Your search keyword '"Scott W. Canna"' showing total 61 results

1. Mortality Risk in Pediatric Sepsis Based on C-reactive Protein and Ferritin Levels

Author

Christopher M, Horvat, Anthony, Fabio, Daniel S, Nagin, Russell K, Banks, Yidi, Qin, Hyun-Jung, Park, Kate F, Kernan, Scott W, Canna, Robert A, Berg, David, Wessel, Murray M, Pollack, Kathleen, Meert, Mark, Hall, Christopher, Newth, John C, Lin, Allan, Doctor, Tom, Shanley, Tim, Cornell, Rick E, Harrison, Athena F, Zuppa, Ron W, Reeder, Kathy, Sward, Richard, Holubkov, Daniel A, Notterman, J Michael, Dean, and Joseph A, Carcillo

Subjects

Inflammation, C-Reactive Protein, Sepsis, Ferritins, Humans, COVID-19, Cytokines, Prospective Studies, Child, Pandemics, Biomarkers

Abstract

Interest in using bedside C-reactive protein (CRP) and ferritin levels to identify patients with hyperinflammatory sepsis who might benefit from anti-inflammatory therapies has piqued with the COVID-19 pandemic experience. Our first objective was to identify patterns in CRP and ferritin trajectory among critically ill pediatric sepsis patients. We then examined the association between these different groups of patients in their inflammatory cytokine responses, systemic inflammation, and mortality risks.A prospective, observational cohort study.Children with sepsis and organ failure in nine pediatric intensive care units in the United States.Two hundred and fifty-five children were enrolled. Five distinct clinical multi-trajectory groups were identified. Plasma CRP (mg/dL), ferritin (ng/mL), and 31 cytokine levels were measured at two timepoints during sepsis (median Day 2 and Day 5). Group-based multi-trajectory models (GBMTM) identified groups of children with distinct patterns of CRP and ferritin.Group 1 had normal CRP and ferritin levels ( n = 8; 0% mortality); Group 2 had high CRP levels that became normal, with normal ferritin levels throughout ( n = 80; 5% mortality); Group 3 had high ferritin levels alone ( n = 16; 6% mortality); Group 4 had very high CRP levels, and high ferritin levels ( n = 121; 11% mortality); and Group 5 had very high CRP and very high ferritin levels ( n = 30; 40% mortality). Cytokine responses differed across the five groups, with ferritin levels correlated with macrophage inflammatory protein 1α levels and CRP levels reflective of many cytokines.Bedside CRP and ferritin levels can be used together to distinguish groups of children with sepsis who have different systemic inflammation cytokine responses and mortality risks. These data suggest future potential value in personalized clinical trials with specific targets for anti-inflammatory therapies.

Published

2023

2. Improvement of Refractory Systemic Juvenile Idiopathic Arthritis-Associated Lung Disease with Single-Agent Blockade of IL-1β and IL-18

Author

Julia E. Rood, Ayman Rezk, Jennifer Pogoriler, Laura S. Finn, Jon M. Burnham, Maureen B. Josephson, Amit Bar-Or, Edward M. Behrens, and Scott W. Canna

Subjects

Immunology, Immunology and Allergy

Published

2022

3. Identification of Distinct Inflammatory Programs and Biomarkers in Systemic Juvenile Idiopathic Arthritis and Related Lung Disease by Serum Proteome Analysis

Author

Guangbo Chen, Gail H. Deutsch, Grant S. Schulert, Hong Zheng, SoRi Jang, Bruce Trapnell, Pui Y. Lee, Claudia Macaubas, Katherine Ho, Corinne Schneider, Vivian E. Saper, Adriana Almeida de Jesus, Mark A. Krasnow, Alexei Grom, Raphaela Goldbach‐Mansky, Purvesh Khatri, Elizabeth D. Mellins, and Scott W. Canna

Subjects

Rheumatology, Immunology, Immunology and Allergy

Published

2022

4. Cytokine Storm Syndromes in Pediatric Patients

Author

Caroline Diorio, David T. Teachey, and Scott W. Canna

Subjects

Immunology and Allergy

Published

2023

5. mTORC1 links pathology in experimental models of Still’s disease and macrophage activation syndrome

Author

Zhengping Huang, Xiaomeng You, Liang Chen, Yan Du, Kailey Brodeur, Hyuk Jee, Qiang Wang, Grace Linder, Roxane Darbousset, Pierre Cunin, Margaret H. Chang, Alexandra Wactor, Brian M. Wauford, Marc J. C. Todd, Kevin Wei, Ying Li, Anais Levescot, Yoichiro Iwakura, Virginia Pascual, Nicole E. Baldwin, Pierre Quartier, Tianwang Li, Maria T. Gianatasio, Robert P. Hasserjian, Lauren A. Henderson, David B. Sykes, Elizabeth D. Mellins, Scott W. Canna, Julia F. Charles, Peter A. Nigrovic, and Pui Y. Lee

Subjects

Adult, Multidisciplinary, Macrophage Activation Syndrome, General Physics and Astronomy, General Chemistry, Mechanistic Target of Rapamycin Complex 1, Models, Theoretical, Arthritis, Juvenile, Lymphohistiocytosis, Hemophagocytic, General Biochemistry, Genetics and Molecular Biology, Mice, Humans, Animals, Child

Abstract

Still’s disease is a severe inflammatory syndrome characterized by fever, skin rash and arthritis affecting children and adults. Patients with Still’s disease may also develop macrophage activation syndrome, a potentially fatal complication of immune dysregulation resulting in cytokine storm. Here we show that mTORC1 (mechanistic target of rapamycin complex 1) underpins the pathology of Still’s disease and macrophage activation syndrome. Single-cell RNA sequencing in a murine model of Still’s disease shows preferential activation of mTORC1 in monocytes; both mTOR inhibition and monocyte depletion attenuate disease severity. Transcriptomic data from patients with Still’s disease suggest decreased expression of the mTORC1 inhibitors TSC1/TSC2 and an mTORC1 gene signature that strongly correlates with disease activity and treatment response. Unrestricted activation of mTORC1 by Tsc2 deletion in mice is sufficient to trigger a Still’s disease-like syndrome, including both inflammatory arthritis and macrophage activation syndrome with hemophagocytosis, a cellular manifestation that is reproduced in human monocytes by CRISPR/Cas-mediated deletion of TSC2. Consistent with this observation, hemophagocytic histiocytes from patients with macrophage activation syndrome display prominent mTORC1 activity. Our study suggests a mechanistic link of mTORC1 to inflammation that connects the pathogenesis of Still’s disease and macrophage activation syndrome.

Published

2022

6. Genetic and commensal induction of IL-18 drive intestinal epithelial MHCII via IFNγ

Author

L. Yang, Corinne Schneider, Vinh Dang, L. A. Van Der Kraak, J. A. Varghese, Timothy W. Hand, Eric S. Weiss, Scott W. Canna, and Ansen H.P. Burr

Subjects

0301 basic medicine, Inflammasomes, Immunology, Gene Expression, enterocyte, chemical and pharmacologic phenomena, Biology, Systemic inflammation, Models, Biological, Article, Immunophenotyping, Interferon-gamma, Mice, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, inflammasome, NLRC4, medicine, Animals, Immunology and Allergy, Interferon gamma, Intestinal Mucosa, Immunity, Mucosal, Homeodomain Proteins, Mice, Knockout, Histocompatibility Antigens Class II, Interleukin-18, Interleukin, Inflammasome, dysbiosis, respiratory system, medicine.disease, Gastrointestinal Microbiome, Cell biology, Enterocytes, 030104 developmental biology, MHCII, Toll-Like Receptor 9, Cytokines, Interleukin 18, medicine.symptom, Dysbiosis, Biomarkers, 030215 immunology, medicine.drug

Abstract

Major Histocompatibility Complex Class II (MHCII) is dynamically expressed on intestinal epithelial cells (IECs) throughout the intestine, but its regulation remains poorly understood. We observed that spontaneous upregulation of IEC MHCII in locally-bred Rag1−/− mice correlated with serum Interleukin (IL)-18, was transferrable via cohousing to commercially-bred immunodeficient mice and could be inhibited by both IL-12 and IL-18 blockade. Overproduction of intestinal IL-18 due to an activating Nlrc4 mutation upregulated IEC MHCII via classical inflammasome machinery independently of immunodeficiency or dysbiosis. Immunodeficient dysbiosis increased Il18 transcription, which synergized with NLRC4 inflammasome activity to drive elevations in serum IL-18. This IL-18-MHCII axis was confirmed in several other models of intestinal and systemic inflammation. Elevated IL-18 reliably preceded MHCII upregulation, suggesting an indirect effect on IECs, and mice with IL-18 overproduction showed activation or expansion of type 1 lymphocytes. Interferon Gamma (IFNg) was uniquely able to upregulate IEC MHCII in enteroid cultures and was required for MHCII upregulation in several in vivo systems. Thus, we have linked intestinal dysbiosis, systemic inflammation, and inflammasome activity to IEC MHCII upregulation via an intestinal IL-18-IFNg axis. Understanding this process may be crucial for determining the contribution of IEC MHCII to intestinal homeostasis, host defense, and tolerance., Graphical Abstract

Published

2021

7. Systemic and Nodular Hyperinflammation in a Patient with Refractory Familial Hemophagocytic Lymphohistiocytosis 2

Author

Scott W. Canna, Jessie L. Barnum, Darshit Thakrar, Corinne Schneider, Julia Segal, Steven William Allen, Miguel Reyes-Múgica, Jessica D Daley, Cláudia M. Salgado, and Serter Gumus

Subjects

0301 basic medicine, endocrine system, medicine.medical_specialty, Immunology, Anti-Inflammatory Agents, Salvage therapy, Tachypnea, Gastroenterology, Article, Dexamethasone, Lymphohistiocytosis, Hemophagocytic, 03 medical and health sciences, Fatal Outcome, 0302 clinical medicine, hemic and lymphatic diseases, Internal medicine, Humans, Immunologic Factors, Immunology and Allergy, Medicine, Alemtuzumab, Etoposide, Inflammation, Salvage Therapy, Anakinra, Hemophagocytic lymphohistiocytosis, biology, Perforin, business.industry, Perforin Deficiency, fungi, Antibodies, Monoclonal, Immunoglobulins, Intravenous, Infant, Familial Hemophagocytic Lymphohistiocytosis, musculoskeletal system, medicine.disease, Antibodies, Neutralizing, Interleukin 1 Receptor Antagonist Protein, 030104 developmental biology, biology.protein, Female, medicine.symptom, business, hormones, hormone substitutes, and hormone antagonists, 030215 immunology, medicine.drug

Abstract

Familial hemophagocytic lymphohistiocytosis (HLH) is a life-threatening hyperinflammatory syndrome resulting from defective cytotoxicity. A previously healthy 3-month-old female presented with fever, irritability, abdominal distention, and tachypnea. She ultimately met all eight HLH-2004 diagnostic criteria, accompanied by elevated CXCL9. Initial empiric anti-inflammatory treatment included anakinra and IVIg, which stabilized ferritin and cytopenias. She had molecular and genetic confirmation of perforin deficiency and was started on dexamethasone and etoposide per HLH-94. She clinically improved, though CXCL9 and sIL-2Ra remained elevated. She was readmitted at week 8 for relapsed HLH without clear trigger and HLH-94 induction therapy was reinitiated. Her systemic HLH symptoms failed to respond and she soon developed symptomatic CNS HLH. She was incidentally found to have multifocal lung and kidney nodules, which were sterile and consisted largely of histiocytes and activated, oligoclonal CD8 T cells. The patient had a laboratory response to salvage therapy with alemtuzumab and emapalumab, but progressive neurologic decline led to withdrawal of care. This report highlights HLH foci manifest as pulmonary/renal nodules, demonstrates the utility of monitoring an array of HLH biomarkers, and suggests possible benefit of earlier salvage therapy.

Published

2021

8. Improvement of Refractory Systemic Juvenile Idiopathic Arthritis-Associated Lung Disease with Single-Agent Blockade of IL-1β and IL-18

Author

Julia E, Rood, Ayman, Rezk, Jennifer, Pogoriler, Laura S, Finn, Jon M, Burnham, Maureen B, Josephson, Amit, Bar-Or, Edward M, Behrens, and Scott W, Canna

Abstract

Systemic juvenile idiopathic arthritis associated with interstitial lung disease (SJIA-LD) represents a highly morbid subset of SJIA for which effective therapies are lacking. We report the case of a patient with refractory SJIA-LD who underwent treatment with MAS-825, an investigational bispecific monoclonal antibody targeting IL-1β and IL-18. MAS-825 treatment was associated with a marked reduction in total IL-18 and free IL-18 in both serum and bronchoalveolar lavage fluid (BAL). Baseline oxygen saturation, exercise tolerance, and quality of life metrics improved after treatment with MAS-825, while pulmonary function testing remained stable. Following treatment, the BAL showed no evidence of pulmonary alveolar proteinosis and inflammatory infiltrates were markedly reduced, reflected by decreased numbers of CD4 T-cells, CD8 T-cells, and macrophages. The patient was able to wean entirely off systemic corticosteroids and other biologics after 10 months of treatment with MAS-825 and experienced no side effects of the drug. This case demonstrates improvement in pulmonary symptoms, lung inflammation, and burden of immunomodulatory therapy after treatment with MAS-825 and suggests that simultaneous targeting of both IL-1β and IL-18 may be a safe and effective treatment strategy in SJIA-LD.

