Your search keyword '"Sarah L. Gaffen"' showing total 202 results

1. A gut-oral microbiome–driven axis controls oropharyngeal candidiasis through retinoic acid

Author

Felix E.Y. Aggor, Martinna Bertolini, Chunsheng Zhou, Tiffany C. Taylor, Darryl A. Abbott, Javonn Musgrove, Vincent M. Bruno, Timothy W. Hand, and Sarah L. Gaffen

Subjects

Immunology, Medicine

Abstract

A side effect of antibiotics is outgrowth of the opportunistic fungus Candida albicans in the oropharynx (oropharyngeal candidiasis, OPC). IL-17 signaling is vital for immunity to OPC, but how the microbiome impacts antifungal immunity is not well understood. Mice in standard specific pathogen–free (SPF) conditions are resistant to OPC, whereas we show that germ-free (GF) or antibiotic-treated mice are susceptible. Oral type 17 cells and IL-17–dependent responses were impaired in antibiotic-treated and GF mice. Susceptibility could be rescued in GF mice by mono-colonization with segmented filamentous bacterium (SFB), an intestine-specific constituent of the microbiota. SFB protection was accompanied by restoration of oral IL-17+CD4+ T cells and gene signatures characteristic of IL-17 signaling. Additionally, RNA-Seq revealed induction of genes in the retinoic acid (RA) and RA receptor–α (RARα) pathway. Administration of RA rescued immunity to OPC in microbiome-depleted or GF mice, while RAR inhibition caused susceptibility in immunocompetent animals. Surprisingly, immunity to OPC was independent of serum amyloids. Moreover, RAR inhibition did not alter oral type 17 cytokine levels. Thus, mono-colonization with a component of the intestinal microflora confers protection against OPC by type 17 and RA/RARα, which act in parallel to promote antifungal immunity. In principle, manipulation of the microbiome could be harnessed to maintain antifungal immunity.

Published

2022

2. The RNA-binding protein IMP2 drives a stromal-Th17 cell circuit in autoimmune neuroinflammation

Author

Rami Bechara, Nilesh Amatya, Saikat Majumder, Chunsheng Zhou, Yang Li, Qixing Liu, Mandy J. McGeachy, and Sarah L. Gaffen

Subjects

Autoimmunity, Immunology, Medicine

Abstract

Stromal cells are emerging as key drivers of autoimmunity, partially because they produce inflammatory chemokines that orchestrate inflammation. Chemokine expression is regulated transcriptionally but also through posttranscriptional mechanisms, the specific drivers of which are still incompletely defined. CCL2 (MCP1) is a multifunctional chemokine that drives myeloid cell recruitment. During experimental autoimmune encephalomyelitis (EAE), an IL-17–driven model of multiple sclerosis, CCL2 produced by lymph node (LN) stromal cells was essential for immunopathology. Here, we showed that Ccl2 mRNA upregulation in human stromal fibroblasts in response to IL-17 required the RNA-binding protein IGF-2 mRNA-binding protein 2 (IGF2BP2, IMP2), which is expressed almost exclusively in nonhematopoietic cells. IMP2 binds directly to CCL2 mRNA, markedly extending its transcript half-life, and is thus required for efficient CCL2 secretion. Consistent with this, Imp2−/− mice showed reduced CCL2 production in LNs during EAE, causing impairments in monocyte recruitment and Th17 cell polarization. Imp2–/– mice were fully protected from CNS inflammation. Moreover, deletion of IMP2 after EAE onset was sufficient to mitigate disease severity. These data showed that posttranscriptional control of Ccl2 in stromal cells by IMP2 was required to permit IL-17–driven progression of EAE pathogenesis.

Published

2022

3. Regnase-1 Deficiency Restrains Klebsiella pneumoniae Infection by Regulation of a Type I Interferon Response

Author

Giraldina Trevejo-Nuñez, Becky Lin, Li Fan, Felix E. Y. Aggor, Partha S. Biswas, Kong Chen, and Sarah L. Gaffen

Subjects

Klebsiella, RNA binding proteins, Regnase, Microbiology, QR1-502

Abstract

ABSTRACT Excessive inflammation can cause tissue damage and autoimmunity, sometimes accompanied by severe morbidity or mortality. Numerous negative feedback mechanisms exist to prevent unchecked inflammation, but this restraint may come at the cost of suboptimal infection control. Regnase-1 (MCPIP1), a feedback regulator of IL-17 and LPS signaling, binds and degrades target mRNAs. Consequently, Reg1 deficiency exacerbates autoimmunity in multiple models. However, the role of Reg1 in bacterial immunity remains poorly defined. Here, we show that mice deficient in Reg1 are resistant to Klebsiella pneumoniae (KP). Reg1 deficiency did not accelerate bacterial eradication. Rather, Reg1-deficient alveolar macrophages had elevated Ifnb1 and enrichment of type I IFN genes. Blockade of IFNR during KP infection reversed disease improvement. Reg1 did not impact Ifnb1 stability directly, but Irf7 expression was affected. Thus, Reg1 suppresses type I IFN signaling restricting resistance to KP, suggesting that Reg1 could potentially be a target in severe bacterial infections. IMPORTANCE Klebsiella pneumoniae (KP) can cause life-threatening bacterial pneumonia and is the third most common cause of ventilator-associated pneumonia in the United States. Host inflammatory responses to infection are necessary to control disease, yet at the same time can cause collateral damage or immunopathology. During immune responses, many events are established within the infected tissue to limit unchecked inflammation. However, this restraint of immunity can impair infection control, and it is not fully understood how this balance is maintained during different infection settings. In this study we explored the possibility that a host-derived negative regulator of RNA, Regnase-1, limits immunity to KP by dampening inflammation. Indeed, mice with reduced Regnase-1 levels showed improved survival to KP infection, linked to regulation of type I interferons. Therefore, although restraint of Reg1 is beneficial to prevent immunopathology, temporary blockade of Reg1 could potentially be exploited to improve host defense during infectious settings such as KP.

Published

2022

4. The Globular C1q Receptor Is Required for Epidermal Growth Factor Receptor Signaling during Candida albicans Infection

Author

Quynh T. Phan, Jianfeng Lin, Norma V. Solis, Michael Eng, Marc Swidergall, Feng Wang, Shan Li, Sarah L. Gaffen, Tsui-Fen Chou, and Scott G. Filler

Subjects

Candida albicans, oral epithelial cells, endocytosis, epidermal growth factor receptor, host defense, Microbiology, QR1-502

Abstract

ABSTRACT During oropharyngeal candidiasis, Candida albicans activates the epidermal growth factor receptor (EGFR), which induces oral epithelial cells to endocytose the fungus and synthesize proinflammatory mediators. To elucidate EGFR signaling pathways that are stimulated by C. albicans, we used proteomics to identify 1,214 proteins that were associated with EGFR in C. albicans-infected cells. Seven of these proteins were selected for additional study. Among these proteins, WW domain-binding protein 2, Toll-interacting protein, interferon-induced transmembrane protein 3 (IFITM3), and the globular C1q receptor (gC1qR) were found to associate with EGFR in viable oral epithelial cells. Each of these proteins was required for maximal endocytosis of C. albicans, and all regulated fungus-induced production of interleukin-1β (IL-1β) and/or IL-8, either positively or negatively. gC1qR was found to function as a key coreceptor with EGFR. Interacting with the C. albicans Als3 invasin, gC1qR was required for the fungus to induce autophosphorylation of both EGFR and the ephrin type A receptor 2. The combination of gC1qR and EGFR was necessary for maximal endocytosis of C. albicans and secretion of IL-1β, IL-8, and granulocyte-macrophage colony-stimulating factor (GM-CSF) by human oral epithelial cells. In mouse oral epithelial cells, inhibition of gC1qR failed to block C. albicans-induced phosphorylation, and knockdown of IFITM3 did not inhibit C. albicans endocytosis, indicating that gC1qR and IFITM3 function differently in mouse versus human oral epithelial cells. Thus, this work provides an atlas of proteins that associate with EGFR and identifies several that play a central role in the response of human oral epithelial cells to C. albicans infection. IMPORTANCE Oral epithelial cells play a key role in the pathogenesis of oropharyngeal candidiasis. In addition to being target host cells for C. albicans adherence and invasion, they secrete proinflammatory cytokines and chemokines that recruit T cells and activated phagocytes to foci of infection. It is known that C. albicans activates EGFR on oral epithelial cells, which induces these cells to endocytose the organism and stimulates them to secrete proinflammatory mediators. To elucidate the EGFR signaling pathways that govern these responses, we analyzed the epithelial cell proteins that associate with EGFR in C. albicans-infected epithelial cells. We identified four proteins that physically associate with EGFR and that regulate different aspects of the epithelial response to C. albicans. One of these is gC1qR, which is required for C. albicans to activate EGFR, induce endocytosis, and stimulate the secretion of proinflammatory mediators, indicating that gC1qR functions as a key coreceptor with EGFR.

Published

2021

5. RTEC-intrinsic IL-17–driven inflammatory circuit amplifies antibody-induced glomerulonephritis and is constrained by Regnase-1

Author

De-Dong Li, Rami Bechara, Kritika Ramani, Chetan V. Jawale, Yang Li, Jay K. Kolls, Sarah L. Gaffen, and Partha S. Biswas

Subjects

Immunology, Inflammation, Medicine

Abstract

Antibody-mediated glomerulonephritis (AGN) is a clinical manifestation of many autoimmune kidney diseases for which few effective treatments exist. Chronic inflammatory circuits in renal glomerular and tubular cells lead to tissue damage in AGN. These cells are targeted by the cytokine IL-17, which has recently been shown to be a central driver of the pathogenesis of AGN. However, surprisingly little is known about the regulation of pathogenic IL-17 signaling in the kidney. Here, using a well-characterized mouse model of AGN, we show that IL-17 signaling in renal tubular epithelial cells (RTECs) is necessary for AGN development. We also show that Regnase-1, an RNA binding protein with endoribonuclease activity, is a negative regulator of IL-17 signaling in RTECs. Accordingly, mice with a selective Regnase-1 deficiency in RTECs exhibited exacerbated kidney dysfunction in AGN. Mechanistically, Regnase-1 inhibits IL-17–driven expression of the transcription factor IκBξ and, consequently, its downstream gene targets, including Il6 and Lcn2. Moreover, deletion of Regnase-1 in human RTECs reduced inflammatory gene expression in a IκBξ-dependent manner. Overall, these data identify an IL-17–driven inflammatory circuit in RTECs during AGN that is constrained by Regnase-1.

Published

2021

6. Candidalysin activates innate epithelial immune responses via epidermal growth factor receptor

Author

Jemima Ho, Xuexin Yang, Spyridoula-Angeliki Nikou, Nessim Kichik, Andrew Donkin, Nicole O. Ponde, Jonathan P. Richardson, Remi L. Gratacap, Linda S. Archambault, Christian P. Zwirner, Celia Murciano, Rhonda Henley-Smith, Selvam Thavaraj, Christopher J. Tynan, Sarah L. Gaffen, Bernhard Hube, Robert T. Wheeler, David L. Moyes, and Julian R. Naglik

Subjects

Science

Abstract

Candida albicans is an opportunistic fungus primarily affecting immunocompromised patients. Here, the authors identify a novel mechanism of host immune stimulation and highlight candidalysin and EGFR signalling components as potential targets for prophylactic and therapeutic intervention of mucosal candidiasis.

