes linked to T-cell activation and apoptosis, INF-γ signalling and leukocyte migration and down-regulation of those linked to the complement pathway. CDKN1a, up-regulated in high-risk PBC, correlated with significantly increased expression of its gene product, the senescence marker p21WAF1/Cip, by biliary epithelial cells. Our findings suggest high- and low-risk PBC are biologically different from disease outset and senescence an early feature in high-risk disease. Identification of a high-risk ‘signal’ early from standard FFPE tissue sections has clear clinical utility allowing for patient stratification and second-line therapeutic intervention., Highlights • 30% of PBC patients have high-risk disease defined after a year of non-response to ursodeoxycholic acid therapy. • Gene-expression profiles from FFPE archival index liver biopsies demonstrate distinct clustering of high- and low-risk PBC. • High-risk genes are linked to T-cell activation, apoptosis, migration; IFN-γ signalling; and biliary senescence. • The risk ‘signal’, detectable from FFPE liver biopsy samples, has potential utility as a clinical diagnostic tool. PBC is a chronic disease causing injury to bile ducts within the liver. 70% of patients have low-risk PBC and respond to treatment. The remaining 30% have un-responsive, high-risk disease that can progress to cirrhosis, liver-failure and the need for liver transplantation. Currently high-risk disease is only determined after a year of treatment failure. This study demonstrates that genes expressed in liver biopsies taken at diagnosis from patients with PBC allow high-risk disease to be identified earlier and this could be developed as a diagnostic tool. In addition, these data will guide further research and development of new treatments.

Published

2016

25. Donor monocyte-derived macrophages promote human acute graft versus host disease

Author

Smeera Nair, Muzlifah Haniffa, Gary Reynolds, Xiao-Nong Wang, Merry Gunawan, Graham H. Jackson, Matthew Collin, A. J. Simpson, Amy Publicover, Kile Green, Venetia Bigley, Sarah Pagan, Urszula Cytlak, Laura Jardine, M. Pradnya, Christopher A. Lamb, Erin Hurst, and Anna Long

Subjects

0303 health sciences, CD14, Monocyte, Antigen presentation, CD11c, Biology, medicine.disease, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, Graft-versus-host disease, medicine.anatomical_structure, Antigen, Immunology, medicine, Macrophage, Myelopoiesis, 030304 developmental biology, 030215 immunology

Abstract

Myelopoiesis is invariably present, and contributes to pathology, in animal models of graft versus host disease (GVHD). In humans, a rich inflammatory infiltrate bearing macrophage markers has also been described in histological studies. In order to determine the origin, functional properties and role in pathogenesis of these cells, we isolated single cell suspensions from acute cutaneous GVHD and subjected them to genotype, transcriptome and in vitro functional analysis. A donor-derived population of CD11c+CD14+ cells was the dominant population of all leukocytes in GVHD. Surface phenotype and nanostring gene expression profiling indicated the closest steady-state counterpart of these cells to be monocyte-derived macrophages. In GVHD, however, there was upregulation of monocyte antigens SIRPα and S100A8/9, and transcripts associated with leukocyte trafficking, pattern recognition, antigen presentation, and co-stimulation. Isolated GVHD macrophages stimulated greater proliferation and activation of allogeneic T cells, and secreted higher levels of inflammatory cytokines than their steady-state counterparts. In HLA-matched mixed leukocyte reactions, we also observed differentiation of activated macrophages with a similar phenotype. These exhibited cytopathicity to a cell line and mediated pathological damage to skin explants, independently of T cells. Together, these results define the origin, functional properties and potential pathogenic roles of human GVHD macrophages.

Published

2019

26. Serum Flt3 ligand is biomarker of progenitor cell mass and prognosis in acute myeloid leukemia

Author

Amy Publicover, Paul Milne, Sarah Pagan, Angela Grech, Anne M. Dickinson, Michael R. Grunwald, Gail Jones, Helen Marr, Steven Knapper, Mark Levis, Charlotte Wilhelm-Benartzi, Alan Kenneth Burnett, Nigel H. Russell, Matthew Collin, and Venetia Bigley

Subjects

Lestaurtinib, business.industry, medicine.drug_class, Hematopoietic stem cell, Myeloid leukemia, Induction chemotherapy, medicine.disease, Hypoplasia, Tyrosine-kinase inhibitor, medicine.anatomical_structure, medicine, Cancer research, Biomarker (medicine), Progenitor cell, business, medicine.drug

Abstract

Fms-like tyrosine kinase 3 (Flt3) is a hematopoietic growth factor receptor expressed on lymphomyeloid progenitors and frequently, by AML blasts. Its ligand, Flt3L, has non-hematopoietic and lymphoid origins, is detectable during homeostasis and increases to high levels in states of hypoplasia due to genetic defects or treatment with cytoreductive agents. Measurement of Flt3L by ELISA reveals that Flt3+AML, is associated with depletion of Flt3L to undetectable levels. After induction chemotherapy, Flt3L is restored in patients entering CR, but remains depressed in those with refractory disease. Weekly sampling reveals marked differences in the kinetics of Flt3L response during the first 6 weeks of treatment, proportionate to the clearance of blasts and cellularity of the BM. In the UK NCRI AML17 trial, Flt3L was measured at day 26 in a subgroup of 135 patients with Flt3 mutation randomized to the tyrosine kinase inhibitor lestaurtinib. In these patients, attainment of CR was associated with higher Flt3L at day 26 (Mann-Whitney p < 0.0001). Day 26 Flt3L was also associated with survival: Flt3L ≤ 291pg/ml was associated with inferior event-free survival; and, Flt3L >1185pg/ml was associated with higher overall survival (p = 0.0119). Serial measurement of Flt3L in patients who had received a hematopoietic stem cell transplant for AML further illustrated the potential value of declining Flt3L to identify relapse. Together these observations suggest that measurement of Flt3L provides a non-invasive estimate of progenitor cell mass in most patients with AML, with the potential to inform clinical decisions.Graphical abstract

Published

2019

27. Serum Flt3 ligand is a biomarker of progenitor cell mass and prognosis in acute myeloid leukemia

Author

Nigel H. Russell, Charlotte Wilhelm-Benartzi, Alan Kenneth Burnett, Helen Marr, Mark Levis, Michael R. Grunwald, Matthew Collin, Angela Grech, Gail Jones, Amy Publicover, Richard Dillon, Sarah Pagan, Steven Knapper, Sylvie D. Freeman, Paul Milne, Kathleen Gallagher, Anne M. Dickinson, and Venetia Bigley

Subjects

Oncology, medicine.medical_specialty, Myeloid, medicine.drug_class, medicine.medical_treatment, Gene Expression, Hematopoietic stem cell transplantation, Tyrosine-kinase inhibitor, Immunophenotyping, Internal medicine, hemic and lymphatic diseases, medicine, Humans, Progenitor cell, Proportional Hazards Models, Myeloid Neoplasia, business.industry, Lestaurtinib, Hematopoietic Stem Cell Transplantation, Myeloid leukemia, Membrane Proteins, Hematology, Induction Chemotherapy, medicine.disease, Prognosis, Minimal residual disease, Leukemia, Leukemia, Myeloid, Acute, medicine.anatomical_structure, Treatment Outcome, Neoplastic Stem Cells, business, Biomarkers, medicine.drug