Published

2022

9. Machine learning derivation of four computable 24-h pediatric sepsis phenotypes to facilitate enrollment in early personalized anti-inflammatory clinical trials

Author

Yidi, Qin, Kate F, Kernan, Zhenjiang, Fan, Hyun-Jung, Park, Soyeon, Kim, Scott W, Canna, John A, Kellum, Robert A, Berg, David, Wessel, Murray M, Pollack, Kathleen, Meert, Mark, Hall, Christopher, Newth, John C, Lin, Allan, Doctor, Tom, Shanley, Tim, Cornell, Rick E, Harrison, Athena F, Zuppa, Russell, Banks, Ron W, Reeder, Richard, Holubkov, Daniel A, Notterman, J, Michael Dean, and Joseph A, Carcillo

Subjects

Clinical Trials as Topic, Organ Dysfunction Scores, Macrophage Activation Syndrome, Multiple Organ Failure, Anti-Inflammatory Agents, Reproducibility of Results, Critical Care and Intensive Care Medicine, Thrombocytopenia, Machine Learning, C-Reactive Protein, Phenotype, Creatinine, Sepsis, Ferritins, Humans, Child

Abstract

Background Thrombotic microangiopathy-induced thrombocytopenia-associated multiple organ failure and hyperinflammatory macrophage activation syndrome are important causes of late pediatric sepsis mortality that are often missed or have delayed diagnosis. The National Institutes of General Medical Science sepsis research working group recommendations call for application of new research approaches in extant clinical data sets to improve efficiency of early trials of new sepsis therapies. Our objective is to apply machine learning approaches to derive computable 24-h sepsis phenotypes to facilitate personalized enrollment in early anti-inflammatory trials targeting these conditions. Methods We applied consensus, k-means clustering analysis to our extant PHENOtyping sepsis-induced Multiple organ failure Study (PHENOMS) dataset of 404 children. 24-hour computable phenotypes are derived using 25 available bedside variables including C-reactive protein and ferritin. Results Four computable phenotypes (PedSep-A, B, C, and D) are derived. Compared to all other phenotypes, PedSep-A patients (n = 135; 2% mortality) were younger and previously healthy, with the lowest C-reactive protein and ferritin levels, the highest lymphocyte and platelet counts, highest heart rate, and lowest creatinine (p n = 102; 12% mortality) were most likely to be intubated and had the lowest Glasgow Coma Scale Score (p n = 110; mortality 10%) had the highest temperature and Glasgow Coma Scale Score, least pulmonary failure, and lowest lymphocyte counts (p n = 56, 34% mortality) had the highest creatinine and number of organ failures, including renal, hepatic, and hematologic organ failure, with the lowest platelet counts (p thrombocytopenia-associated multiple organ failure (Adj OR 47.51 95% CI [18.83–136.83], p macrophage activation syndrome (Adj OR 38.63 95% CI [13.26–137.75], p Conclusions Four computable phenotypes are derived, with PedSep-D being optimal for enrollment in early personalized anti-inflammatory trials targeting thrombocytopenia-associated multiple organ failure and macrophage activation syndrome in pediatric sepsis. A computer tool for identification of individual patient membership (www.pedsepsis.pitt.edu) is provided. Reproducibility will be assessed at completion of two ongoing pediatric sepsis studies.

Published

2022

10. IL-1 receptor antagonist, MIS-C, and the peculiar autoimmunity of SARS-CoV-2

Author

Hamid Bassiri and Scott W Canna

Subjects

Rheumatology, Immunology, Immunology and Allergy

Published

2022

11. American College of Rheumatology Clinical Guidance for Multisystem Inflammatory Syndrome in Children Associated With SARS–CoV‐2 and Hyperinflammation in Pediatric COVID‐19: Version 1

Author

Mark Gorelik, Anne Ferris, Grant S. Schulert, Philip Seo, Rae S. M. Yeung, Mary Beth F. Son, Amy S. Mudano, Kate F. Kernan, Adriana H. Tremoulet, Edward M. Behrens, Sivia K. Lapidus, Jay J. Mehta, Scott W. Canna, David R. Karp, Hamid Bassiri, Kevin G. Friedman, Amy S. Turner, and Lauren A. Henderson

Subjects

medicine.medical_specialty, Consensus, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, MEDLINE, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, 030225 pediatrics, Internal medicine, Humans, Immunology and Allergy, Medicine, 030212 general & internal medicine, Intensive care medicine, book, business.industry, COVID-19, Systemic Inflammatory Response Syndrome, Living document, Pediatric Infectious Disease, Etiology, book.journal, business, Pediatric population

Abstract

OBJECTIVE: To provide guidance on the management of multisystem inflammatory syndrome in children (MIS-C), a condition characterized by fever, inflammation, and multiorgan dysfunction that manifests late in the course of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection, and to provide recommendations for children with hyperinflammation during coronavirus disease 2019 (COVID-19), the acute, infectious phase of SARS-CoV-2 infection. METHODS: A multidisciplinary task force was convened by the American College of Rheumatology (ACR) to provide guidance on the management of MIS-C associated with SARS-CoV-2 and hyperinflammation in COVID-19. The task force was composed of 9 pediatric rheumatologists, 2 adult rheumatologists, 2 pediatric cardiologists, 2 pediatric infectious disease specialists, and 1 pediatric critical care physician. Preliminary statements addressing clinical questions related to MIS-C and hyperinflammation in COVID-19 were developed based on evidence reports. Consensus was built through a modified Delphi process that involved 2 rounds of anonymous voting and 2 webinars. A 9-point scale was used to determine the appropriateness of each statement (median scores of 1-3 for inappropriate, 4-6 for uncertain, and 7-9 for appropriate), and consensus was rated as low, moderate, or high based on dispersion of the votes along the numeric scale. Approved guidance statements were those that were classified as appropriate with moderate or high levels of consensus, as prespecified prior to voting. RESULTS: The ACR task force approved a total of 128 guidance statements addressing the management of MIS-C and hyperinflammation in pediatric COVID-19. These statements were refined into 40 final clinical guidance statements, accompanied by a flow diagram depicting the diagnostic pathway for MIS-C. CONCLUSION: Our understanding of SARS-CoV-2-related syndromes in the pediatric population continues to evolve. The guidance provided in this "living document" reflects currently available evidence, coupled with expert opinion, and will be revised as further evidence becomes available.

Published

2020

12. Pediatric hemophagocytic lymphohistiocytosis

Author

Rebecca A. Marsh and Scott W. Canna

Subjects

Epstein-Barr Virus Infections, endocrine system, F-Box-WD Repeat-Containing Protein 7, Immunology, Hepatosplenomegaly, X-Linked Inhibitor of Apoptosis Protein, Disease, Biochemistry, Lymphohistiocytosis, Hemophagocytic, hemic and lymphatic diseases, Genetic predisposition, Animals, Humans, Medicine, Genetic Predisposition to Disease, UNC13D, Signaling Lymphocytic Activation Molecule Associated Protein, Child, Hemophagocytic lymphohistiocytosis, business.industry, Calcium-Binding Proteins, Review Series, fungi, Genetic disorder, Disease Management, Genetic Variation, X-linked lymphoproliferative disease, Cell Biology, Hematology, medicine.disease, CARD Signaling Adaptor Proteins, Macrophage activation syndrome, medicine.symptom, business

Abstract

Hemophagocytic lymphohistiocytosis (HLH) is a syndrome describing patients with severe systemic hyperinflammation. Characteristic features include unremitting fever, cytopenias, hepatosplenomegaly, and elevation of typical HLH biomarkers. Patients can develop hepatitis, coagulopathy, liver failure, central nervous system involvement, multiorgan failure, and other manifestations. The syndrome has a high mortality rate. More and more, it is recognized that while HLH can be appropriately used as a broad summary diagnosis, many pediatric patients actually suffer from an expanding spectrum of genetic diseases that can be complicated by the syndrome of HLH. Classic genetic diseases in which HLH is a typical and common manifestation include pathogenic changes in familial HLH genes (PRF1, UNC13D, STXBP2, and STX11), several granule/pigment abnormality genes (RAB27A, LYST, and AP3B1), X-linked lymphoproliferative disease genes (SH2D1A and XIAP), and others such as NLRC4, CDC42, and the Epstein-Barr virus susceptibility diseases. There are many other genetic diseases in which HLH is an infrequent complication of the disorder as opposed to a prominent manifestation of the disease caused directly by the genetic defect, including other primary immune deficiencies and inborn errors of metabolism. HLH can also occur in patients with underlying rheumatologic or autoinflammatory disorders and is usually designated macrophage activation syndrome in those settings. Additionally, HLH can develop in patients during infections or malignancies without a known (or as-yet-identified) genetic predisposition. This article will attempt to summarize current concepts in the pediatric HLH field as well as offer a practical diagnostic and treatment overview.

Published

2020

13. Sepsis with liver dysfunction and coagulopathy predicts an inflammatory pattern of macrophage activation

Author

Renee R, Anderko, Hernando, Gómez, Scott W, Canna, Bita, Shakoory, Derek C, Angus, Donald M, Yealy, David T, Huang, John A, Kellum, Joseph A, Carcillo, and Ronald M, Migues

Subjects

Critical Care and Intensive Care Medicine

Abstract

BackgroundInterleukin-1 receptor antagonists can reduce mortality in septic shock patients with hepatobiliary dysfunction and disseminated intravascular coagulation (HBD + DIC), an organ failure pattern with inflammatory features consistent with macrophage activation. Identification of clinical phenotypes in sepsis may allow for improved care. We aim to describe the occurrence of HBD + DIC in a contemporary cohort of patients with sepsis and determine the association of this phenotype with known macrophage activation syndrome (MAS) biomarkers and mortality. We performed a retrospective nested case–control study in adult septic shock patients with concurrent HBD + DIC and an equal number of age-matched controls, with comparative analyses of all-cause mortality and circulating biomarkers between the groups. Multiple logistic regression explored the effect of HBD + DIC on mortality and the discriminatory power of the measured biomarkers for HBD + DIC and mortality.ResultsSix percent of septic shock patients (n = 82/1341) had HBD + DIC, which was an independent risk factor for 90-day mortality (OR = 3.1, 95% CI 1.4–7.5,p = 0.008). Relative to sepsis controls, the HBD + DIC cohort had increased levels of 21 of the 26 biomarkers related to macrophage activation (p ConclusionThe HBD + DIC phenotype identified patients with high mortality and a molecular signature resembling that of MAS. These observations suggest trials of MAS-directed therapies are warranted.

Published

2022

14. American College of Rheumatology Clinical Guidance for Multisystem Inflammatory Syndrome in Children Associated With SARS–CoV‐2 and Hyperinflammation in Pediatric COVID‐19: Version 3

Author

Lauren A. Henderson, Scott W. Canna, Kevin G. Friedman, Mark Gorelik, Sivia K. Lapidus, Hamid Bassiri, Edward M. Behrens, Kate F. Kernan, Grant S. Schulert, Philip Seo, Mary Beth F. Son, Adriana H. Tremoulet, Christina VanderPluym, Rae S. M. Yeung, Amy S. Mudano, Amy S. Turner, David R. Karp, and Jay J. Mehta

Subjects

Adult, Rheumatology, SARS-CoV-2, Immunology, COVID-19, Humans, Immunology and Allergy, Child, Systemic Inflammatory Response Syndrome, United States

Abstract

To provide guidance on the management of Multisystem Inflammatory Syndrome in Children (MIS-C), a condition characterized by fever, inflammation, and multiorgan dysfunction that manifests late in the course of SARS-CoV-2 infection. Recommendations are also provided for children with hyperinflammation during COVID-19, the acute, infectious phase of SARS-CoV-2 infection.The Task Force is composed of 9 pediatric rheumatologists and 2 adult rheumatologists, 2 pediatric cardiologists, 2 pediatric infectious disease specialists, and 1 pediatric critical care physician. Preliminary statements addressing clinical questions related to MIS-C and hyperinflammation in COVID-19 were developed based on evidence reports. Consensus was built through a modified Delphi process that involved anonymous voting and webinar discussion. A 9-point scale was used to determine the appropriateness of each statement (median scores of 1-3 for inappropriate, 4-6 for uncertain, and 7-9 for appropriate). Consensus was rated as low, moderate, or high based on dispersion of the votes. Approved guidance statements were those that were classified as appropriate with moderate or high levels of consensus, which were prespecified before voting.The guidance was approved in June 2020 and updated in November 2020 and October 2021, and consists of 41 final guidance statements accompanied by flow diagrams depicting the diagnostic pathway for MIS-C and recommendations for initial immunomodulatory treatment of MIS-C.Our understanding of SARS-CoV-2-related syndromes in the pediatric population continues to evolve. This guidance document reflects currently available evidence coupled with expert opinion, and will be revised as further evidence becomes available.