Published

2019

7. T Cell Receptor-Independent, CD31/IL-17A-Driven Inflammatory Axis Shapes Synovitis in Juvenile Idiopathic Arthritis

Author

Ian D. Ferguson, Patricia Griffin, Joshua J. Michel, Hiroshi Yano, Sarah L. Gaffen, Robert G. Mueller, Jeffrey A. Dvergsten, Jon D. Piganelli, Margalit E. Rosenkranz, Daniel A. Kietz, and Abbe N. Vallejo

Subjects

CD31, double negative alpha beta T cells, fibrocyte-like cells, IL-17, juvenile idiopathic arthritis, oxidoreductase, Immunologic diseases. Allergy, RC581-607

Abstract

T cells are considered autoimmune effectors in juvenile idiopathic arthritis (JIA), but the antigenic cause of arthritis remains elusive. Since T cells comprise a significant proportion of joint-infiltrating cells, we examined whether the environment in the joint could be shaped through the inflammatory activation by T cells that is independent of conventional TCR signaling. We focused on the analysis of synovial fluid (SF) collected from children with oligoarticular and rheumatoid factor-negative polyarticular JIA. Cytokine profiling of SF showed dominance of five molecules including IL-17A. Cytometric analysis of the same SF samples showed enrichment of αβT cells that lacked both CD4 and CD8 co-receptors [herein called double negative (DN) T cells] and also lacked the CD28 costimulatory receptor. However, these synovial αβT cells expressed high levels of CD31, an adhesion molecule that is normally employed by granulocytes when they transit to sites of injury. In receptor crosslinking assays, ligation of CD31 alone on synovial CD28nullCD31+ DN αβT cells effectively and sufficiently induced phosphorylation of signaling substrates and increased intracytoplasmic stores of cytokines including IL-17A. CD31 ligation was also sufficient to induce RORγT expression and trans-activation of the IL-17A promoter. In addition to T cells, SF contained fibrocyte-like cells (FLC) expressing IL-17 receptor A (IL-17RA) and CD38, a known ligand for CD31. Stimulation of FLC with IL-17A led to CD38 upregulation, and to production of cytokines and tissue-destructive molecules. Addition of an oxidoreductase analog to the bioassays suppressed the CD31-driven IL-17A production by T cells. It also suppressed the downstream IL-17A-mediated production of effectors by FLC. The levels of suppression of FLC effector activities by the oxidoreductase analog were comparable to those seen with corticosteroid and/or biologic inhibitors to IL-6 and TNFα. Collectively, our data suggest that activation of a CD31-driven, αβTCR-independent, IL-17A-mediated T cell-FLC inflammatory circuit drives and/or perpetuates synovitis. With the notable finding that the oxidoreductase mimic suppresses the effector activities of synovial CD31+CD28null αβT cells and IL-17RA+CD38+ FLC, this small molecule could be used to probe further the intricacies of this inflammatory circuit. Such bioactivities of this small molecule also provide rationale for new translational avenue(s) to potentially modulate JIA synovitis.

Published

2018

8. Processing of Candida albicans Ece1p Is Critical for Candidalysin Maturation and Fungal Virulence

Author

Jonathan P. Richardson, Selene Mogavero, David L. Moyes, Mariana Blagojevic, Thomas Krüger, Akash H. Verma, Bianca M. Coleman, Jacinto De La Cruz Diaz, Daniela Schulz, Nicole O. Ponde, Giulia Carrano, Olaf Kniemeyer, Duncan Wilson, Oliver Bader, Simona I. Enoiu, Jemima Ho, Nessim Kichik, Sarah L. Gaffen, Bernhard Hube, and Julian R. Naglik

Subjects

Candida albicans, candidalysin, fungal infection, kexin, mucosal immunity, Microbiology, QR1-502

Abstract

ABSTRACT Candida albicans is an opportunistic fungal pathogen responsible for superficial and life-threatening infections in humans. During mucosal infection, C. albicans undergoes a morphological transition from yeast to invasive filamentous hyphae that secrete candidalysin, a 31-amino-acid peptide toxin required for virulence. Candidalysin damages epithelial cell plasma membranes and stimulates the activating protein 1 (AP-1) transcription factor c-Fos (via p38–mitogen-activated protein kinase [MAPK]), and the MAPK phosphatase MKP1 (via extracellular signal-regulated kinases 1 and 2 [ERK1/2]–MAPK), which trigger and regulate proinflammatory cytokine responses, respectively. The candidalysin toxin resides as a discrete cryptic sequence within a larger 271-amino-acid parental preproprotein, Ece1p. Here, we demonstrate that kexin-like proteinases, but not secreted aspartyl proteinases, initiate a two-step posttranslational processing of Ece1p to produce candidalysin. Kex2p-mediated proteolysis of Ece1p after Arg61 and Arg93, but not after other processing sites within Ece1p, is required to generate immature candidalysin from Ece1p, followed by Kex1p-mediated removal of a carboxyl arginine residue to generate mature candidalysin. C. albicans strains harboring mutations of Arg61 and/or Arg93 did not secrete candidalysin, were unable to induce epithelial damage and inflammatory responses in vitro, and showed attenuated virulence in vivo in a murine model of oropharyngeal candidiasis. These observations identify enzymatic processing of C. albicans Ece1p by kexin-like proteinases as crucial steps required for candidalysin production and fungal pathogenicity. IMPORTANCE Candida albicans is an opportunistic fungal pathogen that causes mucosal infection in millions of individuals worldwide. Successful infection requires the secretion of candidalysin, the first cytolytic peptide toxin identified in any human fungal pathogen. Candidalysin is derived from its parent protein Ece1p. Here, we identify two key amino acids within Ece1p vital for processing and production of candidalysin. Mutations of these residues render C. albicans incapable of causing epithelial damage and markedly reduce mucosal infection in vivo. Importantly, candidalysin production requires two individual enzymatic events. The first involves processing of Ece1p by Kex2p, yielding immature candidalysin, which is then further processed by Kex1p to produce the mature toxin. These observations identify important steps for C. albicans pathogenicity at mucosal surfaces.

Published

2018

9. Neutrophils Do Not Express IL-17A in the Context of Acute Oropharyngeal Candidiasis

Author

Anna R. Huppler, Akash H. Verma, Heather R. Conti, and Sarah L. Gaffen

Subjects

IL-17, Th17, Candida albicans, neutrophils, fungal infection, oral candidiasis, innate lymphocyte, TCR, γδ-T cell, mice, Medicine

Abstract

IL-17 protects against pathogens by acting on nonhematopoietic cells to induce neutrophil recruitment through upregulation of chemokines and G-CSF. IL-17- and Th17-deficient humans and mice are susceptible to mucosal Candida albicans infections, linked to impaired neutrophil responses. IL-17 production is traditionally associated with CD4+ Th17 cells. However, IL-17 is also expressed during innate responses to facilitate rapid pathogen clearance. Innate IL-17-expressing cells include various lymphocyte-type subsets, including ILC3, NKT, γδ-T and “natural” Th17 (nTh17) cells. Some reports suggest that neutrophils can express IL-17 during fungal infections. Here, we asked whether neutrophils serve as a source of IL-17 during acute oropharyngeal candidiasis (OPC) using an IL-17A fate-tracking reporter mouse. Mice were subjected to OPC for two days, and oral tissue was analyzed by flow cytometry. IL-17A was expressed by γδ-T cells and TCRβ+ natural Th17 (nTh17) cells, as recently reported. Although infiltrating neutrophils were recruited to the tongue following infection, they did not express the IL-17A reporter. Moreover, neutrophil-depleted mice exhibited normal transcription of both Il17a and downstream IL-17-dependent gene targets after Candida challenge. Thus, in acute OPC, neutrophils are not a measurable source of IL-17 production, nor are they necessary to trigger IL-17-dependent gene expression, although they are essential for ultimate pathogen control.

Published

2015

10. The Aryl Hydrocarbon Receptor Governs Epithelial Cell Invasion during Oropharyngeal Candidiasis

Author

Norma V. Solis, Marc Swidergall, Vincent M. Bruno, Sarah L. Gaffen, and Scott G. Filler

Subjects

Candida albicans, aryl hydrocarbon receptor, epithelial cells, host cell invasion, interferon-gamma, Microbiology, QR1-502

Abstract

ABSTRACT Oropharyngeal candidiasis (OPC), caused predominantly by Candida albicans, is a prevalent infection in patients with advanced AIDS, defects in Th17 immunity, and head and neck cancer. A characteristic feature of OPC is fungal invasion of the oral epithelial cells. One mechanism by which C. albicans hyphae can invade oral epithelial cells is by expressing the Als3 and Ssa1 invasins that interact with the epidermal growth factor receptor (EGFR) on epithelial cells and stimulate endocytosis of the organism. However, the signaling pathways that function downstream of EGFR and mediate C. albicans endocytosis are poorly defined. Here, we report that C. albicans infection activates the aryl hydrocarbon receptor (AhR), leading to activation of Src family kinases (SFKs), which in turn phosphorylate EGFR and induce endocytosis of the fungus. Furthermore, treatment of oral epithelial cells with interferon gamma inhibits fungal endocytosis by inducing the synthesis of kynurenines, which cause prolonged activation of AhR and SFKs, thereby interfering with C. albicans-induced EGFR signaling. Treatment of both immunosuppressed and immunocompetent mice with an AhR inhibitor decreases phosphorylation of SFKs and EGFR in the oral mucosa, reduces fungal invasion, and lessens the severity of OPC. Thus, our data indicate that AhR plays a central role in governing the pathogenic interactions of C. albicans with oral epithelial cells during OPC and suggest that this receptor is a potential therapeutic target. IMPORTANCE OPC is caused predominantly by the fungus C. albicans, which can invade the oral epithelium by several mechanisms. One of these mechanisms is induced endocytosis, which is stimulated when fungal invasins bind to epithelial cell receptors such as EGFR. Receptor binding causes rearrangement of epithelial cell microfilaments, leading to the formation of pseudopods that engulf the fungus and pull it into the epithelial cell. We discovered AhR acts via SFKs to phosphorylate EGFR and induce the endocytosis of C. albicans. Our finding that a small molecule inhibitor of AhR ameliorates OPC in mice suggests that a strategy of targeting host cell signaling pathways that govern epithelial cell endocytosis of C. albicans holds promise as a new approach to preventing or treating OPC.

Published

2017

11. Empowering Women: Moving from Awareness to Action at the Immunology of Fungal Infections Gordon Research Conference

Author

Elizabeth R. Ballou, Sarah L. Gaffen, Neil A. R. Gow, and Amy G. Hise

Subjects

gender disparity, unconscious bias, women in science, women in medicine, Medicine

Abstract

Despite the high prevalence of women in graduate degree programs and equal or more women earning PhDs, MDs, and MD/PhDs, and despite efforts at individual and institutional levels to promote women in STEM fields, there remains a disparity in pay and academic advancement of women. Likewise, there is a paucity of women in top scientific and academic leadership positions. The causes of this gender disparity are complex and multi-factorial and to date no “magic bullet” approach has been successful in changing the landscape for women in academic and scientific fields. In this report we detail our experiences with a novel mechanism for promoting discussion and raising awareness of the challenges of gender disparity in the sciences. The Gordon Research Conferences (GRC) launched the Power Hour at its meetings in 2016: a dedicated, scheduled session held during the scientific meeting to facilitate discussion of challenges specific to women in science. Here we share our experience with hosting the second Power Hour at the 2019 GRC Immunology of Fungal Infections (IFI) meeting held in Galveston, TX. We will discuss the overall structure, key discussion points, and feedback from participants with the aim of supporting future efforts to empower women and underrepresented minority groups in science.

Published

2019

12. Innate Immunity to Mucosal Candida Infections

Author

Akash Verma, Sarah L. Gaffen, and Marc Swidergall

Subjects

oropharyngeal candidiasis, vulvovaginal candidiasis, epithelial cells, antimicrobial peptides, alarmins, IL-17, innate T cells, antifungal immunity, Biology (General), QH301-705.5

Abstract

Mucosal epithelial tissues are exposed to high numbers of microbes, including commensal fungi, and are able to distinguish between those that are avirulent and those that cause disease. Epithelial cells have evolved multiple mechanisms to defend against colonization and invasion by Candida species. The interplay between mucosal epithelial tissues and immune cells is key for control and clearance of fungal infections. Our understanding of the mucosal innate host defense system has expanded recently with new studies bringing to light the importance of epithelial cell responses, innate T cells, neutrophils, and other phagocytes during Candida infections. Epithelial tissues release cytokines, host defense peptides, and alarmins during Candida invasion that act in concert to limit fungal proliferation and recruit immune effector cells. The innate T cell/IL-17 axis and recruitment of neutrophils are of central importance in controlling mucosal fungal infections. Here, we review current knowledge of the innate immunity at sites of mucosal Candida infection, with a focus on infections caused by C. albicans.

Published

2017

13. When IL-17 gets on your nerves

Author

Iliyan D. Iliev, Woan-Yu Lin, and Sarah L. Gaffen

Subjects

General Biochemistry, Genetics and Molecular Biology

Published

2023

14. ‘(m6)A’ stands for ‘autoimmunity’: reading, writing, and erasing RNA modifications during inflammation

Author

Rami Bechara and Sarah L. Gaffen

Subjects

Inflammation, media_common.quotation_subject, Immunology, RNA, Autoimmunity, Context (language use), Autoimmune responses, Computational biology, Biology, medicine.disease_cause, Article, Functional diversity, Reading (process), Gene expression, medicine, Humans, Immunology and Allergy, RNA, Messenger, medicine.symptom, media_common

Abstract

Covalent modifications of RNA that regulate gene expression post-transcriptionally, in particular N6-methyladenosine (m(6)A), are emerging as important regulators of autoimmune responses. This article highlights new findings describing the functional diversity and specificity of m(6)A modifications and their regulation in the context of autoimmunity.

