Your search keyword '"Canna, Scott"' showing total 17 results

1. Cytokine Storm Syndrome Associated with Systemic Juvenile Idiopathic Arthritis

Author

Infection & Immunity, Immunologie/Reumatologie, Immuno/reuma onderzoek 1 (Vastert), CTI Van Loosdregt, Child Health, Vastert, Sebastiaan J., Canny, Susan P., Canna, Scott W., Schneider, Rayfel, Mellins, Elizabeth D., Infection & Immunity, Immunologie/Reumatologie, Immuno/reuma onderzoek 1 (Vastert), CTI Van Loosdregt, Child Health, Vastert, Sebastiaan J., Canny, Susan P., Canna, Scott W., Schneider, Rayfel, and Mellins, Elizabeth D.

Published

2024

2. The 2022 EULAR/ACR points to consider at the early stages of diagnosis and management of suspected haemophagocytic lymphohistiocytosis/macrophage activation syndrome (HLH/MAS)

Author

CTI Van Loosdregt, Research UMC Utrecht, Immuno/reuma onderzoek 1 (Vastert), Immunologie/Reumatologie, Child Health, Shakoory, Bita, Geerlinks, Ashley, Wilejto, Marta, Kernan, Kate, Hines, Melissa, Romano, Micol, Piskin, David, Ravelli, Angelo, Sinha, Rashmi, Aletaha, Daniel, Allen, Carl, Bassiri, Hamid, Behrens, Edward M., Carcillo, Joseph, Carl, Linda, Chatham, Winn, Cohen, Jeffrey I., Cron, Randy Q., Drewniak, Erik, Grom, Alexei A., Henderson, Lauren A., Horne, Annacarin, Jordan, Michael B., Nichols, Kim E., Schulert, Grant, Vastert, Sebastiaan, Demirkaya, Erkan, Goldbach-Mansky, Raphaela, De Benedetti, Fabrizio, Marsh, Rebecca A., Canna, Scott W., CTI Van Loosdregt, Research UMC Utrecht, Immuno/reuma onderzoek 1 (Vastert), Immunologie/Reumatologie, Child Health, Shakoory, Bita, Geerlinks, Ashley, Wilejto, Marta, Kernan, Kate, Hines, Melissa, Romano, Micol, Piskin, David, Ravelli, Angelo, Sinha, Rashmi, Aletaha, Daniel, Allen, Carl, Bassiri, Hamid, Behrens, Edward M., Carcillo, Joseph, Carl, Linda, Chatham, Winn, Cohen, Jeffrey I., Cron, Randy Q., Drewniak, Erik, Grom, Alexei A., Henderson, Lauren A., Horne, Annacarin, Jordan, Michael B., Nichols, Kim E., Schulert, Grant, Vastert, Sebastiaan, Demirkaya, Erkan, Goldbach-Mansky, Raphaela, De Benedetti, Fabrizio, Marsh, Rebecca A., and Canna, Scott W.

Published

2023

3. 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

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

Abstract

ObjectiveTo 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.MethodsThe 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.ResultsThe 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.ConclusionOur 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

4. 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

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

Abstract

ObjectiveTo 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.MethodsThe 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.ResultsThe 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.ConclusionOur 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

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

Author

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

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 < 0.05). This panel was predictive of both HBD + DIC (sensitivity = 82%, specificity = 84%) and mortality (sensitivity = 92%, specificity = 90%).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

6. Severe delayed hypersensitivity reactions to IL-1 and IL-6 inhibitors link to common HLA-DRB1*15 alleles.

Author

Saper, Vivian, Saper, Vivian, Ombrello, Michael, Montero-Martin, Gonzalo, Prahalad, Sampath, Canna, Scott, Shimizu, Chisato, Deutsch, Gail, Tan, Serena, Remmers, Elaine, Monos, Dimitri, Hahn, Timothy, Phadke, Omkar, Cassidy, Elaine, Ferguson, Ian, Mallajosyula, Vamsee, Xu, Jianpeng, Rosa Duque, Jaime, Chua, Gilbert, Ghosh, Debopam, Szymanski, Ann, Rubin, Danielle, Tian, Lu, Fernandez-Vina, Marcelo, Mellins, Elizabeth, Burns, Jane, Tremoulet, Adriana, Hollenbach, Jill, Saper, Vivian, Saper, Vivian, Ombrello, Michael, Montero-Martin, Gonzalo, Prahalad, Sampath, Canna, Scott, Shimizu, Chisato, Deutsch, Gail, Tan, Serena, Remmers, Elaine, Monos, Dimitri, Hahn, Timothy, Phadke, Omkar, Cassidy, Elaine, Ferguson, Ian, Mallajosyula, Vamsee, Xu, Jianpeng, Rosa Duque, Jaime, Chua, Gilbert, Ghosh, Debopam, Szymanski, Ann, Rubin, Danielle, Tian, Lu, Fernandez-Vina, Marcelo, Mellins, Elizabeth, Burns, Jane, Tremoulet, Adriana, and Hollenbach, Jill