Abstract

Fms-like tyrosine kinase 3 (Flt3) is expressed on progenitor cells and acute myeloid leukemia (AML) blasts. Fms-like tyrosine kinase 3 ligand (Flt3L) is detectable during homeostasis and increases in hypoplasia due to genetic defects or treatment with cytoreductive agents. Conversely, Flt31 AML is associated with depletion of Flt3L to undetectable levels. After induction chemotherapy, Flt3L is restored in patients entering complete remission (CR) but remains depressed in those with refractory disease. Weekly sampling reveals marked differences in the kinetics of Flt3L response during the first 6 weeks of treatment, proportionate to the clearance of blasts and cellularity of the bone marrow. In the UK NCRI AML17 trial, Flt3L was measured at day 26 in a subgroup of 140 patients with Flt3 mutation randomized to the tyrosine kinase inhibitor lestaurtinib or placebo. In these patients, attainment of CR was associated with higher Flt3L at day 26 (Mann-Whitney U P, .0001). Day 26 Flt3L was also associated with survival; Flt3L #291 pg/mL was associated with inferior event-free survival (EFS), and Flt3L .1185 pg/mL was associated with higher overall survival (OS; P 5 .0119). The separation of EFS and OS curves increased when minimal residual disease (MRD) status was combined with Flt3L measurement, and Flt3L retained a near-significant association with survival after adjusting for MRD in a proportional hazards model. Serial measurement of Flt3L in patients who had received a hematopoietic stem cell transplant for AML illustrates the potential value of monitoring Flt3L to identify relapse. Measurement of Flt3L is a noninvasive test with the potential to inform clinical decisions in patients with AML.

Published

2019

28. Hematopoietic origin of Langerhans cell histiocytosis and Erdheim-Chester disease in adults

Author

Johannes Visser, Venetia Bigley, Kenneth L. McClain, Chris M. Bacon, David Hunt, Benjamin H. Durham, Paul Milne, Carl E. Allen, Simon Bomken, Mac Macheta, Matthew Collin, Naomi McGovern, Muzlifah Haniffa, Omar Abdel-Wahab, Harsha P. Gunawardena, Antoine Néel, Eli L. Diamond, McGovern, Naomi [0000-0001-5200-2698], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, Male, Pathology, Myeloid, Lipopolysaccharide Receptors, Gene Expression, Biochemistry, Monocytes, Antigens, CD1, 0302 clinical medicine, Immunophenotyping, Langerhans cell histiocytosis, Transforming Growth Factor beta, Myeloid Neoplasia, biology, Receptors, Notch, Cell Differentiation, Hematology, Haematopoiesis, Histiocytosis, medicine.anatomical_structure, Female, Adult, Proto-Oncogene Proteins B-raf, medicine.medical_specialty, Erdheim-Chester Disease, Langerin, Immunology, Bone Marrow Cells, Diagnosis, Differential, 03 medical and health sciences, Antigens, CD, medicine, Humans, Lectins, C-Type, Histiocyte, Alleles, Glycoproteins, business.industry, Granulocyte-Macrophage Colony-Stimulating Factor, Cell Biology, Dendritic Cells, medicine.disease, Hematopoietic Stem Cells, Histiocytosis, Langerhans-Cell, 030104 developmental biology, Mannose-Binding Lectins, Mutation, biology.protein, Bone marrow, business, 030215 immunology, Foam Cells

Abstract

Langerhans cell histiocytosis (LCH) and Erdheim-Chester disease (ECD) are rare histiocytic disorders induced by somatic mutation of MAPK pathway genes. BRAFV600E mutation is the most common mutation in both conditions and also occurs in the hematopoietic neoplasm hairy cell leukemia (HCL). It is not known if adult LCH or ECD arises from hematopoietic stem cells (HSCs), nor which potential blood borne precursors lead to the formation of histiocytic lesions. In this study, BRAFV600E allele-specific polymerase chain reaction was used to map the neoplastic clone in 20 adults with LCH, ECD, and HCL. BRAFV600E was tracked to classical monocytes, nonclassical monocytes, and CD1c+ myeloid dendritic cells (DCs) in the blood, and mutations were observed in HSCs and myeloid progenitors in the bone marrow of 4 patients. The pattern of involvement of peripheral blood myeloid cells was indistinguishable between LCH and ECD, although the histiocytic disorders were distinct to HCL. As reported in children, detection of BRAFV600E in peripheral blood of adults was a marker of active multisystem LCH. The healthy counterparts of myeloid cells affected by BRAF mutation had a range of differentiation potentials depending on exogenous signals. CD1c+ DCs acquired high langerin and CD1a with granulocyte-macrophage colony-stimulating factor and transforming growth factor β alone, whereas CD14+ classical monocytes required additional notch ligation. Both classical and nonclassical monocytes, but not CD1c+ DCs, made foamy macrophages easily in vitro with macrophage colony-stimulating factor and human serum. These studies are consistent with a hematopoietic origin and >1 immediate cellular precursor in both LCH and ECD.

Published

2019

29. Differential IRF8 Requirement Defines Two Pathways of Dendritic Cell Development in Humans

Author

Benjamin C. Carpenter, Sarah Pagan, Sophie Hambleton, Gina M. Doody, Paul Milne, James Thaventhiran, Rosie Hague, Matthew Collin, Venetia Bigley, Kile Green, Anastasia Resteu, Andrew Filby, Urszula Cytlak, Sheetal Maisuria, Hana Lango Allen, Rachel Queen, Gillian Hulme, and David McDonald

Subjects

Cyclin-dependent kinase 1, education.field_of_study, Myeloid, Population, Dendritic cell, Biology, In vitro, Cell biology, Haematopoiesis, medicine.anatomical_structure, medicine, IRF8, education, Transcription factor

Abstract

The formation of human dendritic cells (DC) is controlled by multiple hematopoietic transcription factors, including IRF8. Loss of IRF8 differentially affects plasmacytoid DC (pDC) and the classical DC lineages, cDC1 and cDC2. Additionally, cDC2 are heterogeneous, comprising DC-like DC2 and monocyte-like DC3. Using high dimensional analysis, in vitro differentiation, and an allelic series of human IRF8 deficiency, we show that CD1c+DC heterogeneity originates from two distinct pathways of DC development. The lymphoid-primed IRF8high pathway carries pDC, cDC1, and DC2 trajectories, while the common myeloid IRF8low pathway forms DC3 and monocytes. We trace distinct trajectories of cDC1, DC2 and DC3 through the GMP showing that AXL+SIGLEC6+ pre-DC map exclusively to the DC2 pathway. The preservation of human CD1c+DC in partial IRF8 deficiency is explained by the replacement of DC2 by an expanded DC3 population. These observations are congruent with lineage-primed models of hematopoiesis, illustrating new links between immune cell function and ontogeny.