Published

2021

15. The Candida albicans toxin candidalysin mediates distinct epithelial inflammatory responses through p38 and EGFR-ERK pathways

Author

Spyridoula-Angeliki Nikou, Chunsheng Zhou, James S. Griffiths, Natalia K. Kotowicz, Bianca M. Coleman, Mary J. Green, David L. Moyes, Sarah L. Gaffen, Julian R. Naglik, and Peter J. Parker

Subjects

Cell Biology, Molecular Biology, Biochemistry

Abstract

The fungal pathogen Candida albicans secretes the peptide toxin candidalysin, which damages epithelial cells and drives an innate inflammatory response mediated by the epidermal growth factor receptor (EGFR) and mitogen-activated protein kinase (MAPK) pathways and the transcription factor c-Fos. In cultured oral epithelial cells, candidalysin activated the MAPK p38, which resulted in heat shock protein 27 (Hsp27) activation, IL-6 release, and EGFR phosphorylation without affecting the induction of c-Fos. p38 activation was not triggered by EGFR but by two nonredundant pathways involving MAPK kinases (MKKs) and the kinase Src, which differentially controlled p38 signaling outputs. Whereas MKKs mainly promoted p38-dependent release of IL-6, Src promoted p38-mediated phosphorylation of EGFR in a ligand-independent fashion. In parallel, candidalysin also activated the EGFR-ERK pathway in a ligand-dependent manner, resulting in c-Fos activation and release of the neutrophil-activating chemokines G-CSF and GM-CSF. In mice, early clearance events of oral C. albicans infection required p38 but not c-Fos. These findings delineate how candidalysin activates the pathways downstream of the MAPKs p38 and ERK that differentially contribute to immune activation during C. albicans infection.

Published

2022

16. The

Author

Spyridoula-Angeliki, Nikou, Chunsheng, Zhou, James S, Griffiths, Natalia K, Kotowicz, Bianca M, Coleman, Mary J, Green, David L, Moyes, Sarah L, Gaffen, Julian R, Naglik, and Peter J, Parker

Subjects

ErbB Receptors, Fungal Proteins, Mice, MAP Kinase Signaling System, Candida albicans, Animals, Phosphorylation, p38 Mitogen-Activated Protein Kinases

Abstract

The fungal pathogen

Published

2022

17. Fungal sensing enhances neutrophil metabolic fitness by regulating antifungal Glut1 activity

Author

De-Dong Li, Chetan V. Jawale, Chunsheng Zhou, Li Lin, Giraldina J. Trevejo-Nunez, Syed A. Rahman, Steven J. Mullet, Jishnu Das, Stacy G. Wendell, Greg M. Delgoffe, Michail S. Lionakis, Sarah L. Gaffen, and Partha S. Biswas

Subjects

CARD Signaling Adaptor Proteins, Glucose Transporter Type 1, Mice, beta-Glucans, Glucose, Neutrophils, Virology, Candida albicans, Candidiasis, Animals, Parasitology, Microbiology, Article

Abstract

Combating fungal pathogens poses metabolic challenges for neutrophils, key innate cells in anti-Candida albicans immunity, yet how host-pathogen interactions cause remodeling of the neutrophil metabolism is unclear. We show that neutrophils mediate renal immunity to disseminated candidiasis by upregulating glucose uptake via selective expression of glucose transporter 1 (Glut1). Mechanistically, dectin-1-mediated recognition of β-glucan leads to activation of PKCδ, which triggers phosphorylation, localization, and early glucose transport by a pool of pre-formed Glut1 in neutrophils. These events are followed by increased Glut1 gene transcription, leading to more sustained Glut1 accumulation, which is also dependent on the β-glucan/dectin-1/CARD9 axis. Card9-deficient neutrophils show diminished glucose incorporation in candidiasis. Neutrophil-specific Glut1-ablated mice exhibit increased mortality in candidiasis caused by compromised neutrophil phagocytosis, reactive oxygen species (ROS), and neutrophil extracellular trap (NET) formation. In human neutrophils, β-glucan triggers metabolic remodeling and enhances candidacidal function. Our data show that the host-pathogen interface increases glycolytic activity in neutrophils by regulating Glut1 expression, localization, and function.

Published

2022

18. Receptor-kinase EGFR-MAPK adaptor proteins mediate the epithelial response to Candida albicans via the cytolytic peptide toxin, candidalysin

Author

Nicole O. Ponde, Léa Lortal, Antzela Tsavou, Olivia W. Hepworth, Don N. Wickramasinghe, Jemima Ho, Jonathan P. Richardson, David L. Moyes, Sarah L. Gaffen, and Julian R. Naglik

Subjects

ErbB Receptors, Fungal Proteins, Shc Signaling Adaptor Proteins, Candidiasis, Oral, Candida albicans, Mouth Mucosa, Humans, Cytokines, Epithelial Cells, Cell Biology, Molecular Biology, Biochemistry

Abstract

Candida albicans (C. albicans) is a dimorphic commensal human fungal pathogen that can cause severe oropharyngeal candidiasis (oral thrush) in susceptible hosts. During invasive infection, C. albicans hyphae invade oral epithelial cells (OECs) and secrete candidalysin, a pore-forming cytolytic peptide that is required for C. albicans pathogenesis at mucosal surfaces. Candidalysin is produced in the hyphal invasion pocket and triggers cell damage responses in OECs. Candidalysin also activates multiple MAPK-based signaling events that collectively drive the production of downstream inflammatory mediators that coordinate downstream innate and adaptive immune responses. The activities of candidalysin are dependent on signaling through the epidermal growth factor receptor (EGFR). Here, we interrogated known EGFR-MAPK signaling intermediates for their roles mediating the OEC response to C. albicans infection. Using RNA silencing and pharmacological inhibition, we identified five key adaptors, including growth factor receptor-bound protein 2 (Grb2), Grb2-associated binding protein 1 (Gab1), Src homology and collagen (Shc), SH2-containing protein tyrosine phosphatase-2 (Shp2), and casitas B-lineage lymphoma (c-Cbl). We determined that all of these signaling effectors were inducibly phosphorylated in response to C. albicans. These phosphorylation events occurred in a candidalysin-dependent manner and additionally required EGFR phosphorylation, matrix metalloproteinases (MMPs), and cellular calcium flux to activate a complete OEC response to fungal infection. Of these, Gab1, Grb2, and Shp2 were the dominant drivers of ERK1/2 activation and the subsequent production of downstream innate-acting cytokines. Together, these results identify the key adaptor proteins that drive the EGFR signaling mechanisms that underlie oral epithelial responses to C. albicans.

Published

2022

19. EGFR-MAPK adaptor proteins mediate the epithelial response to Candida albicans via the cytolytic peptide toxin, candidalysin

Author

Nicole O. Ponde, Léa Lortal, Antzela Tsavou, Olivia W. Hepworth, Don N. Wickramansinghe, Jemima Ho, Jonathan P. Richardson, David L. Moyes, Sarah L. Gaffen, and Julian R. Naglik

Abstract

Candida albicans (C. albicans) is a dimorphic human fungal pathogen that can cause severe oropharyngeal candidiasis (OPC, oral thrush) in susceptible hosts. During invasive infection, C. albicans hyphae invade oral epithelial cells (OECs) and secrete candidalysin, a pore-forming cytolytic peptide that is required for fungal pathogenesis at mucosal surfaces. Candidalysin induces cell damage and activates multiple MAPK-based innate signaling events that collectively drive the production of downstream inflammatory mediators. The activities of candidalysin are also dependent on the epidermal growth factor receptor (EGFR), but how these signals are integrated is undefined. Here, we identified five essential adaptor proteins as key mediators of the epithelial response to C. albicans infection on cultured OECs, including growth factor receptor bound protein 2 (Grb2), Grb2-associated-binding protein 1 (Gab1), Src homology and collagen (Shc), SH2 containing protein tyrosine phosphatase-2 (Shp2) and casitas B-lineage lymphoma (c-Cbl). All these signaling effectors were inducibly phosphorylated in response to C. albicans, in a candidalysin-dependent mechanism but additionally required EGFR phosphorylation, matrix metalloproteinases (MMPs) and cellular calcium flux. Of these, Gab1, Grb2 and Shp2 were the dominant drivers of ERK1/2 signaling and production of downstream cytokines. Together, these results identify the key adaptor proteins that drive EGFR signaling mechanisms, which determine oral epithelial responses to C. albicans.

Published

2022

20. Arid5a mediates an IL-17-dependent pathway that drives autoimmunity but not antifungal host defense

Author

Tiffany C. Taylor, Yang Li, De-Dong Li, Saikat Majumder, Mandy J. McGeachy, Partha S. Biswas, Sebastien Gingras, and Sarah L. Gaffen

Subjects

Biological Products, Encephalomyelitis, Autoimmune, Experimental, Receptors, Interleukin-17, Immunology, Interleukin-17, Candidiasis, RNA-Binding Proteins, Autoimmunity, DNA-Binding Proteins, Mice, Immunology and Allergy, Animals, Humans, RNA, Messenger, Transcription Factors

Abstract

IL-17 contributes to the pathogenesis of certain autoimmune diseases, but conversely is essential for host defense against fungi. Antibody-based biologic drugs that neutralize IL-17 are effective in autoimmunity but can be accompanied by adverse side effects. Candida albicans is a commensal fungus that is the primary causative agent of oropharyngeal and disseminated candidiasis. Defects in IL-17 signaling cause susceptibility to candidiasis in mice and humans. A key facet of IL-17 receptor signaling involves RNA binding proteins (RBP), which orchestrate the fate of target mRNA transcripts. In tissue culture models we showed that the RBP AT-rich interacting protein 5a (Arid5a) promotes the stability and/or translation of multiple IL-17-dependent mRNAs. Moreover, during OPC, Arid5a is elevated within the oral mucosa in an IL-17-dependent manner. However, the contribution of Arid5a to IL-17-driven events in vivo is poorly defined. Here, we used CRISPR/Cas9 to generate mice lacking Arid5a. Arid5a-/- mice were fully resistant to experimental autoimmune encephalomyelitis (EAE), an autoimmune setting in which IL-17 signaling drives pathology. Surprisingly, Arid5a-/- mice were resistant to OPC and systemic candidiasis, similar to immunocompetent WT mice and contrasting with mice defective in IL-17 signaling. Therefore, Arid5a-dependent signals mediate pathology in autoimmunity yet are not required for immunity to candidiasis, indicating that selective targeting of IL-17 signaling pathway components may be a viable strategy for development of therapeutics that spare IL-17-driven host defense.

Published

2022

21. IL-17RA-signaling in Lgr5(+) intestinal stem cells induces expression of transcription factor ATOH1 to promote secretory cell lineage commitment

Author

Xun Lin, Stephen J. Gaudino, Kyung Ku Jang, Tej Bahadur, Ankita Singh, Anirban Banerjee, Michael Beaupre, Timothy Chu, Hoi Tong Wong, Chang-Kyung Kim, Cody Kempen, Jordan Axelrad, Huakang Huang, Saba Khalid, Vyom Shah, Onur Eskiocak, Olivia B. Parks, Artan Berisha, Jeremy P. McAleer, Misty Good, Miko Hoshino, Richard Blumberg, Agnieszka B. Bialkowska, Sarah L. Gaffen, Jay K. Kolls, Vincent W. Yang, Semir Beyaz, Ken Cadwell, and Pawan Kumar

Subjects

Mice, Knockout, Receptors, Interleukin-17, Stem Cells, Immunology, Dextran Sulfate, Interleukin-17, NF-kappa B, Cell Differentiation, SOX9 Transcription Factor, Cell Communication, Colitis, Article, Receptors, G-Protein-Coupled, Intestines, Mice, Infectious Diseases, Basic Helix-Loop-Helix Transcription Factors, Immunology and Allergy, Animals, Humans, Cell Lineage, Intestinal Mucosa, Signal Transduction

Abstract

The Th17 cell lineage-defining cytokine IL-17A contributes to host defense and inflammatory disease by coordinating multicellular immune responses. The IL-17 receptor (IL-17RA) is expressed by diverse intestinal cell types, and therapies targeting IL-17A induce adverse intestinal events, suggestive of additional tissue-specific functions. Here, we used multiple conditional deletion models to identify a role for IL-17A in secretory epithelial cell differentiation in the gut. Paneth, tuft, goblet, and enteroendocrine cell numbers were dependent on IL-17A-mediated induction of the transcription factor Atoh1 in Lgr5(+) intestinal epithelial stem cells. Although dispensable at steady state, IL-17RA signaling in ATOH1(+) cells was required to regenerate secretory cells following injury. Finally, IL-17A stimulation of human-derived intestinal organoids that were locked into a cystic immature state induced ATOH1 expression and rescued secretory cell differentiation. Our data suggest that the crosstalk between immune cells and stem cells regulates secretory cell lineage commitment and the integrity of the mucosa.