Published

2022

15. DDX17 is an essential mediator of sterile NLRC4 inflammasome activation by retrotransposon RNAs

Author

Vidya L. Ambati, Ivana Apicella, Srinivas R. Sadda, Peirong Huang, Akhil Varshney, Nagaraj Kerur, Shaobin Wang, Meenakshi Ambati, Felipe Pereira, Siddharth Narendran, Kameshwari Ambati, Kirstie Baker, Yosuke Nagasaka, Dionne Argyle, Bo Liu, Bradley D. Gelfand, Kenneth M. Marion, Tamer Sallam, Scott W. Canna, Kartik Gupta, Praveen Yerramothu, Jayakrishna Ambati, Shuichiro Hirahara, and David R. Hinton

Subjects

Mice, Knockout, Retroelements, Inflammasomes, Calcium-Binding Proteins, Immunology, Inflammasome, Retrotransposon, General Medicine, Biology, Cell biology, DEAD-box RNA Helicases, Mice, Inbred C57BL, Mice, Mediator, NLRC4, medicine, Animals, RNA, Apoptosis Regulatory Proteins, Cells, Cultured, medicine.drug

Abstract

Detection of microbial products by multiprotein complexes known as inflammasomes is pivotal to host defense against pathogens. Nucleotide-binding domain leucine-rich repeat (NLR) CARD domain containing 4 (NLRC4) forms an inflammasome in response to bacterial products; this requires their detection by NLR family apoptosis inhibitory proteins (NAIPs), with which NLRC4 physically associates. However, the mechanisms underlying sterile NLRC4 inflammasome activation, which is implicated in chronic noninfectious diseases, remain unknown. Here, we report that endogenous short interspersed nuclear element (SINE) RNAs, which promote atrophic macular degeneration (AMD) and systemic lupus erythematosus (SLE), induce NLRC4 inflammasome activation independent of NAIPs. We identify DDX17, a DExD/H box RNA helicase, as the sensor of SINE RNAs that licenses assembly of an inflammasome comprising NLRC4, NLR pyrin domain–containing protein 3, and apoptosis-associated speck-like protein–containing CARD and induces caspase-1 activation and cytokine release. Inhibiting DDX17-mediated NLRC4 inflammasome activation decreased interleukin-18 release in peripheral blood mononuclear cells of patients with SLE and prevented retinal degeneration in an animal model of AMD. Our findings uncover a previously unrecognized noncanonical NLRC4 inflammasome activated by endogenous retrotransposons and provide potential therapeutic targets for SINE RNA–driven diseases.

Published

2021

16. Proteomic profiling of MIS-C patients indicates heterogeneity relating to interferon gamma dysregulation and vascular endothelial dysfunction

Author

Caroline Diorio, Rawan Shraim, Laura A. Vella, Josephine R. Giles, Amy E. Baxter, Derek A. Oldridge, Scott W. Canna, Sarah E. Henrickson, Kevin O. McNerney, Frances Balamuth, Chakkapong Burudpakdee, Jessica Lee, Tomas Leng, Alvin Farrel, Michele P. Lambert, Kathleen E. Sullivan, E. John Wherry, David T. Teachey, Hamid Bassiri, and Edward M. Behrens

Subjects

Multidisciplinary, endocrine system diseases, Science, fungi, food and beverages, General Physics and Astronomy, General Chemistry, Predictive markers, Article, General Biochemistry, Genetics and Molecular Biology, Rheumatology, Viral infection, otorhinolaryngologic diseases, Interferons, Chemokines, skin and connective tissue diseases

Abstract

Multi-system Inflammatory Syndrome in Children (MIS-C) is a major complication of Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) infection in pediatric patients. Weeks after an often mild or asymptomatic initial infection with SARS-CoV-2 children may present with a severe shock-like picture and marked inflammation. Children with MIS-C present with varying degrees of cardiovascular and hyperinflammatory symptoms. Here we perform a comprehensive analysis of the plasma proteome of more than 1400 proteins in children with SARS-CoV-2. We hypothesize that the proteome would reflect heterogeneity in hyperinflammation and vascular injury, and further identify pathogenic mediators of disease. We show that protein signatures demonstrate overlap between MIS-C, and the inflammatory syndromes macrophage activation syndrome (MAS) and thrombotic microangiopathy (TMA). We demonstrate that PLA2G2A is an important marker of MIS-C that associates with TMA. We find that IFNγ responses are dysregulated in MIS-C patients, and that IFNγ levels delineate clinical heterogeneity., Multi-inflammatory syndrome in children (MIS-C) can be associated with SARS-CoV-2 infection but can also be similar to other inflammatory syndromes. Here the authors characterise the plasma proteome phenotype in MIS-C and compare to other SARS-CoV-2 related syndromes and find disproportionately high IFN-γ responses in MIS-C patients.

Published

2021

17. Derivation of four computable 24-hour pediatric sepsis phenotypes to facilitate personalized enrollment in early precise anti-inflammatory clinical trials

Author

Yidi Qin, Kate F. Kernan, Zhenjiang Fan, Hyun-Jung Park, Soyeon Kim, Scott W. Canna, John A Kellum, Robert A. Berg, David Wessel, Murray M. Pollack, Kathleen Meert, Mark Hall, Christopher Newth, John C. Lin, Allan Doctor, Tom Shanley, Tim Cornell, Rick E. Harrison, Athena F. Zuppa, Russell Banks, Ron W. Reeder, Richard Holubkov, Daniel A. Notterman, J. Michael Dean, and Joseph A. Carcillo

Abstract

ObjectiveThrombotic microangiopathy induced Thrombocytopenia Associated Multiple Organ Failure and hyperinflammatory Macrophage Activation Syndrome are important causes of late pediatric sepsis mortality that are often missed or have delayed diagnosis. Our objective is to derive computable 24-hour sepsis phenotypes to facilitate enrollment in early precise anti-inflammatory trials targeting mortality from these conditions.DesignMachine learning analysis using consensus k-means clustering.SettingNine pediatric intensive care units.Patients404 children with severe sepsis.Interventions24-hour computable phenotypes derived using 25 bedside variables including C-reactive protein and ferritin.Measurements and Main ResultsFour computable phenotypes (PedSep-A, B, C, and D) are derived. Compared to the overall population mean, PedSep-A has the least inflammation (median C-reactive protein 7.3 mg/dL, ferritin 125 ng/mL), younger age, less chronic illness, and more respiratory failure (n = 135; 2% mortality); PedSep-B (median C-reactive protein 13.2 mg/dL, ferritin 225 ng/ mL) has organ failure with intubated respiratory failure, shock, and Glasgow Coma Scale score < 7 (n = 102, 12% mortality); PedSep-C (median C-reactive protein 15.2 mg/dL, ferritin 405 ng/mL) has elevated ferritin, lymphopenia, more shock, more hepatic failure and less respiratory failure (n = 110; mortality 10%); and, PedSep D (median C-reactive protein 13.1 mg/dL ferritin 610 ng/mL), has hyperferritinemic, thrombocytopenic multiple organ failure with more cardiovascular, respiratory, hepatic, renal, hematologic, and neurologic system failures (n = 56, 34% mortality). PedSep-D has highest likelihood of Thrombocytopenia Associated Multiple Organ Failure (Adj OR 47.51 95% CI [18.83-136.83], p < 0.0001) and Macrophage Activation Syndrome (Adj OR 38.63 95% CI [13.26-137.75], p CONCLUSIONS AND RELEVANCEMachine learning identifies four computable phenotypes (www.pedsepsis.pitt.edu). Membership in PedSep-D appears optimal for enrollment in early anti-inflammatory trials targeting Thrombocytopenia Associated Multiple Organ Failure and Macrophage Activation Syndrome.Author’s CommentQuestionCan machine learning methods derive 24-hour computable pediatric sepsis phenotypes that facilitate early identification of patients for enrollment in precise anti-inflammatory therapy trials?FindingsFour distinct phenotypes (PedSep-A, B, C, and D) were derived by assessing 25 bedside clinical variables in 404 children with sepsis. PedSep-D patients had a thrombotic microangiopathy and hyperinflammatory macrophage activation biomarker response, and improved survival odds associated with combined methylprednisolone plus intravenous immunoglobulin therapy.MeaningFour novel computable 24-hour phenotypes are identifiable (www.pedsepsis.pitt.edu) that could potentially facilitate enrollment in early precise anti-inflammatory trials targeting thrombotic microangiopathy and macrophage activation in pediatric sepsis.

Published

2021

18. Excess Serum Interleukin-18 Distinguishes Patients With Pathogenic Mutations in PSTPIP1

Author

Adriana de Jesus, Daniel L. Kastner, Charlotte Girard-Guyonvarc'h, Scott W. Canna, Wonyong Lee, Amanda K. Ombrello, Corinne Schneider, Jae Jin Chae, Ivona Aksentijevich, Juan I. Aróstegui, Raphaela Goldbach-Mansky, Cem Gabay, Vinh Dang, and Deborah L. Stone

Subjects

Adult, Male, Adolescent, Immunology, Arthritis, Familial Mediterranean fever, Article, Young Adult, Rheumatology, Acne Vulgaris, medicine, Immunology and Allergy, Humans, Child, Adaptor Proteins, Signal Transducing, Retrospective Studies, Enterocolitis, Arthritis, Infectious, business.industry, Interleukin-18, Interleukin, Infant, PAPA syndrome, Middle Aged, medicine.disease, Pyoderma Gangrenosum, Cytoskeletal Proteins, Macrophage activation syndrome, Child, Preschool, Mutation, Interleukin 18, Female, medicine.symptom, business, Pyoderma gangrenosum

Abstract

Dominantly inherited PSTPIP1 mutations cause a spectrum of autoinflammatory manifestations epitomized by PAPA syndrome (pyogenic sterile arthritis, pyoderma gangrenosum, and acne (PAPA) syndrome.). The connections between PSTPIP1 and PAPA syndrome are poorly understood, although evidence suggests involvement of pyrin inflammasome activation. Interleukin-18 (IL-18) is an inflammasome-activated cytokine associated with susceptibility to macrophage activation syndrome (MAS). This study was undertaken to investigate an association of IL-18 with PAPA syndrome.Clinical and genetic data and serum samples were obtained from patients referred to institutions due to symptoms indicative of PAPA syndrome. Serum IL-18, IL-18 binding protein (IL-18BP), and CXCL9 levels were assessed by bead-based assay, and free IL-18 levels were assessed by enzyme-linked immunosorbent assay.The symptoms of PSTPIP1-positive patients with PAPA syndrome overlapped with those of mutation-negative patients with PAPA-like conditions, but mutation-positive patients had earlier onset and a greater proportion had a history of arthritis. We found uniform elevation of total serum IL-18 in treated PAPA syndrome patients at levels nearly as high as those seen in NLRC4-associated autoinflammation with infantile enterocolitis patients, and well above levels found in most familial Mediterranean fever patients. Serum IL-18 elevation in PAPA syndrome patients persisted despite fluctuations in disease activity. Levels of the soluble IL-18 antagonist IL-18BP were modestly elevated, and PAPA syndrome patients had detectable free IL-18. PAPA syndrome was rarely associated with elevation of CXCL9, an indicator of interferon-γ activity, but no PAPA syndrome patients had a history of MAS.PAPA syndrome is a refractory and often disabling monogenic autoinflammatory disease associated with chronic and unopposed elevation of serum IL-18 levels but not with risk of MAS. These findings affect our understanding of the diseases in which IL-18 is overproduced and suggest a link between pyrin inflammasome activation, IL-18, and autoinflammation, without susceptibility to MAS.

Published

2021

19. Causal inference using deep-learning variable selection identifies and incorporates direct and indirect causalities in complex biological systems

Author

Zhenjiang Fan, Scott W. Canna, Soyeon Kim, Panayiotis V. Benos, Joseph A. Carcillo, Gregory F. Cooper, Hyun Jung Park, and Kate F. Kernan

Subjects

Biological data, Artificial neural network, Computer science, business.industry, Deep learning, Feature selection, Causal structure, Machine learning, computer.software_genre, Causal inference, Identification (biology), Artificial intelligence, Polymicrobial sepsis, business, computer

Abstract

In complex diseases, causal structure learning across biological variables is critical to identify modifiable triggers or potential therapeutic agents. A limitation of existing causal learning methods is that they cannot identify indirect causal relations, those that would interact through latent mediating variables. We developed the first computational method that identifies both direct and indirect causalities, causal inference using deep-learning variable-selection (causalDeepVASE). To accurately identify indirect causalities and incorporate them with direct causalities, causalDeepVASE develops a deep neural network approach and extends a flexible causal inference method. In simulated and biological data of various contexts, causalDeepVASE outperforms existing methods in identifying expected or validated causal relations. Further, causalDeepVASE facilitates a systematic understanding of complex diseases. For example, causalDeepVASE uniquely identified a possible causal relation between IFNγ and creatinine suggested in a polymicrobial sepsis model. In future biomedical studies, causalDeepVASE can facilitate the identification of driver genes and therapeutic agents.

Published

2021

20. Adenosine deaminase 2 as a biomarker of macrophage activation syndrome in systemic juvenile idiopathic arthritis

Author

Esra Meidan, Yuelong Huang, Ying Li, Mindy S. Lo, Mary Beth F. Son, Fatma Dedeoglu, Olha Halyabar, Siobhan M. Case, Robert P. Sundel, Edward T. Richardson, Peter A. Nigrovic, Margaret H. Chang, Pui Y. Lee, Lauren A. Henderson, Kacie J Hoyt, Alexandra Wactor, Scott W. Canna, Thuy Do, Michael S. Hershfield, Rachel B Blaustein, Grant S. Schulert, Jacob Sundel, and Jane W. Newburger

Subjects

musculoskeletal diseases, 0301 basic medicine, Immunology, Arthritis, Inflammation, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, medicine, Immunology and Allergy, Juvenile dermatomyositis, 030203 arthritis & rheumatology, biology, medicine.diagnostic_test, business.industry, fungi, C-reactive protein, Interleukin, medicine.disease, 030104 developmental biology, Macrophage activation syndrome, Erythrocyte sedimentation rate, biology.protein, Biomarker (medicine), medicine.symptom, business

Abstract

ObjectiveMacrophage activation syndrome (MAS) is a life-threatening complication of systemic juvenile idiopathic arthritis (sJIA) characterised by a vicious cycle of immune amplification that can culminate in overwhelming inflammation and multiorgan failure. The clinical features of MAS overlap with those of active sJIA, complicating early diagnosis and treatment. We evaluated adenosine deaminase 2 (ADA2), a protein of unknown function released principally by monocytes and macrophages, as a novel biomarker of MAS.MethodsWe established age-based normal ranges of peripheral blood ADA2 activity in 324 healthy children and adults. We compared these ranges with 173 children with inflammatory and immune-mediated diseases, including systemic and non-systemic JIA, Kawasaki disease, paediatric systemic lupus erythematosus and juvenile dermatomyositis.ResultsADA2 elevation beyond the upper limit of normal in children was largely restricted to sJIA with concomitant MAS, a finding confirmed in a validation cohort of sJIA patients with inactive disease, active sJIA without MAS or sJIA with MAS. ADA2 activity strongly correlated with MAS biomarkers including ferritin, interleukin (IL)-18 and the interferon (IFN)-γ-inducible chemokine CXCL9 but displayed minimal association with the inflammatory markers C reactive protein and erythrocyte sedimentation rate. Correspondingly, ADA2 paralleled disease activity based on serial measurements in patients with recurrent MAS episodes. IL-18 and IFN-γ elicited ADA2 production by peripheral blood mononuclear cells, and ADA2 was abundant in MAS haemophagocytes.ConclusionsThese findings collectively identify the utility of plasma ADA2 activity as a biomarker of MAS and lend further support to a pivotal role of macrophage activation in this condition.