Published

2019

30. Epigenetic Regulator Genes Direct the Fate of Multipotent Progenitor Cell of Origin in Lineage Switched MLL-AF4 Leukaemia

Author

Simon Bomken, James C. Mulloy, Peter Carey, Zoya Kingsbury, Josef Vormoor, Paul Milne, Christine J. Harrison, Helen Blair, Jennifer Becq, Lisa J. Russell, Peter N. Cockerill, Jean-Baptiste Cazier, Constanze Bonifer, Daniel Williamson, James M Allan, Paul Evans, Anetta Ptasinska, Sirintra Nakjang, Maria Rosaria Imperato, Elena Zerkalenkova, Rolf Marschalek, Michael J. Thirman, Shan Lin, Alex Smith, Natalia Miakova, Muzlifa Haniffa, Ricky Tirtakusuma, Simon Bailey, Salam A. Assi, Catherine Cargo, Pierre Cauchy, Y Shi, Hesta McNeill, Yulia Olshanskaya, Fotini Vogiatzi, Claus Meyer, Sarah E. Fordham, Alex Elder, Matthew Collin, Roderick Skinner, Venetia Bigley, Olaf Heidenreich, A Komkov, Cornelia Eckert, Deepali Pal, Denis M. Schewe, N Martinez-Soria, and Oskar A. Haas

Subjects

education.field_of_study, Myeloid, Lineage (genetic), Population, Clone (cell biology), Epigenome, Biology, Cell biology, medicine.anatomical_structure, hemic and lymphatic diseases, medicine, Epigenetics, Progenitor cell, education, neoplasms, Epigenomics

Abstract

SummaryThe translocation MLL-AF4 defines a high-risk subtype of acute leukaemia which, uniquely amongst MLL translocations, is almost exclusively associated with a pro-B lymphoid phenotype. However, the ability to switch lineage at relapse allowed interrogation of the cellular origin and lineage determinants of this leukaemia. The origin of MLL-AF4 lymphoid leukaemia was commonly within a multipotent precursor population. In contrast, relapse as MLL-AF4 AML occurs from either a multipotent progenitor or a committed pro-B leukaemic clone. Lineage switching results from the dysregulation of chromatin modifiers, including the nucleosome remodelling and deacetylation complex, NuRD, completely extinguishing the B lymphoid gene regulatory network, instead establishing a myeloid epigenotype. We propose that, in contrast to mixed phenotype acute leukaemias, lineage switch in MLL-AF4 leukemia is driven and maintained by a reorganised epigenome.

Published

2019

31. Notch Signaling Facilitates In Vitro Generation of Cross-Presenting Classical Dendritic Cells

Author

Margaret E, Kirkling, Urszula, Cytlak, Colleen M, Lau, Kanako L, Lewis, Anastasia, Resteu, Alireza, Khodadadi-Jamayran, Christian W, Siebel, Hélène, Salmon, Miriam, Merad, Aristotelis, Tsirigos, Matthew, Collin, Venetia, Bigley, and Boris, Reizis

Subjects

Receptors, CCR7, Receptors, Notch, Manchester Cancer Research Centre, ResearchInstitutes_Networks_Beacons/mcrc, Vaccination, Bone Marrow Cells, Cell Differentiation, Dendritic Cells, Hematopoietic Stem Cells, Article, Mice, Inbred C57BL, Cross-Priming, Cell Movement, Animals, Humans, Signal Transduction

Abstract

The IRF8-dependent subset of classical dendritic cells (cDCs), termed cDC1, is important for cross-priming cytotoxic T cell responses against pathogens and tumors. Culture of hematopoietic progenitors with DC growth factor FLT3 ligand (FLT3L) yields very few cDC1s (in humans) or only immature “cDC1-like” cells (in the mouse). We report that OP9 stromal cells expressing the Notch ligand Delta-like 1 (OP9-DL1) optimize FLT3L-driven development of cDC1s from murine immortalized progenitors and primary bone marrow cells. Co-culture with OP9-DL1 induced IRF8-dependent cDC1s with a phenotype (CD103+ Dec205+ CD8α+) and expression profile resembling primary splenic cDC1s. OP9-DL1-induced cDC1s showed preferential migration toward CCR7 ligands in vitro and superior T cell cross-priming and antitumor vaccination in vivo. Co-culture with OP9-DL1 also greatly increased the yield of IRF8-dependent CD141+ cDC1s from human bone marrow progenitors cultured with FLT3L. Thus, Notch signaling optimizes cDC generation in vitro and yields authentic cDC1s for functional studies and translational applications. Dendritic cells (DCs) are critical inducers of immune responses, but current methods to generate them in vitro are suboptimal. Kirkling et al. report that Notch signaling facilitates the generation of DCs that closely resemble their in vivo counterparts and show superior capacity to vaccinate against tumors in vivo.

Published

2018

32. Human fetal dendritic cells promote prenatal T-cell immune suppression through arginase-2

Author

Yie Hou Lee, Donovan Low, Yiping Fan, Nurhidaya Binte Shadan, Edwin Huang Kunxiang, Venetia Bigley, Sandra Hubert, Dedrick Kok Hong Chan, Matthew Collin, Anis Larbi, Gillian Low, John Kit Chung Tam, Peter See, Michael Poidinger, Erin Soon, Kaibo Duan, Citra Nurfarah Zaini Mattar, Mahesh Choolani, Esther Wing Hei Mok, Muzlifah Haniffa, Salvatore Albani, Christopher Schuster, Jerry Kok Yen Chan, Baptiste Janela, Naomi McGovern, Florent Ginhoux, Xiao-Nong Wang, Tony Kiat Hon Lim, Evan W. Newell, Rasha Msallam, Leong Jing Yao, Adelheid Elbe-Bürger, Josephine Lum, Ivy Low, Hermi Sumatoh, Andreas Schlitzer, Amanda Shin, Ker-Kan Tan, McGovern, Naomi [0000-0001-5200-2698], and Apollo - University of Cambridge Repository

Subjects

0301 basic medicine, immunology [Dendritic Cells], T-Lymphocytes, T-Lymphocytes, Regulatory, immunology [T-Lymphocytes], Immune tolerance, 0302 clinical medicine, metabolism [Arginase], Cell Movement, Receptor, enzymology [Fetus], Multidisciplinary, Toll-Like Receptors, cytology [Fetus], medicine.anatomical_structure, cytology [T-Lymphocytes, Regulatory], Cytokines, ddc:500, cytology [Lymph Nodes], immunology [T-Lymphocytes, Regulatory], Adult, cytology [T-Lymphocytes], T cell, arginase II, human, Article, 03 medical and health sciences, Immune system, Fetus, Antigen, Immunity, medicine, Immune Tolerance, Humans, immunology [Lymph Nodes], Cell Proliferation, enzymology [Dendritic Cells], Arginase, biosynthesis [Cytokines], immunology [Fetus], Dendrites, Dendritic Cells, 030104 developmental biology, immunology [Toll-Like Receptors], immunology [Cytokines], Immunology, Lymph Nodes, Homeostasis, 030215 immunology

Abstract

During gestation the developing human fetus is exposed to a diverse range of potentially immune-stimulatory molecules including semi-allogeneic antigens from maternal cells, substances from ingested amniotic fluid, food antigens, and microbes. Yet the capacity of the fetal immune system, including antigen-presenting cells, to detect and respond to such stimuli remains unclear. In particular, dendritic cells, which are crucial for effective immunity and tolerance, remain poorly characterized in the developing fetus. Here we show that subsets of antigen-presenting cells can be identified in fetal tissues and are related to adult populations of antigen-presenting cells. Similar to adult dendritic cells, fetal dendritic cells migrate to lymph nodes and respond to toll-like receptor ligation; however, they differ markedly in their response to allogeneic antigens, strongly promoting regulatory T-cell induction and inhibiting T-cell tumour-necrosis factor-α production through arginase-2 activity. Our results reveal a previously unappreciated role of dendritic cells within the developing fetus and indicate that they mediate homeostatic immune-suppressive responses during gestation.