Published

2022

22. IL-17 receptor–based signaling and implications for disease

Author

Mandy J. McGeachy, Junjie Zhao, Sarah L. Gaffen, Rami Bechara, and Xiaoxia Li

Subjects

0301 basic medicine, medicine.medical_treatment, Immunology, Inflammation, Disease, Biology, Article, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, In vivo, Neoplasms, medicine, Animals, Humans, Immunology and Allergy, Receptor, Cells, Cultured, Receptors, Interleukin-7, Interleukin-17, Cancer, medicine.disease, 030104 developmental biology, Cytokine, Immune System Diseases, Signal transduction, medicine.symptom, Neuroscience, Signal Transduction, 030215 immunology

Abstract

IL-17 is a highly versatile pro-inflammatory cytokine crucial for a variety of processes, including host defense, tissue repair, the pathogenesis of inflammatory disease and the progression of cancer. In contrast to its profound impact in vivo, IL-17 exhibits surprisingly moderate activity in cell-culture models, which presents a major knowledge gap about the molecular mechanisms of IL-17 signaling. Emerging studies are revealing a new dimension of complexity in the IL-17 pathway that may help explain its potent and diverse in vivo functions. Discoveries of new mRNA stabilizers and receptor-directed mRNA metabolism have provided insights into the means by which IL-17 cooperates functionally with other stimuli in driving inflammation, whether beneficial or destructive. The integration of IL-17 with growth-receptor signaling in specific cell types offers new understanding of the mitogenic effect of IL-17 on tissue repair and cancer. This Review summarizes new developments in IL-17 signaling and their pathophysiological implications.

Published

2019

23. The Globular C1q Receptor Is Required for Epidermal Growth Factor Receptor Signaling during Candida albicans Infection

Author

Jianfeng Lin, Feng Wang, Scott G. Filler, Sarah L. Gaffen, Shan Li, Michael Eng, Norma V. Solis, Marc Swidergall, Quynh T Phan, Tsui-Fen Chou, and Alspaugh, J Andrew

Subjects

Oral, Chemokine, 1.1 Normal biological development and functioning, Complement, Endocytosis, Microbiology, Proinflammatory cytokine, Mice, Underpinning research, Candidiasis, Oral, Virology, Receptors, Candida albicans, 2.2 Factors relating to the physical environment, 2.1 Biological and endogenous factors, Animals, Humans, endocytosis, Secretion, Epidermal growth factor receptor, Dental/Oral and Craniofacial Disease, Aetiology, Receptor, Inbred BALB C, Mice, Inbred BALB C, Membrane Glycoproteins, biology, Candidiasis, Epithelial Cells, biology.organism_classification, Corpus albicans, QR1-502, Cell biology, Receptors, Complement, ErbB Receptors, oral epithelial cells, Infectious Diseases, host defense, biology.protein, NIH 3T3 Cells, Infection, epidermal growth factor receptor, Protein Binding, Signal Transduction, Research Article

Abstract

During oropharyngeal candidiasis, Candida albicans activates the epidermal growth factor receptor (EGFR), which induces oral epithelial cells to endocytose the fungus and synthesize proinflammatory mediators. To elucidate EGFR signaling pathways that are stimulated by C. albicans, we used proteomics to identify 1,214 proteins that were associated with EGFR in C. albicans-infected cells. Seven of these proteins were selected for additional study. Among these proteins, WW domain-binding protein 2, Toll-interacting protein, interferon-induced transmembrane protein 3 (IFITM3), and the globular C1q receptor (gC1qR) were found to associate with EGFR in viable oral epithelial cells. Each of these proteins was required for maximal endocytosis of C. albicans, and all regulated fungus-induced production of interleukin-1β (IL-1β) and/or IL-8, either positively or negatively. gC1qR was found to function as a key coreceptor with EGFR. Interacting with the C. albicans Als3 invasin, gC1qR was required for the fungus to induce autophosphorylation of both EGFR and the ephrin type A receptor 2. The combination of gC1qR and EGFR was necessary for maximal endocytosis of C. albicans and secretion of IL-1β, IL-8, and granulocyte-macrophage colony-stimulating factor (GM-CSF) by human oral epithelial cells. In mouse oral epithelial cells, inhibition of gC1qR failed to block C. albicans-induced phosphorylation, and knockdown of IFITM3 did not inhibit C. albicans endocytosis, indicating that gC1qR and IFITM3 function differently in mouse versus human oral epithelial cells. Thus, this work provides an atlas of proteins that associate with EGFR and identifies several that play a central role in the response of human oral epithelial cells to C. albicans infection. IMPORTANCE Oral epithelial cells play a key role in the pathogenesis of oropharyngeal candidiasis. In addition to being target host cells for C. albicans adherence and invasion, they secrete proinflammatory cytokines and chemokines that recruit T cells and activated phagocytes to foci of infection. It is known that C. albicans activates EGFR on oral epithelial cells, which induces these cells to endocytose the organism and stimulates them to secrete proinflammatory mediators. To elucidate the EGFR signaling pathways that govern these responses, we analyzed the epithelial cell proteins that associate with EGFR in C. albicans-infected epithelial cells. We identified four proteins that physically associate with EGFR and that regulate different aspects of the epithelial response to C. albicans. One of these is gC1qR, which is required for C. albicans to activate EGFR, induce endocytosis, and stimulate the secretion of proinflammatory mediators, indicating that gC1qR functions as a key coreceptor with EGFR.

Published

2021

24. Regnase-1 deficiency restrains Klebsiella pneumoniae infection by regulation of a Type I interferon response

Author

Giraldina Trevejo-Nunez, Kong Chen, Felix E. Y. Aggor, Becky Lin, Partha S. Biswas, Li Fan, and Sarah L. Gaffen

Subjects

Messenger RNA, Regulator, RNA-binding protein, Inflammation, Biology, Microbiology, Interferon, Immunity, Virology, Klebsiella, Immunology, medicine, IRF7, Regnase, RNA binding proteins, Signal transduction, medicine.symptom, Research Article, medicine.drug

Abstract

Excessive inflammatory responses can cause collateral tissue damage or autoimmune inflammation, sometimes with severe morbidity or mortality. During host defense responses, numerous negative feedback mechanisms are established to prevent excessive unchecked inflammation. However, this restraint can sometimes come at the cost of suboptimal infection control, and we do not fully understand how this balance is maintained during different infection settings. The endoribonuclease Regnase-1 (Reg1, Zc3h12a, MCPIP1) is an RNA binding protein (RBP) that binds and degrades many target mRNA transcripts. Reg1 is a potent feedback regulator of IL-17 and LPS signal transduction, among other stimuli. Consequently, Reg1 deficiency exacerbates autoimmune inflammation in multiple mouse models, but on the other hand, reduced Reg1 improves immunity to fungal infection. To date, the role of Reg1 in bacterial immunity is poorly defined. Here, we show that mice deficient in Reg1 are more resistant to pulmonary Klebsiella pneumoniae (KP) infection. Unexpectedly, effects of Reg1 deficiency were not due to accelerated eradication of bacteria or increased pro-inflammatory cytokine expression. Rather, alveolar macrophages from Reg1-deficient mice showed enrichment of Type I IFN-related genes upon KP infection, accompanied by increased Ifnb1 expression. Surprisingly, the stability of Ifnb1 mRNA was not altered by Reg1-deficiency; rather, mRNA encoding its upstream regulator IRF7 appeared to be a more prominent target. Blockade of IFNR during KP infection reversed disease improvement. Thus, impaired Reg1 induces Type I IFN and enhances resistance to KP, raising the possibility that Reg1 could be a potential clinical target in acute bacterial infections.Graphical abstract

Published

2021

25. The m 6 A reader IMP2 directs autoimmune inflammation through an IL-17– and TNFα-dependent C/EBP transcription factor axis

Author

Nandan S. Gokhale, Sarah L. Gaffen, Rami Bechara, Nilesh Amatya, Stacy M. Horner, Yang Li, Rachel D. Bailey, Bianca M. Coleman, Partha S. Biswas, Felix E. Y. Aggor, Chetan V. Jawale, Ning Dai, Anita Bansal, Tiffany C. Taylor, Amanda C. Poholek, and De-Dong Li

Subjects

0301 basic medicine, Messenger RNA, Chemistry, Effector, MRNA modification, Immunology, General Medicine, MRNA stabilization, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Enhancer binding, CEBPB, Tumor necrosis factor alpha, Transcription factor

Abstract

Excessive cytokine activity underlies many autoimmune conditions, particularly through the interleukin-17 (IL-17) and tumor necrosis factor-α (TNFα) signaling axis. Both cytokines activate nuclear factor κB, but appropriate induction of downstream effector genes requires coordinated activation of other transcription factors, notably, CCAAT/enhancer binding proteins (C/EBPs). Here, we demonstrate the unexpected involvement of a posttranscriptional "epitranscriptomic" mRNA modification [N6-methyladenosine (m6A)] in regulating C/EBPβ and C/EBPδ in response to IL-17A, as well as IL-17F and TNFα. Prompted by the observation that C/EBPβ/δ-encoding transcripts contain m6A consensus sites, we show that Cebpd and Cebpb mRNAs are subject to m6A modification. Induction of C/EBPs is enhanced by an m6A methylase "writer" and suppressed by a demethylase "eraser." The only m6A "reader" found to be involved in this pathway was IGF2BP2 (IMP2), and IMP2 occupancy of Cebpd and Cebpb mRNA was enhanced by m6A modification. IMP2 facilitated IL-17-mediated Cebpd mRNA stabilization and promoted translation of C/EBPβ/δ in response to IL-17A, IL-17F, and TNFα. RNA sequencing revealed transcriptome-wide IL-17-induced transcripts that are IMP2 influenced, and RNA immunoprecipitation sequencing identified the subset of mRNAs that are directly occupied by IMP2, which included Cebpb and Cebpd Lipocalin-2 (Lcn2), a hallmark of autoimmune kidney injury, was strongly dependent on IL-17, IMP2, and C/EBPβ/δ. Imp2-/- mice were resistant to autoantibody-induced glomerulonephritis (AGN), showing impaired renal expression of C/EBPs and Lcn2 Moreover, IMP2 deletion initiated only after AGN onset ameliorated disease. Thus, posttranscriptional regulation of C/EBPs through m6A/IMP2 represents a previously unidentified paradigm of cytokine-driven autoimmune inflammation.

Published

2021

26. RTEC-intrinsic IL-17–driven inflammatory circuit amplifies antibody-induced glomerulonephritis and is constrained by Regnase-1

Author

Rami Bechara, Jay K. Kolls, Kritika Ramani, Partha S. Biswas, Chetan V. Jawale, Yang Li, Sarah L. Gaffen, and De-Dong Li

Subjects

Autoimmune diseases, medicine.medical_treatment, Endoribonuclease activity, Immunology, Inflammation, Biology, Mice, Glomerulonephritis, Ribonucleases, Proto-Oncogene Proteins, medicine, Animals, Renal Insufficiency, Transcription factor, Innate immunity, Kidney, Innate immune system, Interleukin-17, Epithelial Cells, General Medicine, medicine.disease, Immunity, Innate, Kidney Tubules, Cytokine, medicine.anatomical_structure, Cancer research, Cytokines, I-kappa B Proteins, Interleukin 17, medicine.symptom, Research Article, Signal Transduction

Abstract

Antibody-mediated glomerulonephritis (AGN) is a clinical manifestation of many autoimmune kidney diseases for which few effective treatments exist. Chronic inflammatory circuits in renal glomerular and tubular cells lead to tissue damage in AGN. These cells are targeted by the cytokine IL-17, which has recently been shown to be a central driver of the pathogenesis of AGN. However, surprisingly little is known about the regulation of pathogenic IL-17 signaling in the kidney. Here, using a well-characterized mouse model of AGN, we show that IL-17 signaling in renal tubular epithelial cells (RTECs) is necessary for AGN development. We also show that Regnase-1, an RNA binding protein with endoribonuclease activity, is a negative regulator of IL-17 signaling in RTECs. Accordingly, mice with a selective Regnase-1 deficiency in RTECs exhibited exacerbated kidney dysfunction in AGN. Mechanistically, Regnase-1 inhibits IL-17-driven expression of the transcription factor IκBξ and, consequently, its downstream gene targets, including Il6 and Lcn2. Moreover, deletion of Regnase-1 in human RTECs reduced inflammatory gene expression in a IκBξ-dependent manner. Overall, these data identify an IL-17-driven inflammatory circuit in RTECs during AGN that is constrained by Regnase-1.