Published

2019

21. IL-18 as a biomarker linking systemic juvenile idiopathic arthritis and macrophage activation syndrome

Author

Ndate Fall, Rachel A. Brown, Cem Gabay, Scott W. Canna, Grant S. Schulert, Shima Yasin, Alexei A. Grom, Maggie Henderlight, and Charlotte Girard-Guyonvarc'h

Subjects

musculoskeletal diseases, Male, 0301 basic medicine, medicine.medical_specialty, Childhood arthritis, Macrophage Activation Syndrome/blood/diagnosis, Arthritis, Chemokine CXCL9/blood, Chemokine CXCL9, Severity of Illness Index, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Rheumatology, Interquartile range, Internal medicine, Humans, Medicine, Pharmacology (medical), ddc:616, 030203 arthritis & rheumatology, Arthritis, Juvenile/blood/diagnosis, biology, business.industry, Ferritins/blood, Macrophage Activation Syndrome, fungi, S100 Proteins, Interleukin-18, Area under the curve, S100 Proteins/blood, Clinical Science, medicine.disease, Arthritis, Juvenile, body regions, Ferritin, 030104 developmental biology, Macrophage activation syndrome, Ferritins, biology.protein, Biomarker (medicine), lipids (amino acids, peptides, and proteins), Female, Interleukin 18, business, Interleukin-18/blood, hormones, hormone substitutes, and hormone antagonists, Biomarkers/blood, Biomarkers

Abstract

Objectives Systemic juvenile idiopathic arthritis (sJIA) is a childhood arthritis with features of autoinflammation and high risk of macrophage activation syndrome (MAS). IL-18 has been shown to have key roles in sJIA and MAS. We aimed to examine IL-18 levels in sJIA in relation to disease activity and history of MAS and other disease biomarkers namely S100 proteins and CXCL9. Methods Total IL-18, CXCL9 and S100 proteins levels were determined in 40 sJIA patients, and IL-18 levels were compared between patients with regards to disease activity, history of MAS, and other biomarkers. Results Total IL-18 levels were significantly higher in patients with active sJIA (median 16 499 pg/ml; interquartile range (IQR) 4816–61 839), and remained persistently elevated even in the majority of patients with inactive disease (1164 pg/ml; IQR 587–3444). Patients with history of MAS had significantly higher IL-18 levels (13 380 pg/ml; IQR 4212–62 628) as compared with those without MAS history (956.5 pg/ml; IQR 276.3–4262.5). Total IL-18 performed well with area under the curve of 0.8145 and 0.84 in predicting disease activity and history of MAS, respectively. We observed moderate correlation between IL-18 and CXCL9 (R = 0.56), S100A8/A9 (R = 0.47) and S100A12 (R = 0.46). The correlation was stronger for ferritin (R = 0.74) and overall for those with active disease. Conclusion Total IL-18 levels were elevated in the majority of sJIA patients regardless of clinical features, but were higher in patients with active disease and history of MAS. Change in IL-18 may reflect increased disease activity or development of MAS.

Published

2019

22. Proteomic Profiling of MIS-C Patients Reveals Heterogeneity Relating to Interferon Gamma Dysregulation and Vascular Endothelial Dysfunction

Author

Chakkapong Burudpakdee, E. John Wherry, Rawan Shraim, Caroline Diorio, Fran Balamuth, Laura A. Vella, Kathleen E. Sullivan, Kevin O McNerney, Tomas Leng, Derek A. Oldridge, Edward M. Behrens, Josephine R. Giles, Sarah E. Henrickson, Hamid Bassiri, David T. Teachey, Scott W. Canna, Alvin Farrel, Michele P. Lambert, Amy E. Baxter, and Jessica Lee

Subjects

Proteomics, Thrombotic microangiopathy, Proteome, Inflammation, Disease, Chemokine CXCL9, Group II Phospholipases A2, Asymptomatic, Article, Interferon-gamma, medicine, Humans, Interferon gamma, Vascular Diseases, Endothelial dysfunction, Child, business.industry, COVID-19, medicine.disease, Systemic Inflammatory Response Syndrome, Interleukin-10, Case-Control Studies, Macrophage activation syndrome, Immunology, Endothelium, Vascular, medicine.symptom, business, Biomarkers, medicine.drug

Abstract

Multi-system Inflammatory Syndrome in Children (MIS-C) is a major complication of the Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) pandemic in pediatric patients. Weeks after an often mild or asymptomatic initial infection with SARS-CoV-2 children may present with a severe shock-like picture and marked inflammation. Children with MIS-C present with varying degrees of cardiovascular and hyperinflammatory symptoms. We performed a comprehensive analysis of the plasma proteome of more than 1400 proteins in children with SARS-CoV-2. We hypothesized that the proteome would reflect heterogeneity in hyperinflammation and vascular injury, and further identify pathogenic mediators of disease. Protein signatures demonstrated overlap between MIS-C, and the inflammatory syndromes macrophage activation syndrome (MAS) and thrombotic microangiopathy (TMA). We demonstrate that PLA2G2A is a key marker of MIS-C that associates with TMA. We found that IFNγ responses are dysregulated in MIS-C patients, and that IFNγ levels delineate clinical heterogeneity.

Published

2021

23. Excess Serum Interleukin-18 Distinguishes Patients with Pathogenic Mutations in PSTPIP1

Author

Scott W. Canna, Daniel L. Kastner, Corinne Schneider, Wonyong Lee, Juan I. Aróstegui, Jae Jin Chae, Adriana de Jesus, Charlotte Girard-Guyonvarc'h, Raphaela Goldbach-Mansky, Amanda K. Ombrello, Ivona Aksentijevich, Deborah L. Stone, and Cem Gabay

Subjects

business.industry, Macrophage activation syndrome, Immunology, medicine, Arthritis, Familial Mediterranean fever, CXCL9, Interleukin 18, Disease, PAPA syndrome, medicine.disease, business, Pyoderma gangrenosum

Abstract

ObjectiveDominantly-inherited mutations in PSTPIP1 cause a family of monogenic autoinflammatory diseases epitomized by Pyogenic Arthritis, Pyoderma gangrenosum, and Acne (PAPA) syndrome. The connections between PSTPIP1 and PAPA are poorly understood, although in vitro evidence suggests increased activation of the pyrin-inflammasome. We sought to identify biomarkers of potential mechanistic, diagnostic, and therapeutic utility specific to autoinflammatory diseases.MethodsClinical and genetic data and sera were obtained from patients referred with concern for PAPA syndrome, as well as relevant disease controls. Serum Interleukin-18 (IL-18) and related biomarkers were assessed by bead-based assay.ResultsSymptoms in PSTPIP1 mutation-positive PAPA patients overlapped with those of mutation-negative PAPA-like patients, but the former were younger at onset and had more arthritis. We found uniform elevation of total IL-18 in PAPA patients at a level approaching NLRC4-associated Macrophage Activation Syndrome (MAS) and well beyond Familial Mediterranean Fever. IL-18 elevation in PAPA patients’ sera persisted despite fluctuations in disease activity. IL-18 Binding Protein (IL-18BP) was modestly elevated, and as such PAPA patients had detectable free IL-18. PAPA patients did not develop MAS, and CXCL9 (an indicator of Interferon-gamma activity) was rarely elevated in their sera.ConclusionPAPA syndrome is a refractory, and often disabling monogenic autoinflammatory disease associated with chronic elevation of serum IL-18, but not risk for MAS. This finding instructs our understanding of the origins of excess IL-18, its potential spectrum of pathogenic effects, and the possible role for IL-18 blockade in refractory PAPA syndrome.

Published

2021

24. An immune-based biomarker signature is associated with mortality in COVID-19 patients

Author

Michael S. Abers, Ottavia M. Delmonte, Emily E. Ricotta, Jonathan Fintzi, Danielle L. Fink, Adriana A. Almeida de Jesus, Kol A. Zarember, Sara Alehashemi, Vasileios Oikonomou, Jigar V. Desai, Scott W. Canna, Bita Shakoory, Kerry Dobbs, Luisa Imberti, Alessandra Sottini, Eugenia Quiros-Roldan, Francesco Castelli, Camillo Rossi, Duilio Brugnoni, Andrea Biondi, Laura Rachele Bettini, Mariella D’Angio’, Paolo Bonfanti, Riccardo Castagnoli, Daniela Montagna, Amelia Licari, Gian Luigi Marseglia, Emily F. Gliniewicz, Elana Shaw, Dana E. Kahle, Andre T. Rastegar, Michael Stack, Katherine Myint-Hpu, Susan L. Levinson, Mark J. DiNubile, Daniel W. Chertow, Peter D. Burbelo, Jeffrey I. Cohen, Katherine R. Calvo, John S. Tsang, NIAID COVID-19 Consortium, Helen C. Su, John I. Gallin, Douglas B. Kuhns, Raphaela Goldbach-Mansky, Michail S. Lionakis, Luigi D. Notarangelo, Abers, M, Delmonte, O, Ricotta, E, Fintzi, J, Fink, D, de Jesus, A, Zarember, K, Alehashemi, S, Oikonomou, V, Desai, J, Canna, S, Shakoory, B, Dobbs, K, Imberti, L, Sottini, A, Quiros-Roldan, E, Castelli, F, Rossi, C, Brugnoni, D, Biondi, A, Bettini, L, D'Angio', M, Bonfanti, P, Castagnoli, R, Montagna, D, Licari, A, Marseglia, G, Gliniewicz, E, Shaw, E, Kahle, D, Rastegar, A, Stack, M, Myint-Hpu, K, Levinson, S, Dinubile, M, Chertow, D, Burbelo, P, Cohen, J, Calvo, K, Tsang, J, Su, H, Gallin, J, Kuhns, D, Goldbach-Mansky, R, Lionakis, M, and Notarangelo, L

Subjects

Male, 0301 basic medicine, Chemokine, Azithromycin, Chemokine CXCL9, Severity of Illness Index, 0302 clinical medicine, Adrenal Cortex Hormones, Medicine, Enzyme Inhibitors, Chemokine CCL2, Interleukin-15, biology, Lactoferrin, NF-kappa B, General Medicine, Middle Aged, Prognosis, Anti-Bacterial Agents, Interleukin-10, Matrix Metalloproteinase 9, Receptors, Tumor Necrosis Factor, Type I, 030220 oncology & carcinogenesis, Interferon Type I, Cytokines, Biomarker (medicine), CXCL9, Female, Chemokines, Research Article, Hydroxychloroquine, Adult, Immunology, CCL2, Antibodies, Monoclonal, Humanized, Antiviral Agents, S100A9, COVID-19, Interferon-gamma, 03 medical and health sciences, Immune system, Lipocalin-2, Calgranulin B, Humans, Immunologic Factors, Cytokine, Aged, Vascular Endothelial Growth Factor Receptor-1, Interleukin-6, SARS-CoV-2, business.industry, Gene Expression Profiling, Interleukin-1 Receptor-Like 1 Protein, Ferritin, 030104 developmental biology, Case-Control Studies, Ferritins, Multivariate Analysis, biology.protein, Interleukin-2, business, Biomarkers

Abstract

Immune and inflammatory responses to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) contribute to disease severity of coronavirus disease 2019 (COVID-19). However, the utility of specific immune-based biomarkers to predict clinical outcome remains elusive. Here, we analyzed levels of 66 soluble biomarkers in 175 Italian patients with COVID-19 ranging from mild/moderate to critical severity and assessed type I IFN-, type II IFN-, and NF-κB-dependent whole-blood transcriptional signatures. A broad inflammatory signature was observed, implicating activation of various immune and nonhematopoietic cell subsets. Discordance between IFN-α2a protein and IFNA2 transcript levels in blood suggests that type I IFNs during COVID-19 may be primarily produced by tissue-resident cells. Multivariable analysis of patients' first samples revealed 12 biomarkers (CCL2, IL-15, soluble ST2 [sST2], NGAL, sTNFRSF1A, ferritin, IL-6, S100A9, MMP-9, IL-2, sVEGFR1, IL-10) that when increased were independently associated with mortality. Multivariate analyses of longitudinal biomarker trajectories identified 8 of the aforementioned biomarkers (IL-15, IL-2, NGAL, CCL2, MMP-9, sTNFRSF1A, sST2, IL-10) and 2 additional biomarkers (lactoferrin, CXCL9) that were substantially associated with mortality when increased, while IL-1α was associated with mortality when decreased. Among these, sST2, sTNFRSF1A, IL-10, and IL-15 were consistently higher throughout the hospitalization in patients who died versus those who recovered, suggesting that these biomarkers may provide an early warning of eventual disease outcome.