Published

2018

33. Cell(s) of Origin of Langerhans Cell Histiocytosis

Author

Kenneth L. McClain, Venetia Bigley, Carl E. Allen, and Matthew Collin

Subjects

Pathology, medicine.medical_specialty, Myeloid, Langerin, biology, business.industry, Cellular differentiation, Hematology, Dendritic cell, medicine.disease, Haematopoiesis, medicine.anatomical_structure, Oncology, Langerhans cell histiocytosis, biology.protein, medicine, Progenitor cell, business, Histiocyte

Abstract

Langerhans cell histiocytosis (LCH) is heterogeneous disease characterized by common histology of inflammatory lesions containing Langerin(+) (CD207) histiocytes. Emerging data support a model in which MAPK activation in self-renewing hematopoietic progenitors may drive disseminated high-risk disease, whereas MAPK activation in more differentiated committed myeloid populations may induce low-risk LCH. The heterogeneous clinical manifestations with shared histology may represent the final common pathway of an acquired defect of differentiation, initiated at more than one point. Implications of this model include re-definition of LCH as a myeloid neoplasia and re-focusing therapeutic strategies on the cells and lineages of origin.

Published

2015

34. Human mononuclear phagocyte system reunited

Author

Muzlifah Haniffa, Venetia Bigley, and Matthew Collin

Subjects

Antigen presentation, Inflammation, Adaptive Immunity, Biology, Monocytes, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Homologous chromosome, Animals, Humans, Macrophage, Mononuclear Phagocyte System, 030304 developmental biology, 0303 health sciences, Macrophages, Monocyte, Models, Immunological, Cell Differentiation, Dendritic Cells, Cell Biology, Mononuclear phagocyte system, Acquired immune system, medicine.anatomical_structure, Immunology, medicine.symptom, 030215 immunology, Developmental Biology

Abstract

The human mononuclear phagocyte network comprises dendritic cells (DCs), monocytes and macrophages with a range of immune functions including antigen presentation linking innate and adaptive immunity. A number of DC, monocyte and macrophage subsets have been described in lymphoid and non-lymphoid tissues of mouse and human, with increased understanding of their distinct functional properties and genetic and cellular pathways of development. More recently, through comparative biology studies, a unified nomenclature of mononuclear phagocytes has begun to emerge with the identification of homologous subsets in several species. In this review, we discuss the current classification of human mononuclear phagocytes and the parallel organization of this network in the mouse. We also review the genetic control and developmental pathway of human mononuclear phagocytes and the immunological functions of the distinct subsets in health and inflammation.

Published

2015

35. Langerin-expressing dendritic cells in human tissues are related to CD1c+ dendritic cells and distinct from Langerhans cells and CD141high XCR1+ dendritic cells

Author

Venetia, Bigley, Naomi, McGovern, Paul, Milne, Rachel, Dickinson, Sarah, Pagan, Sharon, Cookson, Muzlifah, Haniffa, and Matthew, Collin

Subjects

Serum, Lymphoid Tissue, Thrombomodulin, Receptors, G-Protein-Coupled, Antigens, CD1, Mice, Transforming Growth Factor beta, Antigens, CD, GATA2, Homeostasis, Animals, Humans, Lectins, C-Type, Lung, Bone Morphogenetic Protein Receptors, Type I, Skin, DCML deficiency, Glycoproteins, integumentary system, Gene Expression Profiling, differentiation, Dendritic Cells, Antigens, Differentiation, Mannose-Binding Lectins, Liver, Organ Specificity, Langerhans Cells, antigen presenting cell, Antigens, Surface, HSCT, Spotlight on Leading Edge Research

Abstract

Langerin is not restricted to Langerhans cells, but expressed at low levels by CD1c+ dendritic cells and is inducible by TGFβ in humans., Langerin is a C-type lectin expressed at high level by LCs of the epidermis. Langerin is also expressed by CD8+/CD103+ XCR1+ cross-presenting DCs of mice but is not found on the homologous human CD141high XCR1+ myeloid DC. Here, we show that langerin is expressed at a low level on DCs isolated from dermis, lung, liver, and lymphoid tissue and that langerin+ DCs are closely related to CD1c+ myeloid DCs. They are distinguishable from LCs by the level of expression of CD1a, EpCAM, CD11b, CD11c, CD13, and CD33 and are found in tissues and tissue-draining LNs devoid of LCs. They are unrelated to CD141high XCR1+ myeloid DCs, lacking the characteristic expression profile of cross-presenting DCs, conserved between mammalian species. Stem cell transplantation and DC deficiency models confirm that dermal langerin+ DCs have an independent homeostasis to LCs. Langerin is not expressed by freshly isolated CD1c+ blood DCs but is rapidly induced on CD1c+ DCs by serum or TGF-β via an ALK-3-dependent pathway. These results show that langerin is expressed outside of the LC compartment of humans and highlight a species difference: langerin is expressed by the XCR1+ "DC1" population of mice but is restricted to the CD1c+ "DC2" population of humans (homologous to CD11b+ DCs in the mouse).

Published

2014

36. Successful outcome following allogeneic hematopoietic stem cell transplantation in adults with primary immunodeficiency

Author

Karl S. Peggs, Shari Denovan, Victoria Grandage, Andrew Symes, Sarah Grace, B Carpenter, Stephen Mackinnon, Ronjon Chakraverty, BJ Uttenthal, Emma C. Morris, Thomas A. Fox, Adele K. Fielding, Rachael Hough, Venetia Bigley, Kirsty Thomson, David M. Lowe, Sarita Workman, Matthew Buckland, Julia Dahlstrom, Panagiotis D. Kottaridis, and Siobhan O. Burns

Subjects

0301 basic medicine, Adult, medicine.medical_specialty, Transplantation Conditioning, Adolescent, medicine.medical_treatment, Immunology, Hematopoietic stem cell transplantation, Biochemistry, Cohort Studies, 03 medical and health sciences, Young Adult, Internal medicine, medicine, Humans, Transplantation, Homologous, Survival rate, business.industry, Hematopoietic Stem Cell Transplantation, Immunologic Deficiency Syndromes, Cell Biology, Hematology, Middle Aged, medicine.disease, Prognosis, Fludarabine, Transplantation, Survival Rate, 030104 developmental biology, Primary immunodeficiency, Alemtuzumab, Female, business, Busulfan, medicine.drug

Abstract

The primary immunodeficiencies (PIDs), rare inherited diseases characterized by severe dysfunction of immunity, have been successfully treated by allogeneic hematopoietic stem cell transplantation (Allo-HSCT) in childhood. Controversy exists regarding optimal timing and use of Allo-HSCT in adults, due to lack of experience and previous poor outcomes. Twenty-nine consecutive adult patients, with a mean age at transplant of 24 years (range, 17-50 years), underwent Allo-HSCT. Reduced-intensity conditioning (RIC) included fludarabine (Flu)/melphalan/alemtuzumab (n = 20), Flu/busulfan (Bu)/alemtuzumab (n = 8), and Flu/Bu/antithymocyte globulin (n = 1). Stem cell donors were matched unrelated donors or mismatched unrelated donors (n = 18) and matched related donors (n = 11). Overall survival (OS), event-free survival, transplant-related mortality (TRM), acute and chronic graft-versus-host disease incidence and severity, time to engraftment, lineage-specific chimerism, immune reconstitution, and discontinuation of immunoglobulin replacement therapy were recorded. OS at 3 years for the whole cohort was 85.2%. The rarer PID patients without chronic granulomatous disease (CGD) achieved an OS at 3 years of 88.9% (n = 18), compared with 81.8% for CGD patients (n = 11). TRM was low with only 4 deaths observed at a median follow-up of 3.5 years. There were no cases of early or late rejection. In all surviving patients, either stable mixed chimerism or full donor chimerism were observed. At last follow-up, 87% of the surviving patients had no evidence of persistent or recurrent infections. Allo-HSCT is safe and effective in young adult patients with severe PID and should be considered the treatment of choice where an appropriate donor is available.