Published

2021

27. The globular C1q receptor is required for epidermal growth factor receptor signaling during Candida albicans infection

Author

Quynh T Phan, Marc Swidergall, Michael Eng, Jianfeng Lin, Tsui-Fen Chou, Norma V. Solis, Shan Li, Feng Wang, Sarah L. Gaffen, and Scott G. Filler

Subjects

Chemokine, Immune system, biology, biology.protein, Ephrin, Secretion, Signal transduction, Candida albicans, biology.organism_classification, Corpus albicans, Proinflammatory cytokine, Cell biology

Abstract

During oropharyngeal candidiasis, Candida albicans activates the epidermal growth factor receptor (EGFR), which induces oral epithelial cells to both endocytose the fungus and synthesize proinflammatory mediators that orchestrate the host immune response. To elucidate the signaling pathways that are stimulated when C. albicans interacts with EGFR, we analyzed the proteins that associate with EGFR when C. albicans infects human oral epithelial cells. We identified 1214 proteins that were associated with EGFR in C. albicans-infected cells. We investigated the function of seven of these proteins that either showed increased association with EGFR in response to C. albicans or that mediated the interaction of other microbial pathogens with epithelial cells. Among these proteins, EGFR was found to associate with WW domain-binding protein 2, toll-interacting protein, interferon-induced transmembrane protein 3, and the globular C1q receptor (gC1qR) in viable epithelial cells. Each of these proteins was required for maximal endocytosis of C. albicans and they all regulated fungal-induced production of IL-1β and/or IL-8, either positively or negatively. gC1qR functioned as a key coreceptor with EGFR. Interacting with the C. albicans Als3 invasin, gC1qR was required for the fungus to stimulate both EGFR and the ephrin type-A receptor 2. The combination of gC1qR and EGFR was necessary for maximal endocytosis of C. albicans and secretion of IL-1β, IL-8, and GM-CSF. Thus, this work provides an atlas of proteins that associate with EGFR and identifies several that play a central role in the response of human oral epithelial cells to C. albicans infection.IMPORTANCEOral epithelial cells play a key role in the pathogenesis of oropharyngeal candidiasis. In addition to being target host cells for C. albicans adherence and invasion, they secrete proinflammatory cytokines and chemokines that recruit T cells and activated phagocytes to foci of infection. It is known that C. albicans activates EGFR on oral epithelial cells, which induces these cells to endocytose the organism and stimulates them to secrete proinflammatory mediators. To elucidate the EGFR signaling pathways that govern these responses, we analyzed the epithelial cell proteins that associate with EGFR in C. albicans-infected epithelial cells. We identified four proteins that physically associate with EGFR and that regulate different aspects of the epithelial response to C. albicans. One of these is gC1qR, which is required for C. albicans to activate EGFR, induce endocytosis, and stimulate the secretion of proinflammatory mediators, indicating that gC1qR functions as a key co-receptor with EGFR.

Published

2021

28. IL-17 metabolically reprograms activated fibroblastic reticular cells for proliferation and survival

Author

Natalie Rittenhouse, Shankar Revu, Saikat Majumder, Fang Du, Sarah L. Gaffen, Ashley V. Menk, Ulrich Siebenlist, Timothy W. Hand, Chetan V. Jawale, Dongwen Wu, Mandy J. McGeachy, Itay Raphael, Nilesh Amatya, Amanda C. Poholek, Greg M. Delgoffe, Saran Kupul, Partha S. Biswas, and Amrita Bhattacharjee

Subjects

0301 basic medicine, Chemokine, Stromal cell, biology, Chemistry, medicine.medical_treatment, Immunology, Germinal center, Inflammation, Acquired immune system, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Cytokine, Reticular cell, biology.protein, medicine, Immunology and Allergy, Interleukin 17, medicine.symptom, 030215 immunology

Abstract

Lymph-node (LN) stromal cell populations expand during the inflammation that accompanies T cell activation. Interleukin-17 (IL-17)-producing helper T cells (TH17 cells) promote inflammation through the induction of cytokines and chemokines in peripheral tissues. We demonstrate a critical requirement for IL-17 in the proliferation of LN and splenic stromal cells, particularly fibroblastic reticular cells (FRCs), during experimental autoimmune encephalomyelitis and colitis. Without signaling via the IL-17 receptor, activated FRCs underwent cell cycle arrest and apoptosis, accompanied by signs of nutrient stress in vivo. IL-17 signaling in FRCs was not required for the development of TH17 cells, but failed FRC proliferation impaired germinal center formation and antigen-specific antibody production. Induction of the transcriptional co-activator IκBζ via IL-17 signaling mediated increased glucose uptake and expression of the gene Cpt1a, encoding CPT1A, a rate-limiting enzyme of mitochondrial fatty acid oxidation. Hence, IL-17 produced by locally differentiating TH17 cells is an important driver of the activation of inflamed LN stromal cells, through metabolic reprogramming required to support proliferation and survival. Fibroblastic reticular cells support lymph-node function and adaptive immunity. McGeachy and colleagues show that the cytokine IL-17 is needed to trigger metabolic changes required for the proliferation and survival of these cells in reactive lymph nodes.

Published

2019

29. The IL-17 Family of Cytokines in Health and Disease

Author

Daniel J. Cua, Sarah L. Gaffen, and Mandy J. McGeachy

Subjects

0301 basic medicine, Immunology, Context (language use), Inflammation, Disease, Biology, Infections, Article, Autoimmune Diseases, Mice, 03 medical and health sciences, 0302 clinical medicine, Stress, Physiological, Neoplasms, medicine, Animals, Humans, Immunology and Allergy, Molecular Targeted Therapy, Regulation of gene expression, Autoimmune disease, Receptors, Interleukin-17, Interleukin-17, Brain, RNA-Binding Proteins, T-Lymphocytes, Helper-Inducer, medicine.disease, IL 17 family, 030104 developmental biology, Infectious Diseases, Gene Expression Regulation, 030220 oncology & carcinogenesis, Cytokines, Wounds and Injuries, Interleukin 17, medicine.symptom, Signal transduction, Signal Transduction

Abstract

The interleukin 17 (IL-17) family of cytokines contains 6 structurally related cytokines, IL-17A through IL-17F. IL-17A, the prototypical member of this family, just passed the 25th anniversary of its discovery. Although less is known about IL-17B–F, IL-17A (commonly known as IL-17) has received much attention for its pro-inflammatory role in autoimmune disease. Over the past decade, however, it has become clear that the functions of IL-17 are far more nuanced than simply turning on inflammation. Accumulating evidence indicates that IL-17 has important context- and tissue-dependent roles in maintaining health during response to injury, physiological stress, and infection. Here, we discuss the functions of the IL-17 family, with a focus on the balance between the pathogenic and protective roles of IL-17 in cancer and autoimmune disease, including results of therapeutic blockade and novel aspects of IL-17 signal transduction regulation.

Published

2019

30. Th17-driven immunity to oral candidiasis is dependent on the microbiome and can be triggered by mono-colonization with segmented filamentous bacteria

Author

Felix E.Y. Aggor, Chunsheng Zhou, Darryl Abbott, Javonn Musgrove, Vincent Bruno, Timothy W. Hand, and Sarah L. Gaffen

Subjects

Immunology, Immunology and Allergy

Abstract

The opportunistic infection oropharyngeal candidiasis (OPC; oral thrush) is a common oral infection among the immunocompromised. The oral cavity is a major entry portal to the body and oral health impacts several aspects of host immunity. While much is now known about microbiome dependent Th17 induction and protection against intestinal candidiasis and other Th17 driven responses, our understanding of the role of the microbiome in oral Th17 induction and oral antifungal immunity is rather rudimentary. We demonstrate a direct role for the microbiome in triggering protection against OPC. While wildtype (WT) mice raised under specific pathogen free (SPF) conditions are resistant to OPC, WT germ free (GF) mice succumbed to infection. Reconstitution of WT-GF mice with segmented filamentous bacteria (SFB) was sufficient to restore protection against OPC with associated increase in Th17 cells, neutrophils, and antimicrobial responses in the oral mucosa. Thus, SFB mono-colonization in WT-GF mice triggers oral mucosal Th17 induction to protect against oral thrush and reveals a role of the microbiome in promoting oral mucosal immunity. Supported by R37-DE022550

Published

2022

31. Antibody-induced glomerulonephritis is amplified by RTEC-intrinsic IL-17 signaling and restrained by IL-17-mediated induction of the endoribonuclease Regnase-1 (Zc3h12a)

Author

Rami Bechara, Sarah L. Gaffen, Yang Li, Jay K. Kolls, Kritika Ramani, Partha S. Biswas, Chetan V. Jawale, and De-Dong Li

Subjects

Kidney, Chemistry, medicine.medical_treatment, Endoribonuclease activity, RNA-binding protein, Glomerulonephritis, medicine.disease, Cell biology, Pathogenesis, Cytokine, medicine.anatomical_structure, medicine, Interleukin 17, Transcription factor

Abstract

Antibody-mediated glomerulonephritis (AGN) is a clinical manifestation of many autoimmune kidney diseases for which few effective treatments exist. Chronic inflammatory circuits in renal glomerular and tubular cells lead to tissue damage in AGN. These cells are targeted by the cytokine IL-17, which has recently been shown to be a central driver of the pathogenesis of AGN. However, surprisingly little is known about the regulation of pathogenic IL-17 signaling in the kidney. Here, using a well characterized mouse model of AGN, we show that IL-17 signaling in renal tubular epithelial cells (RTECs) is necessary for AGN development. We also show that Regnase-1, an RNA binding protein with endoribonuclease activity, is a negative regulator of IL-17 signaling in RTECs. Accordingly, mice with a selective Regnase-1 deficiency in RTECs exhibited exacerbated kidney dysfunction in AGN. Mechanistically, Regnase-1 inhibits IL-17-driven expression of the transcription factor IκBξ and consequently its downstream gene targets including Il6 and Lcn2. Moreover, deletion of Regnase-1 in human RTECs reduced inflammatory gene expression in an IκBξ-dependent manner. Overall, these data identify an IL-17-driven inflammatory circuit in RTECs during AGN that is constrained by Regnase-1.

Published

2021

32. Infections in the monogenic autoimmune syndrome APECED

Author

Vasileios Oikonomou, Niki M. Moutsopoulos, Timothy J. Break, Sarah L. Gaffen, and Michail S. Lionakis

Subjects

animal structures, T-Lymphocytes, Immunology, Autoimmunity, Candidiasis, Cutaneous, medicine.disease_cause, Article, Sepsis, Immune Tolerance, medicine, Animals, Humans, Immunology and Allergy, Chronic mucocutaneous candidiasis, Clonal Selection, Antigen-Mediated, Polyendocrinopathies, Autoimmune, business.industry, Autoantibody, Bacterial pneumonia, COVID-19, medicine.disease, Autoimmune regulator, Bronchiectasis, Pneumonia, Disease Susceptibility, Central tolerance, business, Transcription Factors

Abstract

Autoimmune polyendocrinopathy-candidiasis-ectodermal dystrophy (APECED) is caused by mutations in the Autoimmune Regulator (AIRE) gene, which impair the thymic negative selection of self-reactive T-cells and underlie the development of autoimmunity that targets multiple endocrine and non-endocrine tissues. Beyond autoimmunity, APECED features heightened susceptibility to certain specific infections, which is mediated by anti-cytokine autoantibodies and/or T-cell driven autoimmune tissue injury. These include the 'signature' APECED infection chronic mucocutaneous candidiasis (CMC), but also life-threatening coronavirus disease 2019 (COVID-19) pneumonia, bronchiectasis-associated bacterial pneumonia, and sepsis by encapsulated bacteria. Here we discuss the expanding understanding of the immunological mechanisms that contribute to infection susceptibility in this prototypic syndrome of impaired central tolerance, which provide the foundation for devising improved diagnostic and therapeutic strategies for affected patients.

Published

2021

33. Local sustained delivery of anti-IL-17A antibodies limits inflammatory bone loss in murine experimental periodontitis

Author

Laura L. Thomas, Zhe Zhuang, Sarah L. Gaffen, Steven R. Little, Cinthia M F Pacheco, Mostafa S. Shehabeldin, Gustavo Pompermaier Garlet, Sayuri Yoshizawa, Konstantinos Verdelis, Charles Sfeir, and Katia L M Maltos

Subjects

Male, Drug Compounding, medicine.medical_treatment, Immunology, Alveolar Bone Loss, Capsules, Inflammation, Osteolysis, Bone resorption, Pathogenesis, Mice, 03 medical and health sciences, Drug Delivery Systems, 0302 clinical medicine, Immune system, Polylactic Acid-Polyglycolic Acid Copolymer, medicine, Animals, Immunology and Allergy, Periodontitis, Dental alveolus, REABSORÇÃO ÓSSEA ALVEOLAR, Mice, Inbred BALB C, business.industry, Interleukin-17, OSSO E OSSOS, Periodontium, medicine.disease, Antibodies, Neutralizing, Disease Models, Animal, Drug Liberation, Treatment Outcome, Cytokine, medicine.symptom, business, 030215 immunology

Abstract

Periodontal disease (PD) is a chronic destructive inflammatory disease of the tooth-supporting structures that leads to tooth loss at its advanced stages. Although the disease is initiated by a complex organization of oral microorganisms in the form of a plaque biofilm, it is the uncontrolled immune response to periodontal pathogens that fuels periodontal tissue destruction. IL-17A has been identified as a key cytokine in the pathogenesis of PD. Despite its well documented role in host defense against invading pathogens at oral barrier sites, IL-17A–mediated signaling can also lead to a detrimental inflammatory response, causing periodontal bone destruction. In this study, we developed a local sustained delivery system that restrains IL-17A hyperactivity in periodontal tissues by incorporating neutralizing anti–IL-17A Abs in poly(lactic-coglycolic) acid microparticles (MP). This formulation allowed for controlled release of anti–IL-17A in the periodontium of mice with ligature-induced PD. Local delivery of anti–IL-17A MP after murine PD induction inhibited alveolar bone loss and osteoclastic activity. The anti–IL-17A MP formulation also decreased expression of IL-6, an IL-17A target gene known to induce bone resorption in periodontal tissues. This study demonstrates proof of concept that local and sustained release of IL-17A Abs constitutes a promising therapeutic strategy for PD and may be applicable to other osteolytic bone diseases mediated by IL-17A–driven inflammation.