Published

2021

25. Immunodeficiency and bone marrow failure with mosaic and germline TLR8 gain of function

Author

Marina Cella, Mary C. Dinauer, Elaine Kulm, Michelle A. Ritter, Jahnavi Aluri, Alicia Bach, Elise M. Rizzi, Christina Bemrich-Stolz, Maleewan Kitcharoensakkul, Magdalena Walkiewicz, Jack J. Bleesing, Yi Shan Lee, James A. Connelly, Amy M. Scurlock, Laura G. Schuettpelz, Marwan Shinawi, Shirley M. Abraham, Saara Kaviany, V. Koneti Rao, Jonathan D. Powell, Jeffrey J. Bednarski, Peggy L. Kendall, Luana Chiquetto Paracatu, Raphaela Goldbach-Mansky, Christopher D. Putnam, Michael T. Harmon, Adriana Almeida de Jesus, Scott W. Canna, Stacie M. Jones, Morgan Similuk, Matthew M. Demczko, Nermina Saucier, Suk See De Ravin, Michael Joyce, Molly P. Keppel, and Megan A. Cooper

Subjects

Adult, Male, Immunobiology and Immunotherapy, Adolescent, Pancytopenia, medicine.medical_treatment, T-Lymphocytes, Immunology, Neutropenia, Lymphocyte Activation, Biochemistry, Young Adult, Immune system, Immunity, medicine, Humans, Child, Immunodeficiency, Inflammation, B-Lymphocytes, business.industry, Mosaicism, Bone marrow failure, Immunologic Deficiency Syndromes, Infant, Cell Differentiation, Cell Biology, Hematology, Bone Marrow Failure Disorders, medicine.disease, Prognosis, Pedigree, Transplantation, Haematopoiesis, Cytokine, Toll-Like Receptor 8, Child, Preschool, Gain of Function Mutation, Cytokines, Female, business, Follow-Up Studies

Abstract

Inborn errors of immunity (IEI) are a genetically heterogeneous group of disorders with a broad clinical spectrum. Identification of molecular and functional bases of these disorders is important for diagnosis, treatment, and an understanding of the human immune response. We identified 6 unrelated males with neutropenia, infections, lymphoproliferation, humoral immune defects, and in some cases bone marrow failure associated with 3 different variants in the X-linked gene TLR8, encoding the endosomal Toll-like receptor 8 (TLR8). Interestingly, 5 patients had somatic variants in TLR8 with

Published

2020

26. Highways to hell: Mechanism-based management of cytokine storm syndromes

Author

Randy Q. Cron and Scott W. Canna

Subjects

0301 basic medicine, Cytotoxicity, Immunologic, Immunology, Context (language use), Systemic inflammation, Immunotherapy, Adoptive, Article, Lymphohistiocytosis, Hemophagocytic, 03 medical and health sciences, 0302 clinical medicine, Immunopathology, medicine, Immunology and Allergy, Animals, Humans, Inflammation, Hemophagocytic lymphohistiocytosis, business.industry, Macrophage Activation Syndrome, Interleukin-18, Cytokine Storm, medicine.disease, Systemic inflammatory response syndrome, Cytokine release syndrome, Biomarker, 030104 developmental biology, Virus Diseases, 030220 oncology & carcinogenesis, Hemophagocytic Lymphohistiocytosis, medicine.symptom, Cytokine storm, business, Cytokine Release Syndrome, Neuroscience

Abstract

Since the first textbook devoted to cytokine storm syndromes (CSSs) was published in 2019, the world has changed dramatically and the term's visibility has broadened. Herein, we define CSSs broadly to include life/organ-threatening systemic inflammation and immunopathology regardless of the context in which it occurs, recognizing that the indistinct borders of such a definition limit its utility. Nevertheless, we are focused on the pathomechanisms leading to CSSs, including impairment of granule-mediated cytotoxicity, specific viral infections, excess IL-18, and chimeric antigen receptor T-cell therapy. These mechanisms are often reflected in distinct clinical features, functional tests, and/or biomarker assessments. Moreover, these mechanisms often indicate specific, definitive treatments. This mechanism-focused organization is vital to both advancing the field and understanding the complexities in individual patients. However, increasing evidence suggests that these mechanisms interact and overlap. Likewise, the utility of a broad term such as "cytokine storm" is that it reflects a convergence on a systemic inflammatory phenotype that, regardless of cause or context, may be amenable to "inflammo-stabilization." CSS research must improve our appreciation of its various mechanisms and their interactions and treatments, but it must also identify the signs and interventions that may broadly prevent CSS-induced immunopathology.

Published

2020

27. Distinct interferon signatures and cytokine patterns define additional systemic autoinflammatory diseases

Author

Gulnara Nasrullayeva, Daniela Gerent Petry Piotto, Vafa Mammadova, Zuoming Deng, Vibke Lilleby, Annet van Royen-Kerkhof, Andreas Reiff, Troy R. Torgerson, Sara Taber, Mary Beth F. Son, Laura S. Finn, Anne Marie C. Brescia, Yangfeng Hou, Philip J. Hashkes, Marco Gattorno, Alexei A. Grom, Elizabeth Stringer, Marite Rygg, Lisa G. Rider, Eric P. Hanson, Eric J. Allenspach, Ruy Carrasco, Elizabeth A. Kessler, Susan Moir, Ian Ferguson, Edward M. Behrens, Bita Arabshahi, Heinrike Schmeling, Victoria R. Dimitriades, Theresa Wampler Muskardin, Polly J. Ferguson, Rolando Cimaz, Pascal Pillet, Adriana Almeida de Jesus, Maria Teresa Terreri, Andrew J. Oler, Pui Y. Lee, Liliana Bezrodnik, Laura B Lewandowski, Rita Jerath, Stephen R. Brooks, Bernadette Marrero, Tova Ronis, Hanna Kim, Amina Ahmed, Alice Y. Chan, Yuriy Stepanovskiy, Christiaan Scott, Angelique Biancotto, Nancy Pan, Ronald M. Laxer, Adam L Reinhardt, Yan Huang, Johannes Roth, Paul Dancey, Suzanne C. Li, Lakshmi N. Moorthy, Jason Dare, Gisella Seminario, Raphaela Goldbach-Mansky, Natasha M. Ruth, Gina A. Montealegre Sanchez, Grant S. Schulert, Gerd Horneff, Min Ae Lee-Kirsch, Seza Ozen, Daniel J. Kingsbury, Louise Malle, Susanne M. Benseler, Rafael Rivas-Chacon, Laura L. Tosi, Scott W. Canna, Ronit Herzog, Angela Rösen-Wolff, Katherine R. Calvo, Sharon Bout-Tabaku, Diane E. Brown, Jon M. Burnham, Andrew I. Shulman, Karen Onel, Cynthia J. Tifft, Christian M. Hedrich, Vidya Sivaraman, Marilynn Punaro, Kathleen M. O'Neil, Marietta DeGuzman, and María Soledad Caldirola

Subjects

0301 basic medicine, Male, Panniculitis, Immunology, Gene mutation, Pulmonary Alveolar Proteinosis, medicine.disease_cause, Medical and Health Sciences, LRBA, Autoimmune Diseases, Monogenic diseases, purl.org/becyt/ford/3.3 [https], 03 medical and health sciences, 0302 clinical medicine, Rare Diseases, Clinical Research, IKBKG, medicine, Genetics, Humans, 2.1 Biological and endogenous factors, Aetiology, Inflammation, Innate immunity, business.industry, Macrophage Activation Syndrome, Interstitial lung disease, Interleukin-18, General Medicine, Autoinflammatory interferonopathies, Immune dysregulation, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, Macrophage activation syndrome, Interferon Type I, Mutation, Aicardi–Goutières syndrome, purl.org/becyt/ford/3 [https], Female, Clinical Medicine, business, Genetic diseases

Abstract

BACKGROUND. Undifferentiated systemic autoinflammatory diseases (USAIDs) present diagnostic and therapeutic challenges. Chronic interferon (IFN) signaling and cytokine dysregulation may identify diseases with available targeted treatments. METHODS. Sixty-six consecutively referred USAID patients underwent underwent screening for the presence of an interferon signature using a standardized type-I IFN-response-gene score (IRG-S), cytokine profiling, and genetic evaluation by next-generation sequencing. RESULTS. Thirty-six USAID patients (55%) had elevated IRG-S. Neutrophilic panniculitis (40% vs. 0%), basal ganglia calcifications (46% vs. 0%), interstitial lung disease (47% vs. 5%), and myositis (60% vs. 10%) were more prevalent in patients with elevated IRG-S. Moderate IRG-S elevation and highly elevated serum IL-18 distinguished 8 patients with pulmonary alveolar proteinosis (PAP) and recurrent macrophage activation syndrome (MAS). Among patients with panniculitis and progressive cytopenias, 2 patients were compound heterozygous for potentially novel LRBA mutations, 4 patients harbored potentially novel splice variants in IKBKG (which encodes NF-κB essential modulator [NEMO]), and 6 patients had de novo frameshift mutations in SAMD9L. Of additional 12 patients with elevated IRG-S and CANDLE-, SAVI- or Aicardi-Goutières syndrome-like (AGS-like) phenotypes, 5 patients carried mutations in either SAMHD1, TREX1, PSMB8, or PSMG2. Two patients had anti-MDA5 autoantibody-positive juvenile dermatomyositis, and 7 could not be classified. Patients with LRBA, IKBKG, and SAMD9L mutations showed a pattern of IRG elevation that suggests prominent NF-κB activation different from the canonical interferonopathies CANDLE, SAVI, and AGS. CONCLUSIONS. In patients with elevated IRG-S, we identified characteristic clinical features and 3 additional autoinflammatory diseases: IL-18-mediated PAP and recurrent MAS (IL-18PAP-MAS), NEMO deleted exon 5-autoinflammatory syndrome (NEMO-NDAS), and SAMD9L-associated autoinflammatory disease (SAMD9L-SAAD). The IRG-S expands the diagnostic armamentarium in evaluating USAIDs and points to different pathways regulating IRG expression. Fil: de Jesus, Adriana A.. National Institute Of Allergy And Infectious Diseases; Estados Unidos Fil: Hou, Yangfeng. Shandong University; China Fil: Brooks, Stephen. National Institute Of Arthritis And Musculoskeletal And Skin Diseases; Estados Unidos Fil: Malle, Louise. cahn School of Medicine at Mount Sinai; Estados Unidos Fil: Biancotto, Angelique. No especifíca; Fil: Huang, Yan. National Institute Of Allergy And Infectious Diseases; Estados Unidos Fil: Calvo, Katherine R.. National Institutes of Health; Estados Unidos Fil: Marrero, Bernadette. No especifíca; Fil: Moir, Susan. No especifíca; Fil: Oler, Andrew J.. National Institute Of Allergy And Infectious Diseases ; Estados Unidos Fil: Deng, Zuoming. National Institute Of Arthritis And Musculoskeletal And Skin Diseases; Estados Unidos Fil: Montealegre Sanchez, Gina A.. National Institute Of Allergy And Infectious Diseases ; Estados Unidos Fil: Ahmed, Amina. No especifíca; Fil: Allenspach, Eric. Washington State University; Estados Unidos Fil: Arabshahi, Bita. Virginia Commonwealth University; Estados Unidos Fil: Behrens, Edward. University of Pennsylvania; Estados Unidos Fil: Benseler, Susanne. University of Calgary; Canadá Fil: Bezrodnik, Liliana. Gobierno de la Ciudad de Buenos Aires. Hospital General de Niños "Ricardo Gutiérrez"; Argentina. Consejo Nacional de Investigaciones Científicas y Técnicas; Argentina Fil: Bout Tabaku, Sharon. No especifíca; Fil: Brescia, AnneMarie C.. No especifíca; Fil: Brown, Diane. No especifíca; Fil: Burnham, Jon M.. University of Pennsylvania; Estados Unidos Fil: Caldirola, Maria Soledad. Gobierno de la Ciudad de Buenos Aires. Hospital General de Niños "Ricardo Gutiérrez"; Argentina. Gobierno de la Ciudad de Buenos Aires. Instituto Multidisciplinario de Investigaciones en Patologías Pediátricas. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Houssay. Instituto Multidisciplinario de Investigaciones en Patologías Pediátricas; Argentina Fil: Carrasco, Ruy. No especifíca; Fil: Chan, Alice Y.. University of California; Estados Unidos Fil: Cimaz, Rolando. Università degli Studi di Milano; Italia Fil: Dancey, Paul. Janeway Children's Hospital And Rehabilitation Centre; Canadá Fil: Dare, Jason. University of Arkansas for Medical Sciences; Estados Unidos Fil: DeGuzman, Marietta. Baylor College Of Medicine; Estados Unidos Fil: Dimitriades, Victoria. No especifíca; Fil: Ferguson, Ian. University of Yale. School of Medicine; Estados Unidos Fil: Ferguson, Polly. University of Iowa; Estados Unidos Fil: Finn, Laura. University of Washington; Estados Unidos Fil: Gattorno, Marco. No especifíca; Fil: Grom, Alexei A.. No especifíca; Fil: Hanson, Eric P.. No especifíca; Fil: Hashkes, Philip J.. No especifíca; Fil: Hedrich, Christian M.. University of Liverpool; Reino Unido Fil: Herzog, Ronit. University of New York; Estados Unidos Fil: Horneff, Gerd. Universitat zu Köln; Alemania Fil: Jerath, Rita. Augusta University; Estados Unidos Fil: Kessler, Elizabeth. University of Missouri; Estados Unidos Fil: Kim, Hanna. No especifíca; Fil: Kingsbury, Daniel J.. No especifíca; Fil: Laxer, Ronald M.. University Of Toronto. Hospital For Sick Children; Canadá Fil: Lee, Pui Y.. Children's Hospital Boston; Estados Unidos Fil: Lee Kirsch, Min Ae. Technische Universität Dresden; Alemania Fil: Lewandowski, Laura. No especifíca; Fil: Li, Suzanne. Hackensack University Medical Center; Estados Unidos Fil: Lilleby, Vibke. Oslo University Hospital; Noruega Fil: Mammadova, Vafa. Azerbaijan Medical University; Azerbaiyán Fil: Moorthy, Lakshmi N.. Robert Wood Johnson Medical School; Estados Unidos Fil: Nasrullayeva, Gulnara. Azerbaijan Medical University; Azerbaiyán Fil: O'Neil, Kathleen M.. Riley Hospital for Children; Estados Unidos Fil: Onel, Karen. Hospital for Special Surgery; Estados Unidos Fil: Ozen, Seza. Hacettepe University; Turquía Fil: Pan, Nancy. Hospital for Special Surgery; Estados Unidos Fil: Pillet, Pascal. Children Hospital Pellegrin-Enfants; Francia Fil: Piotto, Daniela G.P.. Universidade Federal de Sao Paulo; Brasil Fil: Punaro, Marilynn G.. University of Texas; Estados Unidos Fil: Reiff, Andreas. University of Nebraska; Estados Unidos Fil: Reinhardt, Adam. University of Nebraska; Estados Unidos Fil: Rider, Lisa G.. No especifíca; Fil: Rivas Chacon, Rafael. Nicklaus Children’s Hospital; Estados Unidos Fil: Ronis, Tova. Children’s National Health System; Estados Unidos Fil: Rösen Wolff, Angela. Technische Universität Dresden; Alemania Fil: Roth, Johannes. Children’s Hospital of Eastern Ontario; Canadá Fil: Mckerran Ruth, Natasha. Medical University of South Carolina; Estados Unidos Fil: Rygg, Marite. Norwegian University of Science and Technology; Noruega Fil: Schmeling, Heinrike. University of Calgary; Canadá Fil: Schulert, Grant. Children’s Hospital Medical Center; Estados Unidos Fil: Scott, Christiaan. University of Cape Town; Sudáfrica Fil: Seminario, Gisella. Gobierno de la Ciudad de Buenos Aires. Hospital General de Niños "Ricardo Gutiérrez"; Argentina Fil: Shulman, Andrew. University of California at Irvine; Estados Unidos Fil: Sivaraman, Vidya. Nationwide Children’s Hospital; Estados Unidos Fil: Son, Mary Beth. Boston Children’s Hospital; Estados Unidos Fil: Stepanovskiy, Yuriy. Shupyk National Medical Academy for Postgraduate Education; Ucrania Fil: Stringer, Elizabeth. Dalhousie University Halifax; Canadá Fil: Taber, Sara. Hospital for Special Surgery; Estados Unidos Fil: Terreri, Maria Teresa. Universidade Federal de Sao Paulo; Brasil Fil: Tifft, Cynthia. No especifíca; Fil: Torgerson, Troy. University of Washington; Estados Unidos Fil: Tosi, Laura. Children’s National Health System; Estados Unidos Fil: van Royen Kerkhof, Annet. Wilhelmina Children’s Hospital Utrech; Países Bajos Fil: Wampler Muskardin, Theresa. New York University School of Medicine; Estados Unidos Fil: Canna, Scott W.. University of Pittsburgh; Estados Unidos Fil: Goldbach Mansky, Raphaela. National Institute Of Allergy And Infectious Diseases ; Estados Unidos