Published

2017

37. Monocyte, Macrophage, and Dendritic Cell Development: the Human Perspective

Author

Matthew Collin and Venetia Bigley

Published

2017

38. Functional characterization of the human dendritic cell immunodeficiency associated with the IRF8K108E mutation

Author

Karina Butler, Jean-Laurent Casanova, Philippe Gros, David Langlais, David L. Burk, Francois Lefebvre, Albert M. Berghuis, Timothy Ronan Leahy, Muzz Haniffa, Sophie Hambleton, Venetia Bigley, Guillaume Bourque, and Sandra Salem

Subjects

Myeloid, Immunology, Mutation, Missense, Biology, Biochemistry, Lymphohistiocytosis, Hemophagocytic, Antigen, T-Lymphocyte Subsets, medicine, Humans, Immunodeficiency, Immunobiology, Clonal Anergy, Antigen Presentation, Protein Stability, Homozygote, Immunologic Deficiency Syndromes, Infant, Dendritic Cells, Cell Biology, Hematology, Dendritic cell, medicine.disease, Transplantation, HEK293 Cells, medicine.anatomical_structure, Amino Acid Substitution, Cord blood, Interferon Regulatory Factors, Cancer research, RNA, Female, Mutant Proteins, Cord Blood Stem Cell Transplantation, IRF8, Protein Processing, Post-Translational, CD81

Abstract

We have previously reported on a unique patient in whom homozygosity for a mutation at IRF8 (IRF8(K108E)) causes a severe immunodeficiency. Laboratory evaluation revealed a highly unusual myeloid compartment, remarkable for the complete absence of CD141 and CD161 monocytes, absence of CD11c1 conventional dendritic cells (DCs) and CD11c1/CD1231 plasmacytoid DCs, and striking granulocytic hyperplasia. The patient initially presented with severe disseminated mycobacterial and mucocutaneous fungal infections and was ultimately cured by cord blood transplant. Sequencing RNA from the IRF8(K108E) patient's primary blood cells prior to transplant shows not only depletion of IRF8-bound and IRF8-regulated transcriptional targets, in keeping with the distorted composition of the myeloid compartment, but also a paucity of transcripts associated with activated CD41 and CD81 T lymphocytes. This suggests that T cells reared in the absence of a functional antigen-presenting compartment in IRF8(K108E) are anergic. Biochemical characterization of the IRF8(K108E) mutant in vitro shows that loss of the positively charged side chain at K108 causes loss of nuclear localization and loss of transcriptional activity, which is concomitant with decreased protein stability, increased ubiquitination, increased small ubiquitin-like modification, and enhanced proteasomal degradation. These findings provide functional insight into the molecular basis of immunodeficiency associated with loss of IRF8.

Published

2014

39. Monocyte, Macrophage, and Dendritic Cell Development: the Human Perspective

Author

Venetia Bigley and Matthew Collin

Subjects

0301 basic medicine, Microbiology (medical), Myeloid, Physiology, Biology, Peripheral blood mononuclear cell, Monocytes, 03 medical and health sciences, 0302 clinical medicine, Immune system, Genetics, medicine, Animals, Humans, General Immunology and Microbiology, Ecology, Macrophages, Cell Biology, Dendritic cell, Mononuclear phagocyte system, Dendritic Cells, Phenotype, Cell biology, Haematopoiesis, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Immunology, Models, Animal, Homeostasis, 030215 immunology

Abstract

The maintenance of monocytes, macrophages, and dendritic cells (DCs) involves manifold pathways of ontogeny and homeostasis that have been the subject of intense study in recent years. The concept of a peripheral mononuclear phagocyte system continually renewed by blood-borne monocytes has been modified to include specialized DC pathways of development that do not involve monocytes, and longevity through self-renewal of tissue macrophages. The study of development remains difficult owing to the plasticity of phenotypes and misconceptions about the fundamental structure of hematopoiesis. However, greater clarity has been achieved in distinguishing inflammatory monocyte-derived DCs from DCs arising in the steady state, and new concepts of conjoined lymphomyeloid hematopoiesis more easily accommodate the shared lymphoid and myeloid phenotypes of some DCs. Cross-species comparisons have also yielded coherent systems of nomenclature for all mammalian monocytes, macrophages, and DCs. Finally, the clear relationships between ontogeny and functional specialization offer information about the regulation of immune responses and provide new tools for the therapeutic manipulation of myeloid mononuclear cells in medicine.

Published

2016

40. Impact of Alemtuzumab Scheduling on Graft-versus-Host Disease after Unrelated Donor Fludarabine and Melphalan Allografts

Author

Charles Craddock, Stephen Mackinnon, Venetia Bigley, Laura Jardine, Kirsty Thomson, Phillip L R Nicolson, Kile Green, Graham Jackson, Rob S. Sellar, Kim F. Pearce, Sandeep Nagra, Matthew Collin, Anne M. Dickinson, and Karl S. Peggs

Subjects

Melphalan, Adult, Male, medicine.medical_specialty, Transplantation Conditioning, Graft vs Host Disease, Gastroenterology, Drug Administration Schedule, Article, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Internal medicine, medicine, Humans, Alemtuzumab, Aged, Retrospective Studies, Transplantation, Dose-Response Relationship, Drug, business.industry, Retrospective cohort study, Hematology, Middle Aged, medicine.disease, Allografts, Fludarabine, Surgery, Regimen, Graft-versus-host disease, surgical procedures, operative, 030220 oncology & carcinogenesis, Hematologic Neoplasms, Cohort, Female, business, Unrelated Donors, Vidarabine, 030215 immunology, medicine.drug

Abstract

Alemtuzumab conditioning is highly effective at reducing the incidence of acute and chronic graft-versus-host disease (GVHD) in reduced-intensity fludarabine and melphalan transplantation with cyclosporine monotherapy. Less frequent and lower dose scheduling may be used with sibling donors, but an optimal regimen for matched unrelated donors has not been defined. In this retrospective observational study of 313 patients, the incidence and severity of GVHD was compared in patients receiving 3 different dose schedules: the standard 100-mg regimen (20 mg on days –7 to –3), 60 mg (30 mg on days –4 and –2), or 50 mg (10 mg on days –7 to –3). Patients treated with 100 mg, 60 mg, or 50 mg developed acute GVHD grades I to IV with an incidence of 74%, 65%, and 64%, respectively, whereas 36%, 32%, and 41% developed chronic GHVD. An excess of severe acute grades III/IV GVHD was observed in the 50-mg cohort (15% versus 2% to 6%; P = .016). The relative risk of severe acute grade GVHD remained more than 3-fold higher in the 50-mg cohort compared with the 100-mg cohort after adjustment for differences in HLA match, age, gender mismatch, cytomegalovirus risk, and diagnosis (P = .030). The findings indicate that the 60-mg alemtuzumab schedule was comparable with the 100-mg schedule, but more attenuated schedules may increase the risk of severe grade GVHD.