Published

2021

34. The metabolism-modulating activity of IL-17 signaling in health and disease

Author

Sarah L. Gaffen, Rami Bechara, and Mandy J. McGeachy

Subjects

0301 basic medicine, medicine.medical_treatment, Immunology, Innate Immunity and Inflammation, Autoimmunity, Disease, Review, Biology, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, medicine, Immunology and Allergy, Pathogenic aspects, Animals, Humans, Cell Proliferation, Interleukin-17, Epithelial Cells, Metabolism, 030104 developmental biology, Cytokine, Glucose, Metabolic regulation, Gene Expression Regulation, Interleukin 17, Signal transduction, Neuroscience, Glycolysis, Function (biology), 030215 immunology, Signal Transduction

Abstract

This review highlights the emergent role of the cytokine IL-17 in orchestrating cellular and organismal metabolism. Metabolism is thereby integrated into the protective and pathogenic aspects of IL-17 responses in a temporally and spatially regulated manner., IL-17 was discovered nearly 30 yr ago, but it has only been recently appreciated that a key function of this cytokine is to orchestrate cellular and organismal metabolism. Indeed, metabolic regulation is integrated into both the physiological and the pathogenic aspects of IL-17 responses. Thus, understanding the interplay between IL-17 and downstream metabolic processes could ultimately inform therapeutic opportunities for diseases involving IL-17, including some not traditionally linked to this cytokine pathway. Here, we discuss the emerging pathophysiological roles of IL-17 related to cellular and organismal metabolism, including metabolic regulation of IL-17 signal transduction.

Published

2020

35. An IL-17F.S65L knockin mouse reveals similarities and differences in IL-17F function in oral candidiasis: A new tool to understand IL-17F

Author

Chunsheng Zhou, Sarah L. Gaffen, Leticia Monin, Rami Bechara, Rachael A. Gordon, Tara N. Edwards, Felix E. Y. Aggor, Sebastien Gingras, and Daniel H. Kaplan

Subjects

medicine.medical_treatment, Immunology, Mutant, Mutation, Missense, Mice, Transgenic, Biology, medicine.disease_cause, Oropharyngeal Candidiasis, Article, Mice, Candida albicans, medicine, Immunology and Allergy, Animals, Gene Knock-In Techniques, Chronic mucocutaneous candidiasis, Phenocopy, Mutation, Interleukin-17, Candidiasis, biology.organism_classification, medicine.disease, Cytokine, IL17A, Mouth Diseases

Abstract

Oropharyngeal candidiasis (OPC) is an opportunistic infection of the oral mucosa caused by the commensal fungus Candida albicans. IL-17R signaling is essential to prevent OPC in mice and humans, but the individual roles of its ligands, IL-17A, IL-17F, and IL-17AF, are less clear. A homozygous IL-17F deficiency in mice does not cause OPC susceptibility, whereas mice lacking IL-17A are moderately susceptible. In humans, a rare heterozygous mutation in IL-17F (IL-17F.S65L) was identified that causes chronic mucocutaneous candidiasis, suggesting the existence of essential antifungal pathways mediated by IL-17F and/or IL-17AF. To investigate the role of IL-17F and IL-17AF in more detail, we exploited this “experiment of nature” by creating a mouse line bearing the homologous mutation in IL-17F (Ser65Leu) by CRISPR/Cas9. Unlike Il17f−/− mice that are resistant to OPC, Il17fS65L/S65L mice showed increased oral fungal burdens similar to Il17a−/− mice. In contrast to humans, however, disease was only evident in homozygous, not heterozygous, mutant mice. The mutation was linked to modestly impaired CXC chemokine expression and neutrophil recruitment to the infected tongue but not to alterations in oral antimicrobial peptide expression. These findings suggest mechanisms by which the enigmatic cytokine IL-17F contributes to host defense against fungi. Moreover, because these mice do not phenocopy Il17f−/− mice, they may provide a valuable tool to interrogate IL-17F and IL-17AF function in vivo in other settings.

Published

2020

36. Restoring glucose uptake rescues neutrophil dysfunction and protects against systemic fungal infection in mouse models of kidney disease

Author

Thomas D. Nolin, Saran Kupul, Michail S. Lionakis, Jigar V. Desai, Chetan V. Jawale, Sarah L. Gaffen, Partha S. Biswas, Bianca M. Coleman, De-Dong Li, Filitsa H. Bender, Li Lin, Greg M. Delgoffe, Alexander J. Prokopienko, Kritika Ramani, and Rohan S. Oberoi

Subjects

0301 basic medicine, biology, business.industry, Glucose uptake, Renal function, General Medicine, medicine.disease, biology.organism_classification, Disseminated Candidiasis, Uremia, Corpus albicans, Nephrotoxicity, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Immunology, medicine, business, Candida albicans, 030217 neurology & neurosurgery, Kidney disease

Abstract

Disseminated candidiasis caused by the fungus Candida albicans is a major clinical problem in individuals with kidney disease and accompanying uremia; disseminated candidiasis fatality is twice as common in patients with uremia as those with normal kidney function. Many antifungal drugs are nephrotoxic, making treatment of these patients particularly challenging. The underlying basis for this impaired capacity to control infections in uremic individuals is poorly understood. Here, we show in multiple models that uremic mice exhibit an increased susceptibility to systemic fungal infection. Uremia inhibits Glut1-mediated uptake of glucose in neutrophils by causing aberrant activation of GSK3β, resulting in reduced ROS generation and hence impaired killing of C. albicans in mice. Consequently, pharmacological inhibition of GSK3β restored glucose uptake and rescued ROS production and candidacidal function of neutrophils in uremic mice. Similarly, neutrophils isolated from patients with kidney disease and undergoing hemodialysis showed similar defect in the fungal killing activity, a phenotype rescued in the presence of a GSK3β inhibitor. These findings reveal a mechanism of neutrophil dysfunction during uremia and suggest a potentially translatable therapeutic avenue for treatment of disseminated candidiasis.

Published

2020

37. The m

Author

Rami, Bechara, Nilesh, Amatya, Rachel D, Bailey, Yang, Li, Felix E Y, Aggor, De-Dong, Li, Chetan V, Jawale, Bianca M, Coleman, Ning, Dai, Nandan S, Gokhale, Tiffany C, Taylor, Stacy M, Horner, Amanda C, Poholek, Anita, Bansal, Partha S, Biswas, and Sarah L, Gaffen

Subjects

Inflammation, Male, Mice, Knockout, Adenosine, Tumor Necrosis Factor-alpha, Interleukin-17, RNA-Binding Proteins, Autoimmunity, Article, Cell Line, Mice, Inbred C57BL, CCAAT-Enhancer-Binding Proteins, Animals, Humans, Female

Abstract

Excessive cytokine activity underlies many autoimmune conditions, particularly through the IL-17 and TNFα signaling axes. Both cytokines activate NF-κB, but appropriate induction of downstream effector genes requires coordinated activation of other transcription factors, notably CCAAT/Enhancer Binding Proteins (C/EBPs). Here we demonstrate the unexpected involvement of a post-transcriptional ‘epitranscriptomic’ mRNA modification (N6-methyladenosine, m(6)A) in regulating C/EBPβ and C/EBPδ in response to IL-17A, as well as IL-17F and TNFα. Prompted by the observation that C/EBPβ/δ-encoding transcripts contain m(6)A consensus sites, we show that Cebpd and Cebpb mRNAs are subject to m(6)A modification. Induction of C/EBPs is enhanced by an m(6)A methylase ‘writer’ and suppressed by a demethylase ‘eraser.’ The only m(6)A ‘reader’ found to be involved in this pathway was IGF2BP2 (IMP2), and IMP2 occupancy of Cebpd and Cebpb mRNA was enhanced by m(6)A modification. IMP2 facilitated IL-17-mediated Cebpd mRNA stabilization and promoted translation of C/EBPβ/δ in response to IL-17A, IL-17F and TNFα. RNASeq revealed transcriptome-wide IL-17-induced transcripts that are IMP2-influenced, and RIPSeq identified the subset of mRNAs that are directly occupied by IMP2, which included Cebpb and Cebpd. Lipocalin-2 (Lcn2), a hallmark of autoimmune kidney injury, was strongly dependent on IL-17, IMP2 and C/EBPβ/δ. Indeed, Imp2(−/−) mice were resistant to autoantibody-induced glomerulonephritis (AGN), showing impaired renal expression of C/EBPs and Lcn2. Moreover, IMP2 deletion initiated only after AGN onset ameliorated disease. Thus, post-transcriptional regulation of C/EBPs through m(6)A/IMP2 represents a new paradigm of cytokine-driven autoimmune inflammation.

Published

2020

38. A loss-of-function mutation in IL-17F enhances susceptibility of mice to oropharyngeal candidiasis

Author

Leticia Monin, Rami Bechara, Chunsheng Zhou, Felix E. Y. Aggor, Tara N. Edwards, Daniel H. Kaplan, Sebastien Gingras, Sarah L. Gaffen, and Rachael A. Gordon

Subjects

0303 health sciences, Mutation, Opportunistic infection, medicine.medical_treatment, Mutant, Biology, medicine.disease, medicine.disease_cause, Oropharyngeal Candidiasis, Corpus albicans, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Cytokine, Homologous chromosome, medicine, Chronic mucocutaneous candidiasis, 030304 developmental biology, 030215 immunology

Abstract

Oropharyngeal candidiasis (OPC) is an opportunistic infection of the oral mucosa caused by the commensal fungusC. albicans. IL-17 receptor signaling is essential to prevent OPC in mice and humans, but the individual roles of its ligands, IL-17A, IL-17F and IL-17AF, are less clear. A homozygous IL-17F deficiency in mice does not cause OPC susceptibility, whereas mice lacking IL-17A are moderately susceptible. In humans, a rare heterozygous mutation in IL-17F (IL-17F.S65L) was identified that causes chronic mucocutaneous candidiasis, suggesting the existence of essential antifungal pathways mediated by IL-17F and/or IL-17AF. To investigate the role of IL-17F and IL-17AF in more detail, we exploited this ‘experiment of nature’ by creating a mouse line bearing the homologous mutation in IL-17F (Ser65Leu) by CRISPR/Cas9.The resultingIl17fS65L/S65Lmice showed increased susceptibility to OPC, but only in homozygous, not heterozygous, mutant mice. The mutation was linked to impaired CXC chemokine expression and neutrophil recruitment to the infected tongue but not to alterations in antimicrobial peptide expression. These findings suggest mechanisms by which the enigmatic cytokine IL-17F contributes to host defense against fungi.