Published

2020

28. Interleukin-18 diagnostically distinguishes and pathogenically promotes human and murine macrophage activation syndrome

Author

Dirk Foell, Alexei A. Grom, Tomoaki Hoshino, Zeshan Tariq, Stephan Ehl, Dirk Holzinger, Jennifer Picarsic, Sandra Ammann, Charlotte Girard-Guyonvarc'h, Eduardo Schiffrin, Adriana Almeida de Jesus, Raphaela Goldbach-Mansky, Cem Gabay, Scott W. Canna, and Eric S. Weiss

Subjects

0301 basic medicine, Genetically modified mouse, Immunobiology and Immunotherapy, Immunology, Medizin, Biochemistry, Mice, 03 medical and health sciences, Downregulation and upregulation, NLRC4, Animals, Humans, Medicine, Cytotoxic T cell, ddc:616, Hemophagocytic lymphohistiocytosis, business.industry, Macrophage Activation Syndrome, Interleukin-18, Inflammasome, Cell Biology, Hematology, medicine.disease, 030104 developmental biology, Macrophage activation syndrome, Cytokines, Interleukin 18, business, medicine.drug

Abstract

Hemophagocytic lymphohistiocytosis (HLH) and macrophage activation syndrome (MAS) are life-threatening hyperferritinemic systemic inflammatory disorders. Although profound cytotoxic impairment causes familial HLH (fHLH), the mechanisms driving non-fHLH and MAS are largely unknown. MAS occurs in patients with suspected rheumatic disease, but the mechanistic basis for its distinction is unclear. Recently, a syndrome of recurrent MAS with infantile enterocolitis caused by NLRC4 inflammasome hyperactivity highlighted the potential importance of interleukin-18 (IL-18). We tested this association in hyperferritinemic and autoinflammatory patients and found a dramatic correlation of MAS risk with chronic (sometimes lifelong) elevation of mature IL-18, particularly with IL-18 unbound by IL-18 binding protein, or free IL-18. In a mouse engineered to carry a disease-causing germ line NLRC4(T337S) mutation, we observed inflammasome-dependent, chronic IL-18 elevation. Surprisingly, this NLRC4(T337S)-induced systemic IL-18 elevation derived entirely from intestinal epithelia. NLRC4(T337S) intestines were histologically normal but showed increased epithelial turnover and upregulation of interferon-γ–induced genes. Assessing cellular and tissue expression, classical inflammasome components such as Il1b, Nlrp3, and Mefv predominated in neutrophils, whereas Nlrc4 and Il18 were distinctly epithelial. Demonstrating the importance of free IL-18, Il18 transgenic mice exhibited free IL-18 elevation and more severe experimental MAS. NLRC4(T337S) mice, whose free IL-18 levels were normal, did not. Thus, we describe a unique connection between MAS risk and chronic IL-18, identify epithelial inflammasome hyperactivity as a potential source, and demonstrate the pathogenicity of free IL-18. These data suggest an IL-18–driven pathway, complementary to the cytotoxic impairment of fHLH, with potential as a distinguishing biomarker and therapeutic target in MAS.

Published

2018

29. A20 haploinsufficiency (HA20): clinical phenotypes and disease course of patients with a newly recognised NF-kB-mediated autoinflammatory disease

Author

Daniella M. Schwartz, Daniel L. Kastner, Florence A. Aeschlimann, Ronald M. Laxer, Ivona Aksentijevich, Patrycja Hoffmann, Helen L. Leavis, Ellen Go, Deborah L. Stone, Seza Ozen, Ahmet Gül, Ezgi Deniz Batu, Annet Van Royen-Kerkof, and Scott W. Canna

Subjects

0301 basic medicine, medicine.medical_specialty, Anti-nuclear antibody, Immunology, Lupus nephritis, Disease, Systemic inflammation, Biochemistry, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, autoinflammatory disease, Rheumatology, Internal medicine, medicine, Immunology and Allergy, Sex organ, ulcers, 030203 arthritis & rheumatology, Biochemistry, Genetics and Molecular Biology(all), business.industry, Autoantibody, medicine.disease, pediatric rheumatology, 030104 developmental biology, medicine.symptom, Haploinsufficiency, business, Genetics and Molecular Biology(all)

Abstract

ObjectivesThe association between mutations in TNFAIP3, encoding the NF-kB regulatory protein A20, and a new autoinflammatory disease has recently been recognised. This study aims at describing the clinical phenotypes and disease course of patients with A20 haploinsufficiency (HA20).MethodsData for all cases from the initial publication, and additional cases identified through collaborations since, were collected using standardised data collection forms.ResultsA total of 16 patients (13 female) from seven families with a genetic diagnosis of HA20 were included. The disease commonly manifested in early childhood (range: first week of life to 29 years of age). The main clinical symptoms were recurrent oral, genital and/or gastrointestinal ulcers (16/16), musculoskeletal (9/16) and gastrointestinal complaints (9/16), cutaneous lesions (8/16), episodic fever (7/16), and recurrent infections (7/16). Clinical phenotypes varied considerably, even within families. Relapsing-remitting disease course was most common, and one patient died. Laboratory abnormalities included elevated acute-phase reactants and fluctuating presence of various autoantibodies such as antinuclear antibodies (4/10 patients tested) and anti-dsDNA (2/5). Tissue biopsy of different sites revealed non-specific chronic inflammation (6/12 patients tested), findings consistent with class V lupus nephritis in one patient, and pustules and normal results in two patients each. All patients were treated: 4/16 received colchicine and 12/16 various immunosuppressive agents. Cytokine inhibitors effectively suppressed systemic inflammation in 7/9 patients.ConclusionsEarly-onset recurrent oral, genital and/or gastrointestinal ulcers are the hallmark feature of HA20. Frequency and intensity of other clinical manifestations varied highly. Treatment regimens should be based on disease severity, and cytokine inhibitors are often required to control relapses.

Published

2018

30. NLRC4 inflammasomopathies

Author

Neil Romberg, Tiphanie P. Vogel, and Scott W. Canna

Subjects

Inflammation, 0301 basic medicine, Urticaria, Inflammasomes, Calcium-Binding Proteins, Immunology, Interleukin-18, Article, Autoimmune Diseases, CARD Signaling Adaptor Proteins, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, 030220 oncology & carcinogenesis, Mutation, Biomarkers, Tumor, Animals, Humans, Immunology and Allergy

Abstract

The purpose of the review is to highlight developments in autoinflammatory diseases associated with gain-of-function mutations in the gene encoding NLR-family CARD-containing protein 4 (NLRC4), the NLRC4-inflammasomopathies.Three years since the identification of the first autoinflammation with infantile enterocolitis (AIFEC) patients, there is an improved understanding of how the NLRC4 inflammasome and interleukin 18 (IL-18) contribute to gut inflammation in myeloid and also intestinal epithelial cells. This information has opened new therapeutic avenues to treat AIFEC patients with targeted agents like recombinant IL-18 binding protein and antiinterferon-γ antibodies. Additional phenotypes traditionally associated with NLRP3 mutations like familial cold autoinflammatory syndrome and neonatal onset multisystem inflammatory disease (NOMID), have now also been associated with gain-of-function NLRC4 mutations. Finally, NLRC4 somatic mosaicism has now been identified in a NOMID and an AIFEC patient, a finding emphasizing nontraditional modes of inheritance in autoinflammatory diseases.The NLRC4 inflammasomopathies constitute a growing autoinflammatory disease category that spans a broad clinical spectrum from cold urticaria to NOMID and the often fatal disease AIFEC. Rapid case identification with biomarkers like elevated serum IL-18 concentrations and early intervention with targeted immunomodulatory therapies are key strategies to improving outcomes for AIFEC patients.

Published

2017

31. No shortcuts: new findings reinforce why nuance is the rule in genetic autoinflammatory syndromes

Author

Scott W. Canna and Paul Tsoukas

Subjects

Inflammation, 0301 basic medicine, Cognitive science, Inflammasomes, business.industry, Hereditary Autoinflammatory Diseases, Autoimmunity, Pyrin, 03 medical and health sciences, Phenotype, 030104 developmental biology, Rheumatology, Mutation, Humans, Medicine, Dose effect, business

Abstract

Purpose of review Practitioners dazed by the evolving concept of autoinflammation are in good company. Despite the clinical challenges autoinflammatory patients present, their study has been fundamental to our understanding of basic human inflammation. This review will focus on the ways in which recent discoveries in genetically mediated autoinflammation broaden and refine the concept. Recent findings Major developments in pyrin inflammasome biology, defective ubiquitination, and the hyperferritinemic syndromes will be highlighted. Summary We offer a brief discussion of discordance, convergence, genotype, and phenotype in autoinflammation. Additionally, we introduce the concepts of mutation dose effect and hybrid nomenclature. Overall, we hope to provide an update on developments in the field of autoinflammation, some conceptual tools to help navigate the rising tide of discovery, and some encouragement that keeping up with developments in autoinflammation is both exciting and necessary.