Published

2016

41. Adaptive NK cells can persist in patients with

Author

Weixin Wang, Katherine R. Calvo, Samuel C. C. Chiang, Matthew Collin, Cynthia E. Dunbar, Venetia Bigley, Thomas Winkler, Steve M. Holland, Pål Aukrust, Ingvild Nordøy, Amy P. Hsu, Danielle M. Townsley, Yenan T. Bryceson, Heinrich Schlums, Moonjung Jung, Jan K Davidson-Moncada, Rachel E. Dickinson, Tim D. Holmes, Hongya Han, David S.J. Allan, and Jakob Theorell

Subjects

0301 basic medicine, Cytotoxicity, Immunologic, Adult, Male, Adolescent, Immunology, Syk, Biology, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, Interferon, Inside BLOOD Commentary, medicine, Cytotoxic T cell, Humans, Syk Kinase, Progenitor cell, Child, Immunobiology, Cell Proliferation, Receptors, IgE, GATA2, Interleukin-18, RNA-Binding Proteins, Cell Biology, Hematology, Middle Aged, Hematopoietic Stem Cells, Interleukin-12, GATA2 Transcription Factor, Killer Cells, Natural, Haematopoiesis, 030104 developmental biology, Mutation, Cancer research, Neural cell adhesion molecule, Calmodulin-Binding Proteins, Female, Stem cell, RNA-Binding Protein EWS, 030215 immunology, medicine.drug, Transcription Factors

Abstract

Heterozygous GATA2 mutation is associated with immunodeficiency, lymphedema, and myelodysplastic syndrome. Disease presentation is variable, often coinciding with loss of circulating dendritic cells, monocytes, B cells, and natural killer (NK) cells. Nonetheless, in a proportion of patients carrying GATA2 mutation, NK cells persist. We found that peripheral blood NK cells in symptomatic patients uniformly lacked expression of the transcription factor promyelocytic leukemia zinc finger (PLZF), as well as expression of intracellular signaling proteins FceRγ, spleen tyrosine kinase (SYK), and EWS/FLI1-Activated Transcript 2 (EAT-2) in a variegated manner. Moreover, consistent with an adaptive identity, NK cells from patients with GATA2 mutation displayed altered expression of cytotoxic granule constituents and produced interferon-γ upon Fc-receptor engagement but not following combined interleukin-12 (IL-12) and IL-18 stimulation. Canonical, PLZF-expressing NK cells were retained in asymptomatic carriers of GATA2 mutation. Developmentally, GATA-binding protein-2 (GATA-2) was expressed in hematopoietic stem cells, but not in NK-cell progenitors, CD3-CD56bright, canonical, or adaptive CD3-CD56dim NK cells. Peripheral blood NK cells from individuals with GATA2 mutation proliferated normally in vitro, whereas lineage-negative progenitors displayed impaired NK-cell differentiation. In summary, adaptive NK cells can persist in patients with GATA2 mutation, even after NK-cell progenitors expire. Moreover, our data suggest that adaptive NK cells are more long-lived than canonical, immunoregulatory NK cells.

Published

2016

42. Human Tissues Contain CD141hi Cross-Presenting Dendritic Cells with Functional Homology to Mouse CD103+ Nonlymphoid Dendritic Cells

Author

Florent Ginhoux, Helen Zhao, Matthew Collin, Michael Poidinger, Antonio Bertoletti, Anis Larbi, Naomi McGovern, Peter See, Venetia Bigley, Amanda Shin, Laurent Rénia, Pavandip Singh Wasan, Benoit Malleret, John Siu-Lun Tam, Rachel E. Dickinson, Sharon Cookson, Ian Dimmick, Colin Song, Ruth F. Jarrett, Jerry Kok Yen Chan, Muzlifah Haniffa, Pearline Teo, Sarah Pagan, Frano Malinarich, Xiao-Nong Wang, Adam J. Gehring, John E. Connolly, and Pearlie W.W. Tan

Subjects

XCR1, Immunology, Biology, Article, Immunophenotyping, Transcriptome, Mice, 03 medical and health sciences, Cross-Priming, 0302 clinical medicine, Antigen, Antigens, CD, Cell Movement, medicine, Animals, Humans, Immunology and Allergy, Antigens, Lymph node, Skin, 030304 developmental biology, 0303 health sciences, Tumor Necrosis Factor-alpha, Gene Expression Profiling, Translation (biology), Dendritic Cells, 3. Good health, Cell biology, Chemokine CXCL10, Gene expression profiling, medicine.anatomical_structure, Infectious Diseases, Langerhans Cells, Tumor necrosis factor alpha, Lymph Nodes, Integrin alpha Chains, 030215 immunology

Abstract

Summary Dendritic cell (DC)-mediated cross-presentation of exogenous antigens acquired in the periphery is critical for the initiation of CD8+ T cell responses. Several DC subsets are described in human tissues but migratory cross-presenting DCs have not been isolated, despite their potential importance in immunity to pathogens, vaccines, and tumors and tolerance to self. Here, we identified a CD141hi DC present in human interstitial dermis, liver, and lung that was distinct from the majority of CD1c+ and CD14+ tissue DCs and superior at cross-presenting soluble antigens. Cutaneous CD141hi DCs were closely related to blood CD141+ DCs, and migratory counterparts were found among skin-draining lymph node DCs. Comparative transcriptomic analysis with mouse showed tissue DC subsets to be conserved between species and permitted close alignment of human and mouse DC subsets. These studies inform the rational design of targeted immunotherapies and facilitate translation of mouse functional DC biology to the human setting., Graphical Abstract Highlights ► Human tissues contain CD1c+ DCs, CD14+ DCs, and a CD141hi cross-presenting DC subset ► CD141hi DCs migrate to draining lymph nodes and probably arise from blood CD141+ DCs ► Human tissue CD141hi DCs are homologous to mouse CD103+ or CD8+ DCs ► Human tissue CD1c+ DCs are homologous to mouse CD4+ DCs

Published

2012

43. Biallelic mutations in IRF8 impair human NK cell maturation and function

Author

Graham D. Hogg, Sumihito Togi, Michael D. Keller, Tram N. Cao, Sinisa Savic, Matthew Collin, Ivan K. Chinn, Levi B. Watkin, Asbjørg Stray-Pedersen, Gina M. Doody, Matthew A. Care, Justin T. Gunesch, Duy T. Le, Shalini N. Jhangiani, Donna M. Muzny, Jordan S. Orange, Emily M. Mace, James R. Lupski, Mayra Hernandez-Sanabria, Andrew J. Cant, Venetia Bigley, Michael A. Caligiuri, Sheetal Maisuria, Steven M. Holland, Zeynep Coban Akdemir, Eva P. Szymanski, Jansen B. Smith, Aharon G. Freud, Silke Paust, Laura S. Angelo, Keiko Ozato, Richard A. Gibbs, and David F. LaRosa