Published

2020

39. Extracellular ATP released from Candida albicans activates non-peptidergic neurons to augment host defense

Author

bernard hube, Selene Mogavero, Brian M. Davis, Jonathan Cohen, Judith Berman, Paul Yifan Zhou, Shiqun Zhang, h richard koeber, marie-elizabeth bougnoux, Sarah L. Gaffen, Kathryn M. Albers, Daniel H. Kaplan, Alicia R. Mathers, Andrew Liu, Tara N. Edwards, and Christophe d'Enfert

Subjects

0303 health sciences, biology, Apyrase, Chemistry, P2RX7, biology.organism_classification, Corpus albicans, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Immune system, Extracellular, Secretion, Candida albicans, 030217 neurology & neurosurgery, Intracellular, 030304 developmental biology

Abstract

Intestinal microbes release ATP to modulate local immune responses. Herein we demonstrates that Candida albicans, an opportunistic commensal fungus, also modulates immune responses via secretion of ATP. We found that ATP secretion from C. albicans varied between standard laboratory strains. A survey of eighty-nine clinical isolates revealed heterogeneity in ATP secretion, independent of growth kinetics and intracellular ATP levels. Isolates from blood released less ATP than commensals, suggesting that ATP secretion assists with commensalism. To confirm this, cohorts of mice were infected with strains matched for origin, and intracellular ATP concentration, but high or low extracellular ATP. In all cases fungal burden was inversely correlated with ATP secretion. Mice lacking P2RX7, the key ATP receptor expressed by immune cells in the skin, showed no alteration in fungal burden. Rather, treatments with a P2RX2/3 antagonist result in increased fungal burden. P2RX2/3 is expressed by non-peptidergic neurons that terminate in the epidermis. Cultured sensory neurons flux Ca2+ when exposed to supernatant from heat-killed C. albicans (HKCA), and these non-peptidergic fibers are the dominant subset that respond to HKCA. Ca2+ flux, but not CGRP-release, can be abrogated by pretreatment of HKCA supernatant with apyrase. To determine whether non-peptidergic neurons participate in host defense, we generated MRGPRD-DTR mice. Infection in these mice resulted in increased CFU only for those C. albicans strains with high ATP secretion. Taken together, our findings indicate that C. albicans releases ATP, which is recognized by non-peptidergic nerves in the skin resulting in augmented anti-Candida immune responses.Author SummaryBacterial release of ATP has been shown to modulate immune responses. Candida albicans displays heterogeneity in ATP release among laboratory strains and commensal clinical isolates release more ATP than invasive isolates. C. albicans strains with high ATP secretion show lower fungal burden following epicutaneous infection. Mice lacking P2RX7, the key ATP receptor expressed by immune cells, showed no alteration in fungal burden. In contrast, treatment with P2RX2/3 antagonists resulted in increased fungal burden. P2RX3 is expressed by a subset of non-peptidergic neurons that terminate in the epidermis. These non-peptidergic fibers are the predominant responders when cultured sensory neurons are exposed to heat-killed C. albicans in vitro. Mice lacking non-peptidergic neurons have increased infection when exposed to high but not low ATP-secreting isolates of C. albicans. Taken together, our findings indicate that C. albicans releases ATP which is recognized by non-peptidergic nerves in the skin resulting in augmented anti-Candida immune responses.Bullet pointsATP released from heat killed C. albicans activates non-peptidergic sensory neuronsLive C. albicans clinical isolates release variable amounts of ATPElevated levels of ATP released by C. albicans correlates with reduced infectivity in vivoMRGPRD-expressing cutaneous neurons are required for defense against ATP-secreting C. albicans

Published

2020

40. Regulation of host-microbe interactions at oral mucosal barriers by type 17 immunity

Author

Sarah L. Gaffen and Niki M. Moutsopoulos

Subjects

0301 basic medicine, T cell, Immunology, Inflammation, Article, Oropharyngeal Candidiasis, 03 medical and health sciences, 0302 clinical medicine, Immunity, medicine, Animals, Humans, Oral mucosa, Candida albicans, Immunity, Mucosal, Periodontitis, biology, business.industry, Microbiota, Interleukin-17, Mouth Mucosa, General Medicine, medicine.disease, biology.organism_classification, stomatognathic diseases, 030104 developmental biology, medicine.anatomical_structure, Host-Pathogen Interactions, Th17 Cells, Oral Microbiome, medicine.symptom, Mouth Diseases, business, 030215 immunology

Abstract

The oral mucosa is a primary barrier site and a portal for entry of microbes, food, and airborne particles into the gastrointestinal tract. Nonetheless, mucosal immunity at this barrier remains understudied compared with other anatomical barrier sites. Here, we review basic aspects of oral mucosal histology, the oral microbiome, and common and clinically significant diseases that present at oral mucosal barriers. We particularly focus on the role of interleukin-17 (IL-17)/T helper 17 (TH17) responses in protective immunity and inflammation in the oral mucosa. IL-17/TH17 responses are highly relevant to maintaining barrier integrity and preventing pathogenic infections by the oral commensal fungus Candida albicans On the other hand, aberrant IL-17/TH17 responses are implicated in driving the pathogenesis of periodontitis and consequent bone and tooth loss. We discuss distinct IL-17-secreting T cell subsets, emphasizing their regulation and function in oropharyngeal candidiasis and periodontitis.

Published

2020

41. IL-36 and IL-1/IL-17 Drive Immunity to Oral Candidiasis via Parallel Mechanisms

Author

David L. Moyes, Julian R. Naglik, Jonathan P. Richardson, Sarah L. Gaffen, Diksha Sihra, J. Ho, Bianca M. Coleman, Felix E. Y. Aggor, Martin Stacey, Akash H. Verma, Olivia W. Hepworth, Joseph S. Ainscough, Bernhard Hube, Hanna Zafar, Nicole O. Ponde, and Mandy J. McGeachy

Subjects

0301 basic medicine, medicine.medical_treatment, Immunology, Biology, Interleukin-23, p38 Mitogen-Activated Protein Kinases, Article, Cell Line, Fungal Proteins, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunity, Candida albicans, medicine, Animals, Immunology and Allergy, Adaptor Proteins, Signal Transducing, Mice, Knockout, Regulation of gene expression, Interleukin-17, Candidiasis, Mouth Mucosa, Receptors, Interleukin-1, biology.organism_classification, Immunity, Innate, Corpus albicans, Mice, Inbred C57BL, 030104 developmental biology, Cytokine, Gene Expression Regulation, Alternative complement pathway, Candidalysin, Interleukin-1, Signal Transduction, 030215 immunology

Abstract

Protection against microbial infection by the induction of inflammation is a key function of the IL-1 superfamily, including both classical IL-1 and the new IL-36 cytokine families. Candida albicans is a frequent human fungal pathogen causing mucosal infections. Although the initiators and effectors important in protective host responses to C. albicans are well described, the key players in driving these responses remain poorly defined. Recent work has identified a central role played by IL-1 in inducing innate Type-17 immune responses to clear C. albicans infections. Despite this, lack of IL-1 signaling does not result in complete loss of immunity, indicating that there are other factors involved in mediating protection to this fungus. In this study, we identify IL-36 cytokines as a new player in these responses. We show that C. albicans infection of the oral mucosa induces the production of IL-36. As with IL-1α/β, induction of epithelial IL-36 depends on the hypha-associated peptide toxin Candidalysin. Epithelial IL-36 gene expression requires p38-MAPK/c-Fos, NF-κB, and PI3K signaling and is regulated by the MAPK phosphatase MKP1. Oral candidiasis in IL-36R−/− mice shows increased fungal burdens and reduced IL-23 gene expression, indicating a key role played by IL-36 and IL-23 in innate protective responses to this fungus. Strikingly, we observed no impact on gene expression of IL-17 or IL-17–dependent genes, indicating that this protection occurs via an alternative pathway to IL-1–driven immunity. Thus, IL-1 and IL-36 represent parallel epithelial cell–driven protective pathways in immunity to oral C. albicans infection.

Published

2018

42. The Interleukin (IL) 17R/IL-22R Signaling Axis Is Dispensable for Vulvovaginal Candidiasis Regardless of Estrogen Status

Author

Felix E. Y. Aggor, Sarah L. Gaffen, Srinivas Bishu, Bianca M. Coleman, Vincent M. Bruno, Anna H Huppler, Brian M. Peters, Ellyse M Cipolla, Akash H. Verma, Katherine S. Barker, and Hubertine M. E. Willems

Subjects

0301 basic medicine, medicine.drug_class, 030106 microbiology, Oropharyngeal Candidiasis, Interleukin 22, 03 medical and health sciences, Mice, Major Articles and Brief Reports, Candidiasis, Oral, Immunopathology, Candida albicans, medicine, Immunology and Allergy, Animals, Candidiasis, Vulvovaginal, Vaginitis, Mucous Membrane, Receptors, Interleukin-17, biology, business.industry, Interleukin-17, Interleukin, Estrogens, Receptors, Interleukin, biology.organism_classification, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Infectious Diseases, Estrogen, Immunology, Vagina, Female, Interleukin 17, business, Signal Transduction

Abstract

Candida albicans, a ubiquitous commensal fungus that colonizes human mucosal tissues and skin, can become pathogenic, clinically manifesting most commonly as oropharyngeal candidiasis and vulvovaginal candidiasis (VVC). Studies in mice and humans convincingly show that T-helper 17 (Th17)/interleukin 17 (IL-17)–driven immunity is essential to control oral and dermal candidiasis. However, the role of the IL-17 pathway during VVC remains controversial, with conflicting reports from human data and mouse models. Like others, we observed induction of a strong IL-17–related gene signature in the vagina during estrogen-dependent murine VVC. As estrogen increases susceptibility to vaginal colonization and resulting immunopathology, we asked whether estrogen use in the standard VVC model masks a role for the Th17/IL-17 axis. We demonstrate that mice lacking IL-17RA, Act1, or interleukin 22 showed no evidence for altered VVC susceptibility or immunopathology, regardless of estrogen administration. Hence, these data support the emerging consensus that Th17/IL-17 axis signaling is dispensable for the immunopathogenesis of VVC.

Published

2019

43. Fungus Among Us: The Frenemies Within

Author

Felix E. Y. Aggor, Sing Sing Way, and Sarah L. Gaffen

Subjects

0301 basic medicine, Cellular differentiation, Immunology, Heterologous, chemical and pharmacologic phenomena, Fungus, Microbiology, Aspergillus fumigatus, 03 medical and health sciences, 0302 clinical medicine, Antigen, Immunity, Candida albicans, Humans, Immunology and Allergy, Inflammation, biology, fungi, Cell Differentiation, biology.organism_classification, Corpus albicans, 030104 developmental biology, Th17 Cells, 030215 immunology

Abstract

A recent study shows that the commensal fungus Candida albicans is an inducer of differentiation of human CD4+ Th17 cells that harbor heterologous specificity for other fungi, which may explain evolutionary benefits of C. albicans as a commensal microbe (Bacher et al. Cell 2019;176;1340–1355). However, Th17 cells that are crossreactive to Aspergillus fumigatus antigens can also drive exaggerated airway inflammation in humans.

Published

2019

44. Oral mucosal IL-22/STAT3 signaling licenses IL-17-mediated immunity to oral candidiasis

Author

Felix E.Y. Aggor, Timothy Break, Giraldina Trevejo-Nunez, Natasha Whibley, Rachel D. Bailey, Daniel H Kaplan, Julian R. Naglik, Wei Shan, Amol C. Shetty, Carrie McCracken, Scott K. Durum, Partha S. Biswas, Vincent M. Bruno, Jay K Kolls, Michail S Lionakis, and Sarah L. Gaffen

Subjects

Immunology, Immunology and Allergy

Abstract

Oropharyngeal candidiasis (OPC) is an opportunistic infection of the oral mucosa caused by the commensal fungus Candida albicans. IL-17 and IL-22 both mediate antifungal immunity yet activate distinct downstream signaling pathways. While much is known about IL-17-dependent immunity in OPC, the activities of IL-22 are less well delineated. We show that induction of Il22 is independent of Dectin-1, CARD9 and aryl hydrocarbon receptor (AhR) and is driven by IL-23 and the C. albicans pore forming peptide candidalysin. Despite similar induction requirements and cellular sources, IL-22 and IL-17 function non-redundantly during OPC and exert opposing roles in neutrophil recruitment. The IL-22 and IL-17 receptors are required in anatomically distinct locations; loss of IL-22RA1 in the oral basal epithelial layer (BEL) but not the suprabasal epithelial layer (SEL) causes susceptibility to OPC, whereas IL-17RA is needed in the SEL. Our data reveal that IL-22 is a major activator of STAT3 in the BEL during OPC. Moreover, loss of STAT3 in the BEL but not the SEL renders mice susceptible to OPC. Transcriptional profiling of RNASeq data linked IL-22/STAT3 to oral epithelial cell proliferation and survival, but also, unexpectedly, to driving an IL-17 gene signature. We show that IL-22 acts on the BEL to replenish the IL-17RA-expressing SEL, thereby restoring the ability of the oral epithelium to respond to IL-17. Consequently, IL-22 signaling in BEL ‘licenses’ IL-17R signaling in the oral epithelium, revealing spatially distinct yet cooperative activities of IL-22 and IL-17 in oral candidiasis. This work also suggests that oral thrush in Jobs’ syndrome patients may be caused by STAT3 impairments in the oral epithelium, not just Th17 cells.