Published

2017

32. A novel Pyrin-Associated Autoinflammation with Neutrophilic Dermatosis mutation further defines 14-3-3 binding of pyrin and distinction to Familial Mediterranean Fever

Author

Fiona Moghaddas, Seth L. Masters, Rafael Llamas, Paul J. Baker, Juan J Martinez-Garcia, Pablo Pelegrín, Scott W. Canna, Ian P. Wicks, Vanessa Gargallo, Juan I. Aróstegui, Pablo Mesa-del-Castillo, Helios Martínez-Banaclocha, Anna Mensa-Vilaro, and Dominic De Nardo

Subjects

Lipopolysaccharides, 0301 basic medicine, medicine.medical_treatment, Immunology, Caspase 1, Familial Mediterranean fever, PAAND, Plasma protein binding, Biology, Peripheral blood mononuclear cell, Pyrin domain, Article, General Biochemistry, Genetics and Molecular Biology, Diagnosis, Differential, 03 medical and health sciences, FMF, autoinflammatory disease, Rheumatology, medicine, Humans, Immunology and Allergy, 14-3-3, Hereditary Autoinflammatory Diseases, Pyrin, Flow Cytometry, MEFV, medicine.disease, Sweet Syndrome, Familial Mediterranean Fever, 030104 developmental biology, Cytokine, 14-3-3 Proteins, Case-Control Studies, Mutation, Leukocytes, Mononuclear, Cytokines, Inflammasome complex, Protein Binding

Abstract

ObjectivePyrin-Associated Autoinflammation with Neutrophilic Dermatosis (PAAND) is a recently described monogenic autoinflammatory disease. The causal p.S242RMEFVmutation disrupts a binding motif of the regulatory 14-3-3 proteins within pyrin. Here, we investigate a family with clinical features consistent with PAAND in whom the novel p.E244KMEFVmutation, located in the +2 site of the 14-3-3 binding motif in pyrin, has been found.MethodsMultiplex cytokine analyses were performed on p.E244K patient and control serum. Peripheral blood mononuclear cells were stimulated ex vivo with lipopolysaccharide (LPS). In vitro, inflammasome complex formation was evaluated by flow cytometry of Apoptosis-associated Speck-like protein containing a Caspase recruitment domain (ASC) specks. Interleukin-1β (IL-1β) and IL-18 production was quantified by ELISA. The ability of the p.E244K pyrin mutation to interact with 14-3-3 was assessed by immunoprecipitation.ResultsPAAND p.E244K patient serum displayed a different cytokine profile compared with patients with Familial Mediterranean Fever (FMF). In overexpression models, p.E244K pyrin was associated with decreased 14-3-3 binding and increased ASC speck formation. THP-1 monocytes expressing PAAND pyrin mutations demonstrated spontaneous caspase-1-dependent IL-1β and IL-18 secretion, as well as cell death, which were significantly greater than those of wild-type and the FMF-associated mutation p.M694V.ConclusionIn PAAND, disruption of the +2 position of a 14-3-3 binding motif in pyrin results in its constitutive activation, with spontaneous production of IL-1β and IL-18, associated with inflammatory cell death. The altered serum cytokine profile may explain the different clinical features exhibited by PAAND patients compared with those with FMF.

Published

2017

33. Should COVID-19 take advice from rheumatologists?

Author

Scott W. Canna and Kate F. Kernan

Subjects

medicine.medical_specialty, 2019-20 coronavirus outbreak, Rheumatology, Coronavirus disease 2019 (COVID-19), business.industry, Family medicine, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, medicine, Immunology and Allergy, business, Article, Advice (programming)

Published

2020

34. A novel de novo NLRC4 mutation reinforces the likely pathogenicity of specific LRR domain mutation

Author

Scott W. Canna, Adiratna Mat Ripen, Saharuddin B. Mohamad, Munirah Hishamshah, Revathy Nallusamy, Mohd Farid Baharin, Chai Teng Chear, Hamidah Ghani, and Kwai Cheng Chan

Subjects

0301 basic medicine, Skin erythema, Fever, In silico, Immunology, Gene mutation, Biology, medicine.disease_cause, Chemokine CXCL9, Autoimmune Diseases, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Protein Domains, NLRC4, medicine, Immunology and Allergy, Missense mutation, Humans, Child, Exome sequencing, Sanger sequencing, Genetics, Mutation, Arthritis, Calcium-Binding Proteins, Interleukin-18, Syndrome, CARD Signaling Adaptor Proteins, 030104 developmental biology, Erythema, symbols, Female, 030215 immunology

Abstract

Autoinflammatory disorders are characterized by dysregulated innate immune response, resulting in recurrent uncontrolled systemic inflammation and fever. Gain-of-function mutations in NLRC4 have been described to cause a range of autoinflammatory disorders. We report a twelve-year-old Malay girl with recurrent fever, skin erythema, and inflammatory arthritis. Whole exome sequencing and subsequent bidirectional Sanger sequencing identified a heterozygous missense mutation in NLRC4 (NM_001199138: c.1970A > T). This variant was predicted to be damaging in silico, was absent in public and local databases and occurred in a highly conserved residue in the leucine-rich repeat (LRR) domain. Cytokine analysis showed extremely high serum IL-18 and IL-18/CXCL9 ratio, consistent with other NLRC4-MAS patients. In summary, we identified the first patient with a novel de novo heterozygous NLRC4 gene mutation contributing to autoinflammatory disease in Malaysia. Our findings reinforce the likely pathogenicity of specific LRR domain mutations in NLRC4 and expand the clinical spectrum of NLRC4 mutations.

Published

2019

35. P127 Lung disease in systemic JIA: an emerging problem linked with young age and anti-IL-1/IL-6

Author

Scott W. Canna, Mark M. Davis, Gill Bejerano, Gail H. Deutsch, Ann N. Leung, RP Guillerman, Vivian E. Saper, Purvesh Khatri, Johannes Birgmeier, Grant S. Schulert, Elizabeth D. Mellins, A. Grom, Guangbo Chen, Ying Lu, and Karthik A. Jagadeesh

Subjects

medicine.medical_specialty, business.industry, Retrospective cohort study, Disease, medicine.disease, Rash, chemistry.chemical_compound, Tocilizumab, chemistry, Internal medicine, Cohort, medicine, Etiology, medicine.symptom, Complication, Pulmonary alveolar proteinosis, business

Abstract

Career situation of first and presenting author Post-doctoral fellow. Introduction The advent of anti-IL-1/IL-6 therapies transformed the management of systemic juvenile idiopathic arthritis (sJIA), a debilitating childhood inflammatory condition. However, concurrent with practice change, pediatric rheumatologists noted an increase in sporadic cases of types of lung disease in sJIA, that were rarely seen in previous decades. Objectives The study aims to provide an up-to-date characterization of lung disease and identify novel risk factors. Methods We organized a multi-center retrospective study and obtained information on 61 cases of lung disease in children with sJIA or sJIA-like disease. Results Clinical data from our cohort showed that lung disease in the setting of sJIA is associated with distinctive features, including acute clubbing (in 61%), atypical rash (in 56%) and an unusually high frequency of serious adverse reactions to tocilizumab (40%, OR=79 compared to the control). This lung disease has unique radiological findings and lung pathology similar to pulmonary alveolar proteinosis and/or endogenous lipoid pneumonia (PAP/ELP, 64%) often with associated pulmonary vascular changes. Whole-exome sequencing on 18 patients ruled out a novel monogenic disorder or known causes of congenital PAP. Thus, the etiology of the disease is not clear, while its mortality is high (5 years survival: 42%, 25%–68%). When compared to a control cohort of children entered as sJIA in a patient registry, the lung disease cohort has similar overall anti-IL-1/IL-6 exposure level. However, in the anti-IL-1/IL-6 exposed subset, but not in the non-exposed, young sJIA onset age potently increased the risk of lung disease (age Conclusions Lung disease associated with anti-IL-1/anti-IL-6 therapies often presents as an alveolar and pulmonary vascular complication with high mortality in children with sJIA/sJIA-like disease. Risk is significantly increased in children with young age at sJIA onset or concurrent T21. In sJIA patients (including those with initial treatment response), emergence of atypical clinical features, rising ferritin and dropping absolute lymphocyte count should raise suspicion of this complication. Disclosure of Interest G. Chen: None declared, V. Saper: None declared, G. Deutsch: None declared, R. P. Guillerman: None declared, K. Jagadeesh: None declared, G. Schulert: None declared, S. Canna: None declared, Y. Lu: None declared, J. Birgmeier: None declared, A. Leung: None declared, A. Grom: None declared, G. Bejerano : None declared, M. Davis: None declared, P. Khatri: None declared, E. Mellins Grant/research support from: Novartis, GlaxoSmithKline, Codexis, Inc.

Published

2019

36. Other Rare Monogenic Autoinflammatory Diseases

Author

Isabelle Jéru, Eric P. Hanson, and Scott W. Canna

Subjects

Rapid identification, business.industry, Medicine, Identification (biology), In patient, business, Bioinformatics, Autoinflammatory Disorders

Abstract

Over the past decade, major advances have been m`ade in understanding the molecular and cellular bases leading to autoinflammatory diseases, and a number of very rare entities have been described. Next-generation sequencing technologies led to the rapid identification of a number of additional genes responsible for syndromes observed in only a very small number of families or in sporadic cases. The identification of all these new genes and associated molecular pathways underlines that activation of interleukin (IL)-1β signaling is far from being the only pathogenic process involved in autoinflammatory disorders. Genetic defects found in patients with rare monogenic autoinflammatory diseases might also facilitate the study of common autoinflammatory diseases with a genetic component. Since these disorders affect multiple organs with potentially severe complications, management of patients is complex and warrants a multidisciplinary approach. Finally, it is necessary to translate discoveries of the pathophysiology of these conditions into more effective therapies, since the choice of therapeutic options often remains empirical.

Published

2019

37. NLRC4-Associated Autoinflammatory Diseases

Author

Scott W. Canna

Subjects

NLRC4, business.industry, Immunology, Medicine, business

Published

2019

38. The Intersections of Autoinflammation and Cytokine Storm

Author

Scott W. Canna

Subjects

Hemophagocytic lymphohistiocytosis, Innate immune system, business.industry, animal diseases, medicine.medical_treatment, Pyroptosis, Immune dysregulation, medicine.disease, medicine.disease_cause, Cytokine, NLRC4, Immunology, medicine, Interleukin 18, business, Cytokine storm

Abstract

Autoinflammation is a category of human immune dysregulation best exemplified by inborn errors in genes important for innate immunity. Though overproduction of cytokines is a mechanistic feature of most autoinflammatory diseases, only a few have been associated with the phenotype of Cytokine Storm. Rarely, the most severe presentations of some canonical autoinflammatory diseases have featured cytokine storm. Innate immune activation is also part of the pathogenesis of canonical cytokine storm disorders, like hemophagocytic lymphohistiocytosis. More recently, biomarker, mechanistic, and early treatment studies in patients with Still’s disease, or with NLRC4 or XIAP mutations, have placed the inflammasome-activated cytokine IL-18 at the center of the intersection of autoinflammation and cytokine storm.

Published

2019

39. Janus kinase inhibition lessens inflammation and ameliorates disease in murine models of hemophagocytic lymphohistiocytosis

Author

Ross L. Levine, Edward M. Behrens, Leslee Sprague, Peng Guan, Makoto Kurachi, E. John Wherry, Scott W. Canna, Rupali Das, Qi Angel An, Paige Tedrick, Kim E. Nichols, Katherine Verbist, and Cheng Cheng

Subjects

0301 basic medicine, Ruxolitinib, medicine.medical_treatment, Immunology, Inflammation, Lymphocyte Activation, Lymphocytic choriomeningitis, Biochemistry, Lymphohistiocytosis, Hemophagocytic, Proinflammatory cytokine, Mice, 03 medical and health sciences, 0302 clinical medicine, Chlorocebus aethiops, Nitriles, medicine, Animals, Vero Cells, Cells, Cultured, Janus Kinases, Mice, Knockout, Hemophagocytic lymphohistiocytosis, biology, Perforin, business.industry, Cell Biology, Hematology, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Pyrimidines, 030104 developmental biology, Cytokine, 030220 oncology & carcinogenesis, biology.protein, Pyrazoles, CpG Islands, medicine.symptom, business, Janus kinase, medicine.drug

Abstract

Hemophagocytic lymphohistiocytosis (HLH) comprises an emerging spectrum of inherited and noninherited disorders of the immune system characterized by the excessive production of cytokines, including interferon-γ and interleukins 2, 6, and 10 (IL-2, IL-6, and IL-10). The Janus kinases (JAKs) transduce signals initiated following engagement of specific receptors that bind a broad array of cytokines, including those overproduced in HLH. Based on the central role for cytokines in the pathogenesis of HLH, we sought to examine whether the inhibition of JAK function might lessen inflammation in murine models of the disease. Toward this end, we examined the effects of JAK inhibition using a model of primary (inherited) HLH in which perforin-deficient (Prf1(-∕-)) mice are infected with lymphocytic choriomeningitis virus (LCMV) and secondary (noninherited) HLH in which C57BL/6 mice receive repeated injections of CpG DNA. In both models, treatment with the JAK1/2 inhibitor ruxolitinib significantly lessened the clinical and laboratory manifestations of HLH, including weight loss, organomegaly, anemia, thrombocytopenia, hypercytokinemia, and tissue inflammation. Importantly, ruxolitinib treatment also significantly improved the survival of LCMV-infectedPrf1(-∕-)mice. Mechanistic studies revealed that in vivo exposure to ruxolitinib inhibited signal transducer and activation of transcription 1-dependent gene expression, limited CD8(+)T-cell expansion, and greatly reduced proinflammatory cytokine production, without effecting degranulation and cytotoxic function. Collectively, these findings highlight the JAKs as novel, druggable targets for mitigating the cytokine-driven hyperinflammation that occurs in HLH. These observations also support the incorporation of JAK inhibitors such as ruxolitinib into future clinical trials for patients with these life-threatening disorders.