Subjects

0301 basic medicine, Male, Biology, Cell Maturation, medicine.disease_cause, Communicable Diseases, 03 medical and health sciences, Interleukin 21, Mice, 0302 clinical medicine, medicine, Animals, Humans, Genetic Predisposition to Disease, Alleles, Mice, Knockout, Mutation, Cell growth, Janus kinase 3, Immunologic Deficiency Syndromes, General Medicine, CD56 Antigen, 3. Good health, Killer Cells, Natural, 030104 developmental biology, Gene Expression Regulation, Virus Diseases, Immunology, Interferon Regulatory Factors, Interleukin 12, Female, Stem cell, IRF8, Research Article, 030215 immunology

Abstract

Human NK cell deficiencies are rare yet result in severe and often fatal disease, particularly as a result of viral susceptibility. NK cells develop from hematopoietic stem cells, and few monogenic errors that specifically interrupt NK cell development have been reported. Here we have described biallelic mutations in IRF8, which encodes an interferon regulatory factor, as a cause of familial NK cell deficiency that results in fatal and severe viral disease. Compound heterozygous or homozygous mutations in IRF8 in 3 unrelated families resulted in a paucity of mature CD56dim NK cells and an increase in the frequency of the immature CD56bright NK cells, and this impairment in terminal maturation was also observed in Irf8–/–, but not Irf8+/–, mice. We then determined that impaired maturation was NK cell intrinsic, and gene expression analysis of human NK cell developmental subsets showed that multiple genes were dysregulated by IRF8 mutation. The phenotype was accompanied by deficient NK cell function and was stable over time. Together, these data indicate that human NK cells require IRF8 for development and functional maturation and that dysregulation of this function results in severe human disease, thereby emphasizing a critical role for NK cells in human antiviral defense.

Published

2015

44. IRF8Mutations and Human Dendritic-Cell Immunodeficiency

Author

Frederic Geissmann, Xiao-Fei Kong, Rainer Doffinger, Anny Fortin, Sandra Salem, Damien Chaussabel, Dewton Moraes-Vasconcelos, Chris M. Bacon, Venetia Bigley, Anete Sevciovic Grumach, Jacqueline Feinberg, Katia Abarca, Matthew Collin, Karina Butler, Lourdes Ceron-Gutierrez, Florent Ginhoux, Laurent Abel, Muzlifah Haniffa, Marjorie Hubeau, Jacinta Bustamante, Joana Azevedo, Dinakantha S. Kumararatne, Timothy J. Zumwalt, Albert M. Berghuis, David L. Burk, Jean-Laurent Casanova, Alberto José da Silva Duarte, Stéphanie Boisson-Dupuis, Geetha Menon, Eduardo Talesnik, Sophie Hambleton, Andrew J. Cant, Laia Alsina, David McDonald, Céline Trouillet, Philippe Gros, Peter Carey, and Saleh Al-Muhsen

Subjects

Severe combined immunodeficiency, business.industry, Monocyte, General Medicine, Dendritic cell, medicine.disease, Virology, Transplantation, medicine.anatomical_structure, Immunity, Immunology, medicine, IRF8, Antigen-presenting cell, business, Immunodeficiency

Abstract

BACKGROUND The genetic analysis of human primary immunodeficiencies has defined the contribution of specific cell populations and molecular pathways in the host defense against infection. Disseminated infection caused by bacille Calmette-Guerin (BCG) vaccines is an early manifestation of primary immunodeficiencies, such as severe combined immunodeficiency. In many affected persons, the cause of disseminated BCG disease is unexplained. METHODS We evaluated an infant presenting with features of severe immunodeficiency, including early-onset disseminated BCG disease, who required hematopoietic stem-cell transplantation. We also studied two otherwise healthy subjects with a history of disseminated but curable BCG disease in childhood. We characterized the monocyte and dendritic-cell compartments in these three subjects and sequenced candidate genes in which mutations could plausibly confer susceptibility to BCG disease. RESULTS We detected two distinct disease-causing mutations affecting interferon regulatory factor 8 (IRF8). Both K108E and T80A mutations impair IRF8 transcriptional activity by disrupting the interaction between IRF8 and DNA. The K108E variant was associated with an autosomal recessive severe immunodeficiency with a complete lack of circulating monocytes and dendritic cells. The T80A variant was associated with an autosomal dominant, milder immunodeficiency and a selective depletion of CD11c+CD1c+ circulating dendritic cells. CONCLUSIONS These findings define a class of human primary immunodeficiencies that affect the differentiation of mononuclear phagocytes. They also show that human IRF8 is critical for the development of monocytes and dendritic cells and for antimycobacterial immunity. (Funded by the Medical Research Council and others.).

Published

2011

45. The human syndrome of dendritic cell, monocyte, B and NK lymphoid deficiency

Author

Matthew Collin, Rachel E. Dickinson, Jonathan P. Wallis, Muzlifah Haniffa, Xiao-Nong Wang, Sarah Pagan, Naomi McGovern, Laura Jardine, Andrew J. Cant, Cliff Morgan, Venetia Bigley, Mirjam van der Burg, Sergei Doulatov, Jacques J.M. van Dongen, Sophie Hambleton, John E. Dick, James L. Lordan, Ignatius Chua, Rainer Doffinger, Dinakantha S. Kumararatne, Ian Dimmick, and Immunology

Subjects

Adult, CD4 antigen, CD14, Immunology, CD11c, chemical and pharmacologic phenomena, Bone Marrow Cells, Enzyme-Linked Immunosorbent Assay, Biology, Monocytes, Interferon-gamma, chemistry.chemical_compound, Interleukin 21, Antigens, CD, hemic and lymphatic diseases, medicine, Humans, Immunology and Allergy, Child, Mycobacterium Infections, Follicular dendritic cells, Monocyte, Brief Definitive Report, hemic and immune systems, Dendritic Cells, HLA-DR Antigens, Leukopenia, Syndrome, Dendritic cell, Flow Cytometry, Molecular biology, medicine.anatomical_structure, Microscopy, Fluorescence, chemistry, Disease Susceptibility, Bone marrow

Abstract

Human immunodeficiency syndrome with loss of DCs, monocytes, and T reg cells; preservation of Langerhans cells; associated loss of BM multilymphoid progenitors; and overproduction of Flt3 ligand., Congenital or acquired cellular deficiencies in humans have the potential to reveal much about normal hematopoiesis and immune function. We show that a recently described syndrome of monocytopenia, B and NK lymphoid deficiency additionally includes the near absence of dendritic cells. Four subjects showed severe depletion of the peripheral blood HLA-DR+ lineage− compartment, with virtually no CD123+ or CD11c+ dendritic cells (DCs) and very few CD14+ or CD16+ monocytes. The only remaining HLA-DR+ lineage− cells were circulating CD34+ progenitor cells. Dermal CD14+ and CD1a+ DC were also absent, consistent with their dependence on blood-derived precursors. In contrast, epidermal Langerhans cells and tissue macrophages were largely preserved. Combined loss of peripheral DCs, monocytes, and B and NK lymphocytes was mirrored in the bone marrow by complete absence of multilymphoid progenitors and depletion of granulocyte-macrophage progenitors. Depletion of the HLA-DR+ peripheral blood compartment was associated with elevated serum fms-like tyrosine kinase ligand and reduced circulating CD4+CD25hiFoxP3+ T cells, supporting a role for DC in T reg cell homeostasis.