Published

2021

45. RNA m6A methylation guides IL-17-driven autoimmunity through IMP2-dependent regulation of C/EBP transcription factors

Author

Rami Bechara, Nilesh Amatya, Rachel D. Bailey, Yang Li, Felix EY Aggor, De-Dong Li, Chetan V. Jawale, Bianca M. Coleman, Ning Dai, Nandan S. Gokhale, Tiffany C. Taylor, Stacy M. Horner, Amanda C. Poholek, Partha S. Biswas, and Sarah L. Gaffen

Subjects

Immunology, Immunology and Allergy

Abstract

Dysregulated activity of IL-17 underlies many autoimmune conditions, but the molecular mechanisms by which IL-17 mediates pathogenic inflammation remain poorly understood. IL-17 regulates pathogenic inflammatory genes by two key transcription factor classes, NF-κB and CCAAT/Enhancer Binding (C/EBP) proteins. Surprisingly little is known about mechanisms that activate C/EBPs. In seeking to understand how IL-17 upregulates C/EBPs, we found that IL-17 signaling enhanced Cebpd mRNA stability, concomitant with increased levels of C/EBPδ translation. In contrast, IL-17 had only a marginal inductive effect on Cebpb mRNA, yet C/EBPβ protein was strongly upregulated. Examination of Cebpb and Cebpd noncoding sequences identified consensus sites for N6-methyladenosine (m6A) modification, an epitranscriptomic mark that influences mRNA fate. knockdown of the m6A ‘writer’ METTL3 decreased C/EBP expression, which was reversed by the ‘eraser’ FTO. Moreover, we found that loss of an unusual m6A ‘reader’ IGF2BP2 (IMP2), an RNA binding protein known to control mRNA stability, impaired IL-17 induction of C/EBPs. IMP2 bound directly to Cebps transcripts, leading to enhanced Cebpd half-life and enhanced translation of both C/EBPs. Transcriptomic analysis revealed that IMP2 regulates C/EBP-dependent genes, including IL-6 and Lcn2. Lcn2 is a biomarker of autoantibody-induced glomerulonephritis (AGN), a setting of IL-17-driven inflammatory nephritis. Imp2−/− mice were resistant to AGN, which was linked to impaired upregulation of C/EPBs and Lcn2 in kidney. Thus, IL-17-induced autoimmunity is mediated through m6A-dependent post-transcriptional regulation of C/EBP transcription factors.

Published

2021

46. IL-17 Signaling Triggers Degradation of the Constitutive NF-κB Inhibitor ABIN-1

Author

Brian J. Aneskievich, Rudi Beyaert, Sarah L. Gaffen, Lawrence P. Kane, Nilesh Amatya, Erin E. Childs, Abhishek V. Garg, J. Agustin Cruz, and Averil Ma

Subjects

Cell signaling, biology, Immunology, Biology and Life Sciences, NF-κB, General Medicine, Molecular biology, TNFAIP3, Proinflammatory cytokine, Cell biology, chemistry.chemical_compound, Ubiquitin, chemistry, Medicine and Health Sciences, biology.protein, Immunology and Allergy, SOCS5, SOCS6, Interleukin 17

Abstract

IL-17 activates NF-κB and induces expression of proinflammatory genes. IL-17 drives disease in autoimmune conditions, and anti–IL-17 Abs have shown impressive success in the clinic. Although produced by lymphocytes, IL-17 predominantly signals in fibroblasts and epithelial cells. IL-17–driven inflammation is kept in check by negative feedback signaling molecules, including the ubiquitin editing enzyme A20, whose gene TNFAIP3 is linked to autoimmune disease susceptibility. The A20 binding inhibitor of NF-κB activation 1 (ABIN-1) is an A20-binding protein encoded by the TNIP1 gene, which is also linked to autoimmune disease susceptibility including psoriasis. Accordingly, we hypothesized that ABIN-1 might play a role in negatively regulating IL-17 signaling activity. Indeed, ABIN-1 enhanced both tonic and IL-17–dependent NF-κB signaling in IL-17–responsive fibroblast cells. Interestingly, the inhibitory activities of ABIN-1 on IL-17 signaling were independent of A20. ABIN-1 is a known NF-κB target gene, and we found that IL-17–induced activation of NF-κB led to enhanced ABIN-1 mRNA expression and promoter activity. Surprisingly, however, the ABIN-1 protein was inducibly degraded following IL-17 signaling in a proteasome-dependent manner. Thus, ABIN-1, acting independently of A20, restricts both baseline and IL-17–induced inflammatory gene expression. We conclude that IL-17–induced signals lead to degradation of ABIN-1, thereby releasing a constitutive cellular brake on NF-κB activation.

Published

2017

47. Follistatin‐like protein 1 modulates IL‐17 signaling via IL‐17RC regulation in stromal cells

Author

Taylor Eddens, Raphael Hirsch, Jay K. Kolls, Sarah L. Gaffen, William Horne, Yury Chaly, Martin Majewski, Matthew Henkel, and Brian T. Campfield

Subjects

0301 basic medicine, Follistatin-Related Proteins, Stromal cell, RNA Stability, medicine.medical_treatment, Immunology, Article, Embryo Culture Techniques, Gene Knockout Techniques, Mice, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Immunology and Allergy, SOCS5, SOCS6, RNA, Messenger, RNA, Small Interfering, Cells, Cultured, Oligonucleotide Array Sequence Analysis, Inflammation, Regulation of gene expression, biology, Microarray analysis techniques, Interleukin-17, Mesenchymal Stem Cells, Receptors, Interleukin, Cell Biology, 3. Good health, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, Cytokine, Gene Expression Regulation, biology.protein, Signal transduction, Signal Transduction, 030215 immunology, Follistatin

Abstract

Follistatin-like protein 1 (FSTL-1) possesses several newly identified roles in mammalian biology, including autoimmunity and IL-17 driven inflammation, though the mechanism underlying FSTL-1 influence on IL-17 mediated cytokine production is unknown. To examine the role of FSTL-1 in IL-17 signaling, we utilized parallel in vitro bone marrow stromal cell models of FSTL-1 attenuation. Microarray identified FSTL-1 regulated genes that could influence IL-17 dependent production of IL-6 and G-CSF, wherein we discovered that FSTL-1 modulates Il17rc gene expression. Specifically, FSTL-1 was necessary for Il17rc gene transcription, IL-17RC surface protein expression and IL-17-dependent cytokine production. In FSTL-1 KO BMSCs, ectopic Il17rc expression rescued IL-17 stimulated cytokine, and ectopic Fstl1 expression rescued Il17rc expression as well as IL-17 stimulated cytokines. Mechanisms influencing FSTL-1 dependent Il17rc transcript abundance were examined using Actinomycin D and nascent mRNA labeling approaches and identified that FSTL-1 regulates Il17rc gene transcription. Taken together, this work identifies a mechanism by which FSTL-1 influences IL-17 driven inflammation and reveals a novel function for FSTL-1 as a modulator of gene expression. Thus, enhanced understanding of the interplay between FSTL-1 and IL-17 mediated inflammation may provide insight into potential therapeutic targets of IL-17 mediated diseases.

Published

2017

48. IL-17 Signaling: The Yin and the Yang

Author

Abhishek V. Garg, Sarah L. Gaffen, and Nilesh Amatya

Subjects

0301 basic medicine, Immunology, Biology, Article, Autoimmune Diseases, Proinflammatory cytokine, 03 medical and health sciences, 0302 clinical medicine, Immunopathology, medicine, Animals, Humans, Immunology and Allergy, Inflammatory genes, Autoimmune disease, Interleukin-17, Models, Immunological, Interleukin, Cancer, medicine.disease, 030104 developmental biology, Gene Expression Regulation, Cytokines, Interleukin 17, Inflammation Mediators, Signal transduction, Signal Transduction, 030215 immunology

Abstract

Interleukin (IL)-17 is the founding member of a novel family of inflammatory cytokines. While the proinflammatory properties of IL-17 are key to its host-protective capacity, unrestrained IL-17 signaling is associated with immunopathology, autoimmune disease, and cancer progression. In this review we discuss both the activators and the inhibitors of IL-17 signal transduction, and also the physiological implications of these events. We highlight the surprisingly diverse means by which these regulators control expression of IL-17-dependent inflammatory genes, as well as the major target cells that respond to IL-17 signaling.

Published

2017

49. CCAAT/Enhancer-binding protein β promotes pathogenesis of EAE

Author

Amanda C. Poholek, Michelle R. Simpson-Abelson, Ansuman Chattopadhyay, Sarah L. Gaffen, Mandy J. McGeachy, J. Agustin Cruz, Gerard Hernandez-Mir, and Erin E. Childs

Subjects

0301 basic medicine, Encephalomyelitis, Autoimmune, Experimental, medicine.medical_treatment, T cell, Immunology, Cell, Biology, Biochemistry, Article, Mice, 03 medical and health sciences, Enhancer binding, medicine, Animals, Immunology and Allergy, Molecular Biology, Transcription factor, Mice, Knockout, Ccaat-enhancer-binding proteins, CCAAT-Enhancer-Binding Protein-beta, Dendritic Cells, Receptors, Interleukin, Hematology, Molecular biology, 030104 developmental biology, medicine.anatomical_structure, Cytokine, Gene Expression Regulation, Cytokines, Th17 Cells, Interleukin 17, Cell activation

Abstract

The CCAAT/Enhancer Binding Protein β (C/EBPβ) transcription factor is activated by multiple inflammatory stimuli, including IL-17 and LPS, and C/EBPβ itself regulates numerous genes involved in inflammation. However, the role of C/EBPβ in driving autoimmunity is not well understood. Here, we demonstrate that Cebpb−/− mice are resistant to EAE. Cebpb−/− mice exhibited reduced lymphocyte and APC infiltration into CNS following EAE induction. Furthermore, MOG-induced Th17 cytokine production was impaired in draining LN, indicating defects in Th17 cell priming. In vitro Th17 polarization studies indicated that T cell responses are not inherently defective, instead supporting the known roles for C/EBPβ in myeloid lineage cell activation as the likely mechanism for defective Th17 priming in vivo. However, we did uncover an unexpected role for C/EBPβ in regulating ll23r expression in APCs. ChIP assays confirmed that C/EBPβ binds directly to the Il23r gene promoter in dendritic cells and Th17 cells. These data establish C/EBPβ as a key driver of autoimmune inflammation in EAE, and propose a novel role for C/EBPβ in regulation of IL-23R expression.

Published

2017

50. MCPIP1/Regnase-1 Restricts IL-17A– and IL-17C–Dependent Skin Inflammation

Author

Eerin E. Childs, Nilesh Amatya, Sarah L. Gaffen, Abhishek V. Garg, Johann E. Gudjonsson, Bianca M. Coleman, Nicole L. Ward, Akash H. Verma, Alicia R. Mathers, Leticia Monin, Xianying Xing, and Meaghan E. Killeen

Subjects

0301 basic medicine, medicine.diagnostic_test, Immunology, Inflammation, Imiquimod, Stimulation, Biology, medicine.disease, Flow cytometry, Pathogenesis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Downregulation and upregulation, Psoriasis, medicine, Immunology and Allergy, Immunohistochemistry, medicine.symptom, 030215 immunology, medicine.drug

Abstract

The IL-17 family cytokines IL-17A and IL-17C drive the pathogenesis of psoriatic skin inflammation, and anti–IL-17A Abs were recently approved to treat human psoriasis. Little is known about mechanisms that restrain IL-17 cytokine-mediated signaling, particularly IL-17C. In this article, we show that the endoribonuclease MCP-1–induced protein 1 (MCPIP1; also known as regnase-1) is markedly upregulated in human psoriatic skin lesions. Similarly, MCPIP1 was overexpressed in the imiquimod (IMQ)-driven mouse model of cutaneous inflammation. Mice with an MCPIP1 deficiency (Zc3h12a+/−) displayed no baseline skin inflammation, but they showed exacerbated pathology following IMQ treatment. Pathology in Zc3h12a+/− mice was associated with elevated expression of IL-17A– and IL-17C–dependent genes, as well as with increased accumulation of neutrophils in skin. However, IL-17A and IL-17C expression was unaltered, suggesting that the increased inflammation in Zc3h12a+/− mice was due to enhanced downstream IL-17R signaling. Radiation chimeras demonstrated that MCPIP1 in nonhematopoietic cells is responsible for controlling skin pathology. Moreover, Zc3h12a+/−Il17ra−/− mice given IMQ showed almost no disease. To identify which IL-17RA ligand was essential, Zc3h12a+/−Il17a−/− and Zc3h12a+/−Il17c−/− mice were given IMQ; these mice had reduced but not fully abrogated pathology, indicating that MCPIP1 inhibits IL-17A and IL-17C signaling. Confirming this hypothesis, Zc3h12a−/− keratinocytes showed increased responsiveness to IL-17A and IL-17C stimulation. Thus, MCPIP1 is a potent negative regulator of psoriatic skin inflammation through IL-17A and IL-17C. Moreover, to our knowledge, MCPIP1 is the first described negative regulator of IL-17C signaling.

Published

2017