Published

2016

40. Editorial: 21st Century Storm Chasers: Defining Macrophage Activation Syndrome

Author

Peter A. Nigrovic and Scott W. Canna

Subjects

030203 arthritis & rheumatology, 0301 basic medicine, Extramural, business.industry, Immunology, MEDLINE, Arthritis, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Rheumatology, Macrophage activation syndrome, medicine, Immunology and Allergy, business

Published

2016

41. 1690: COMPUTATIONAL MODELING OF SEPSIS-ASSOCIATED MACROPHAGE ACTIVATION SYNDROME

Author

Joseph A. Carcillo, Gilles Clermont, Robert S. Parker, Zachary Aldewereld, and Scott W. Canna

Subjects

Sepsis, business.industry, Macrophage activation syndrome, Immunology, Medicine, Critical Care and Intensive Care Medicine, business, medicine.disease

Published

2020

42. New monogenic autoinflammatory diseases—a clinical overview

Author

Raphaela Goldbach-Mansky and Scott W. Canna

Subjects

Proteasome Endopeptidase Complex, Cellular differentiation, Immunology, Inflammation, Biology, medicine.disease_cause, Article, Autoimmune Diseases, Autoimmunity, medicine, Humans, Immunology and Allergy, Myositis, Immunodeficiency, Macrophage Activation Syndrome, Hereditary Autoinflammatory Diseases, Interleukin-18, Interstitial lung disease, medicine.disease, Phenotype, Macrophage activation syndrome, Mutation, Interferons, medicine.symptom, Organ Specificity, Signal Transduction

Abstract

Translating pathogenic insights gained from mono- genic defects that cause autoinflammatory diseases into novel therapies has dramatically improved the lives of patients with thesesyndromes.Thelast15yearshavefocusedonthecentral role of IL-1 in driving autoinflammatory phenotypes and on therapies blocking IL-1 signaling. Recent discoveries from patients unresponsive to IL-1 blockade have highlighted other key inflammatory mediators and pathways. New genetic dis- coveries have confirmed unifying mechanisms of autoinflammation, including dysregulation of danger sensing, cell stress, and immune-receptor signaling. Recent gene dis- covery in novel diseases has demonstrated new concepts. First, several complex clinical syndromes, caused by muta- tions leading to chronic type I interferon (IFN) production present with organ manifestations different from IL-1 mediat- ed diseases including cerebral calcifications, myositis, and interstitial lung disease and the frequent occurrence of auto- antibodies. These disorders introduce type I IFN' sa s inflam- matory mediators that cause autoinflammatory phenotypes. Second, conditions associated with high IL-18 production may provide a direct linkbetween autoinflammation and mac- rophage activation syndrome. Third, dysregulation of inflam- matory and cell differentiation pathways in nonhematopoietic cells, such as aberrant calcium signaling and impaired endo- thelial or keratinocyte development, provide an understanding of organ specificity in autoinflammatory disorders. Many of these discoveries highlight the intricate interconnections be- tween autoinflammation, autoimmunity, immunodeficiency, and lymphoproliferation and suggest ways in which we may better diagnose and treat autoinflammatory diseases.

Published

2015

43. The NLRC4 Inflammasome

Author

Scott W. Canna and Joseph A. Duncan

Subjects

0301 basic medicine, Inflammasomes, Immunology, Familial Mediterranean fever, Biology, Infections, Pyrin domain, Article, Autoimmune Diseases, 03 medical and health sciences, 0302 clinical medicine, NLRC4, medicine, Immunology and Allergy, Animals, Humans, Inflammation, Effector, Calcium-Binding Proteins, Inflammasome, Pyrin, medicine.disease, MEFV, Structure and function, Familial Mediterranean Fever, CARD Signaling Adaptor Proteins, 030104 developmental biology, 030220 oncology & carcinogenesis, NAIP, Neuroscience, medicine.drug, Signal Transduction

Abstract

15 years ago, the fundamental biology of an inflammatory signaling complex eventually dubbed “the inflammasome” began to unravel in chronologic parallel with the discovery that many inflammatory diseases were associated with its hyperactivity. Though the genetic origins of Familial Mediterranean Fever (FMF, caused my mutations in MEFV) were discovered first, it would take nearly two decades before the mechanistic connections to a Pyrin inflammasome were made1. In the interim, the intensive study of the NLRP3 inflammasome, and the diseases associated with its hyperactivation, have largely dictated the paradigm of inflammasome composition and function. Despite impressive gains, focusing on NLRP3 left gaps in our understanding of inflammasome biology. Foremost among these gaps were how inflammasomes become activated and the connections between inflammasome structure and function. Fortunately, work in another inflammasome inducer, NLRC4, grew to fill those gaps. The current understanding of the NLRC4 inflammasome is perhaps the most comprehensive illustration of the inflammasome paradigm: trigger (e.g. cytosolic flagellin), sensor (NAIP), nucleator (NLRC4), adaptor (ASC), and effector (CASP1). Detailed work has also identified observations that challenge this paradigm. Simultaneously, the features unique to each inflammasome offer a lesson in contrast, providing perspectives on inflammasome activation, regulation, and function. In this review, we endeavor to highlight recent breakthroughs related to NLRC4 inflammasome structure and activation, important in vivo work in infection and systemic inflammation, and the characterization of a spectrum of human NLRC4-associated autoinflammatory diseases.

Published

2017

44. Reply

Author

Scott W. Canna, Charlotte Girard, Louise Malle, Adriana de Jesus, Neil Romberg, Judith Kelsen, Lea F. Surrey, Pierre Russo, Andrew Sleight, Eduardo Schiffrin, Cem Gabay, Raphaela Goldbach-Mansky, and Edward M. Behrens

Subjects

Immunology, Mutation, Immunology and Allergy, Intercellular Signaling Peptides and Proteins, Carrier Proteins

Published

2017

45. Brief Report: Alternative Activation of Laser-Captured Murine Hemophagocytes

Author

Scott W. Canna, Kathleen E. Sullivan, William Bernal, Michele Paessler, Edward M. Behrens, Niansheng Chu, and Patrícia Costa-Reis

Subjects

CD64, Pathology, medicine.medical_specialty, Hemophagocytic lymphohistiocytosis, Immunology, Biology, medicine.disease, Haematopoiesis, medicine.anatomical_structure, Rheumatology, Macrophage activation syndrome, embryonic structures, medicine, Immunology and Allergy, Macrophage, Bone marrow, Hemophagocytosis, CD163

Abstract

Objective Hemophagocytes (HPCs) are activated macrophages that have engulfed other hematopoietic cells. Although HPCs are rarely identified in normal spleen tissue and bone marrow, an excess of these macrophages characterizes many cytokine storm syndromes, particularly macrophage activation syndrome and hemophagocytic lymphohistiocytosis. This study was undertaken to assess the functions of HPCs and their significance in acute inflammatory conditions. Methods HPCs were generated in wild-type mice using repeated stimulation with Toll-like receptor 9 (TLR-9) and interleukin-10 receptor blockade. RNA was extracted from HPCs that had been isolated by laser-captured microdissection. Transcriptional profiles of the HPCs were then compared to those of resting splenic macrophages. In addition, bone marrow samples were obtained from a diverse cohort of patients in whom excess hemophagocytosis was identified by clinical bone marrow biopsy or aspiration. The bone marrow samples were analyzed by immunohistochemistry for markers of classic (CD64) or alternative (CD163 and CD206) macrophage activation. Results Differential gene expression and gene set enrichment analyses of murine HPCs identified up-regulation of genes and gene sets associated with alternative activation of HPCs. Immunohistochemical analyses of HPCs in human bone marrow samples showed universal staining of HPCs for CD163, but rarely for CD206 or CD64. Conclusion Laser-captured murine TLR-9–induced HPCs had a transcriptional profile similar to that of alternatively activated macrophages. In addition, HPC expression of CD163 was confirmed in a uniquely diverse cohort of patients with hemophagocytic syndromes. Collectively, these data support the hypothesis that HPCs have both immunoregulatory and clean-up functions.

Published

2014

46. Editorial: Interferon-γ: Friend or Foe in Systemic Juvenile Idiopathic Arthritis and Adult-Onset Still's Disease?

Author

Scott W. Canna

Subjects

Male, Adult-onset Still's disease, medicine.medical_treatment, Freund's Adjuvant, Immunology, Arthritis, Interferon-gamma, Immune system, Rheumatology, Interferon γ, Animals, Immunology and Allergy, Medicine, Juvenile, Interferon gamma, business.industry, medicine.disease, Arthritis, Juvenile, Disease Models, Animal, Cytokine, Immune System, Female, business, Autoinflammatory Disorders, medicine.drug

Abstract

We may know just enough about cytokines in autoinflammatory diseases to be dangerous. Insights from animal models and cell lines, observations from patient samples, and outcomes of directed cytokine modulating treatments constantly refine this understanding, while also unearthing deeper layers of complexity. The recent advances in our understanding of systemic autoinflammatory disorders have brought the interaction of basic cytokine biology and patient care to the fore.

Published

2014

47. Introduction: Autoinflammatory Syndromes Special Issue—hidden mysteries in the corners of autoinflammation

Author

Scott W. Canna and Raphaela Goldbach-Mansky

Subjects

Inflammation, 0301 basic medicine, Cognitive science, Biological Products, business.industry, Immunology, MEDLINE, Syndrome, General Medicine, Immunity, Innate, Receptors, Tumor Necrosis Factor, Autoimmune Diseases, 03 medical and health sciences, 030104 developmental biology, NLR Family, Pyrin Domain-Containing 3 Protein, Animals, Humans, Immunology and Allergy, Medicine, Featured Article of the Month, Immunotherapy, business, Interleukin-1, Introductory Journal Article

Published

2018

48. Severe autoinflammation in 4 patients with C-terminal variants in cell division control protein 42 homolog (CDC42) successfully treated with IL-1β inhibition

Author

A. Roy, Elizabeth D. Mellins, Daniel J. Lovell, Scott W. Canna, Laura K. Erdman, Claudia Macaubas, Adriana Almeida de Jesus, Susanna Talarico, Yael Gernez, Rosa Bacchetta, Michael Grimley, Hanouf Alsaleem, David B. Lewis, Karthik A. Jagadeesh, Raphaela Goldbach-Mansky, Sara Alehashemi, Katja G. Weinacht, and R. M. Laxer

Subjects

Terminal (electronics), business.industry, Immunology, Immunology and Allergy, Medicine, CDC42, Division (mathematics), business, Molecular biology, Article

Published

2019

49. Interferon-γ Mediates Anemia but Is Dispensable for Fulminant Toll-like Receptor 9-Induced Macrophage Activation Syndrome and Hemophagocytosis in Mice

Author

Michele Paessler, Portia A. Kreiger, Niansheng Chu, Scott W. Canna, Edward M. Behrens, and Julia Wrobel

Subjects

Hemophagocytic lymphohistiocytosis, business.industry, Fulminant, fungi, Immunology, Inflammation, medicine.disease, Rheumatology, Macrophage activation syndrome, medicine, Interleukin 12, Immunology and Allergy, Pharmacology (medical), Interferon gamma, medicine.symptom, Hemophagocytosis, Cytokine storm, business, medicine.drug

Abstract

Objective Macrophage activation syndrome (MAS) is a devastating cytokine storm syndrome complicating many inflammatory diseases and characterized by fever, pancytopenia, and systemic inflammation. It is clinically similar to hemophagocytic lymphohistiocytosis (HLH), which is caused by viral infection of a host with impaired cellular cytotoxicity. Murine models of MAS and HLH illustrate that interferon-γ (IFNγ) is the driving stimulus for hemophagocytosis and immunopathology. This study was undertaken to investigate the inflammatory contributors to a murine model of Toll-like receptor 9 (TLR-9)–induced fulminant MAS. Methods Wild-type, transgenic, and cytokine-inhibited mice were treated with an IL-10 receptor blocking antibody and a TLR-9 agonist, and parameters of MAS were evaluated. Results Fulminant MAS was characterized by dramatic elevations in IFNγ, IL-12, and IL-6 levels. Increased serum IFNγ levels were associated with enhanced IFNγ production within some hepatic cell populations but also with decreased numbers of IFNγ-positive cells. Surprisingly, IFNγ-knockout mice developed immunopathology and hemophagocytosis comparable to that seen in wild-type mice. However, IFNγ-knockout mice did not become anemic and had greater numbers of splenic erythroid precursors. IL-12 neutralization phenocopied disease in IFNγ-knockout mice. Interestingly, type I IFNs contributed to the severity of hypercytokinemia and weight loss, but their absence did not otherwise affect MAS manifestations. Conclusion These data demonstrate that both fulminant MAS and hemophagocytosis can arise independently of IFNγ, IL-12, or type I IFNs. They also suggest that IFNγ-mediated dyserythropoiesis, not hemophagocytosis, is the dominant cause of anemia in fulminant TLR-9–induced MAS. Thus, our data establish a novel mechanism for the acute anemia of inflammation, but suggest that a variety of triggers can result in hemophagocytic disease.

Published

2013

50. IL-10 distinguishes a unique population of activated, effector-like CD8

Author

Julia E, Rood, Scott W, Canna, Lehn K, Weaver, John W, Tobias, and Edward M, Behrens

Subjects

Inflammation, Male, Transcription, Genetic, Inflammation, Extracellular Mediators, & Effector Molecules, Cell Differentiation, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Lymphohistiocytosis, Hemophagocytic, Interleukin-10, Mice, Inbred C57BL, Interferon-gamma, Phenotype, Liver, Toll-Like Receptor 9, Acute Disease, Animals, Intercellular Signaling Peptides and Proteins, Female, Antigens

Abstract

Immune-mediated liver injury is a central feature of hyperinflammatory diseases, such as hemophagocytic syndromes, yet the immunologic mechanisms underlying those processes are incompletely understood. In this study, we used the toll-like receptor 9 (TLR9)-mediated model of a hemophagocytic syndrome known as macrophage activation syndrome (MAS) to dissect the predominant immune cell populations infiltrating the liver during inflammation. We identified CD8

Published

2016