Published

2011

46. Differential rates of replacement of human dermal dendritic cells and macrophages during hematopoietic stem cell transplantation

Author

Trevor A. Booth, Xiao-Nong Wang, M Abel, S Bullock, Venetia Bigley, Ian Dimmick, Florent Ginhoux, Matthew Collin, Catharien M. U. Hilkens, Miriam Merad, Peter J. Taub, Muzlifah Haniffa, and Marcos Augusto Grigolin Grisotto

Subjects

CD4-Positive T-Lymphocytes, CD14, medicine.medical_treatment, Immunology, Graft vs Host Disease, Hematopoietic stem cell transplantation, Biology, CD8-Positive T-Lymphocytes, Article, Proinflammatory cytokine, medicine, Immunology and Allergy, Humans, In Situ Hybridization, Fluorescence, Cell Proliferation, Microscopy, Confocal, Macrophages, Hematopoietic Stem Cell Transplantation, Cell Biology, Dendritic Cells, medicine.disease, Flow Cytometry, Transplantation, Cytokine, Graft-versus-host disease, Myeloid-derived Suppressor Cell, Cytokines, CD8

Abstract

Animal models of hematopoietic stem cell transplantation have been used to analyze the turnover of bone marrow-derived cells and to demonstrate the critical role of recipient antigen-presenting cells (APC) in graft versus host disease (GVHD). In humans, the phenotype and lineage relationships of myeloid-derived tissue APC remain incompletely understood. It has also been proposed that the risk of acute GVHD, which extends over many months, is related to the protracted survival of certain recipient APC. Human dermis contains three principal subsets of CD45(+)HLA-DR(+) cells: CD1a(+)CD14(-) DC, CD1a(-)CD14(+) DC, and CD1a(-)CD14(+)FXIIIa(+) macrophages. In vitro, each subset has characteristic properties. After transplantation, both CD1a(+) and CD14(+) DC are rapidly depleted and replaced by donor cells, but recipient macrophages can be found in GVHD lesions and may persist for many months. Macrophages isolated from normal dermis secrete proinflammatory cytokines. Although they stimulate little proliferation of naive or memory CD4(+) T cells, macrophages induce cytokine expression in memory CD4(+) T cells and activation and proliferation of CD8(+) T cells. These observations suggest that dermal macrophages and DC are from distinct lineages and that persistent recipient macrophages, although unlikely to initiate alloreactivity, may contribute to GVHD by sustaining the responses of previously activated T cells.

Published

2009

47. HUMAN BI-ALLELIC IRF8 MUTATIONS CAUSES DENDRITIC CELL DEFICIENCY AND MULTI-LINEAGE IMMUNE DYSREGULATION

Author

Venetia, Bigley, primary

Published

2017

48. Haematopoietic and immune defects associated with GATA2 mutation

Author

Matthew, Collin, Rachel, Dickinson, and Venetia, Bigley

Subjects

Heterozygote, Immunity, Reviews, Haploinsufficiency, Hematopoiesis, GATA2 Transcription Factor, Gene Expression Regulation, hemic and lymphatic diseases, Mutation, GATA2, Animals, Humans, Genetic Predisposition to Disease, bone marrow failure, immunodeficiency, Genetic Association Studies

Abstract

Heterozygous familial or sporadic GATA2 mutations cause a multifaceted disorder, encompassing susceptibility to infection, pulmonary dysfunction, autoimmunity, lymphoedema and malignancy. Although often healthy in childhood, carriers of defective GATA2 alleles develop progressive loss of mononuclear cells (dendritic cells, monocytes, B and Natural Killer lymphocytes), elevated FLT3 ligand, and a 90% risk of clinical complications, including progression to myelodysplastic syndrome (MDS) by 60 years of age. Premature death may occur from childhood due to infection, pulmonary dysfunction, solid malignancy and MDS/acute myeloid leukaemia. GATA2 mutations include frameshifts, amino acid substitutions, insertions and deletions scattered throughout the gene but concentrated in the region encoding the two zinc finger domains. Mutations appear to cause haplo-insufficiency, which is known to impair haematopoietic stem cell survival in animal models. Management includes genetic counselling, prevention of infection, cancer surveillance, haematopoietic monitoring and, ultimately, stem cell transplantation upon the development of MDS or another life-threatening complication.

Published

2015

49. A novel IKAROS haploinsufficiency kindred with unexpectedly late and variable B-cell maturation defects

Author

Joke Dehoorne, Elfride De Baere, Delfien Bogaert, Katherine R. Calvo, Filomeen Haerynck, Sergio D. Rosenzweig, Carolien Bonroy, Venetia Bigley, Melissa Dullaers, Frans De Baets, Hye Sun Kuehn, Urszula Cytlak, Marieke De Bruyne, and Arnaud Vanlander

Subjects

0301 basic medicine, Genetics, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, Immunity, B cell maturation, Immunology, Immunology and Allergy, Biology, Haploinsufficiency, Article

Published

2017

50. CD1c+ blood dendritic cells have Langerhans cell potential

Author

Muzlifah Haniffa, Matthew Collin, Merry Gunawan, Venetia Bigley, and Paul Milne

Subjects

Myeloid, Langerhans cell, Langerin, Birbeck granules, Cellular differentiation, Bone Morphogenetic Protein 7, Immunology, Biochemistry, Monocytes, Antigens, CD1, Antigens, CD, Transforming Growth Factor beta, medicine, Macrophage, Humans, Lectins, C-Type, Cells, Cultured, Immunobiology, Glycoproteins, Blood Cells, biology, integumentary system, Granulocyte-Macrophage Colony-Stimulating Factor, Cell Differentiation, Cell Biology, Hematology, Transforming growth factor beta, Dendritic Cells, Cadherins, Flow Cytometry, Cell biology, medicine.anatomical_structure, Granulocyte macrophage colony-stimulating factor, Mannose-Binding Lectins, Langerhans Cells, biology.protein, medicine.drug

Abstract

Langerhans cells (LCs) are self-renewing in the steady state but repopulated by myeloid precursors after injury. Human monocytes give rise to langerin-positive cells in vitro, suggesting a potential precursor role. However, differentiation experiments with human lineage-negative cells and CD34(+) progenitors suggest that there is an alternative monocyte-independent pathway of LC differentiation. Recent data in mice also show long-term repopulation of the LC compartment with alternative myeloid precursors. Here we show that, although monocytes are able to express langerin, when cultured with soluble ligands granulocyte macrophage colony-stimulating factor (GM-CSF), transforming growth factor β (TGFβ), and bone morphogenetic protein 7 (BMP7), CD1c(+) dendritic cells (DCs) become much more LC-like with high langerin, Birbeck granules, EpCAM, and E-cadherin expression under the same conditions. These data highlight a new potential precursor function of CD1c(+) DCs and demonstrate an alternative pathway of LC differentiation that may have relevance in vivo.

Published

2014