Abstract

OBJECTIVES: Drug reaction with eosinophilia and systemic symptoms (DRESS) is a severe, delayed hypersensitivity reaction (DHR). We observed DRESS to inhibitors of interleukin 1 (IL-1) or IL-6 in a small group of patients with Stills disease with atypical lung disease. We sought to characterise features of patients with Stills disease with DRESS compared with drug-tolerant Stills controls. We analysed human leucocyte antigen (HLA) alleles for association to inhibitor-related DHR, including in a small Kawasaki disease (KD) cohort. METHODS: In a case/control study, we collected a multicentre series of patients with Stills disease with features of inhibitor-related DRESS (n=66) and drug-tolerant Stills controls (n=65). We retrospectively analysed clinical data from all Stills subjects and typed 94/131 for HLA. European Stills-DRESS cases were ancestry matched to International Childhood Arthritis Genetics Consortium paediatric Stills cases (n=550) and compared for HLA allele frequencies. HLA association also was analysed using Stills-DRESS cases (n=64) compared with drug-tolerant Stills controls (n=30). KD subjects (n=19) were similarly studied. RESULTS: Stills-DRESS features included eosinophilia (89%), AST-ALT elevation (75%) and non-evanescent rash (95%; 88% involving face). Macrophage activation syndrome during treatment was frequent in Stills-DRESS (64%) versus drug-tolerant Stills (3%; p=1.2×10-14). We found striking enrichment for HLA-DRB1*15 haplotypes in Stills-DRESS cases versus INCHARGE Stills controls (p=7.5×10-13) and versus self-identified, ancestry-matched Stills controls (p=6.3×10-10). In the KD cohort, DRB1*15:01 was present only in those with suspected anakinra reactions. CONCLUSIONS: DRESS-type reactions occur among patients treated with IL-1/IL-6 inhibitors and strongly associate with common HLA-DRB1*15 haplotypes. Consideration of preprescription HLA typing and vigilance for serious reactions to these drugs are warranted.

Published

2022

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

Author

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

Abstract

ObjectiveTo 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. Recommendations are also provided for children with hyperinflammation during coronavirus disease 2019 (COVID-19), the acute, infectious phase of SARS-CoV-2 infection.MethodsThe Task Force was 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.ResultsThe first version of the guidance was approved in June 2020, and consisted of 40 final guidance statements accompanied by a flow diagram depicting the diagnostic pathway for MIS-C. The document was revised in November 2020, and a new flow diagram with recommendations for initial immunomodulatory treatment of MIS-C was added.ConclusionOur 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

2021

8. Therapeutic approaches to pediatric COVID-19: an online survey of pediatric rheumatologists.

Author

Minden, Kirsten, Minden, Kirsten, Hinze, Claas, Schulz, Ansgar, Debatin, Klaus-Michael, Hedrich, Christian, Speth, Fabian, Janda, Ales, Schuetz, Catharina, Canna, Scott, Gorelik, Mark, Heeg, Maximilian, Minden, Kirsten, Minden, Kirsten, Hinze, Claas, Schulz, Ansgar, Debatin, Klaus-Michael, Hedrich, Christian, Speth, Fabian, Janda, Ales, Schuetz, Catharina, Canna, Scott, Gorelik, Mark, and Heeg, Maximilian

Abstract

Data on therapy of COVID-19 in immunocompetent and immunosuppressed children are scarce. We aimed to explore management strategies of pediatric rheumatologists. All subscribers to international Pediatric Rheumatology Bulletin Board were invited to take part in an online survey on therapeutic approaches to COVID-19 in healthy children and children with autoimmune/inflammatory diseases (AID). Off-label therapies would be considered by 90.3% of the 93 participating respondents. In stable patients with COVID-19 on oxygen supply (stage I), use of remdesivir (48.3%), azithromycin (26.6%), oral corticosteroids (25.4%) and/or hydroxychloroquine (21.9%) would be recommended. In case of early signs of cytokine storm (stage II) or in critically ill patients (stage III) (a) anakinra (79.5% stage II; 83.6% stage III) or tocilizumab (58.0% and 87.0%, respectively); (b) corticosteroids (oral 67.2% stage II, intravenously 81.7% stage III); (c) intravenous immunoglobulins (both stages 56.5%); or (d) remdesivir (both stages 46.7%) were considered. In AID, > 94.2% of the respondents would not support a preventive adaptation of the immunomodulating therapy. In case of mild COVID-19, more than 50% of the respondents would continue pre-existing treatment with immunoglobulins (100%), hydroxychloroquine (94.2%), anakinra (79.2%) or canakinumab (72.5%), or tocilizumab (69.8%). Long-term corticosteroids would be reduced by 26.9% (< = 2 mg/kg/d) and 50.0% (> 2 mg/kg/day), respectively, with only 5.8% of respondents voting to discontinue the therapy. Conversely, more than 75% of respondents would refrain from administering cyclophosphamide and anti-CD20-antibodies. As evidence on management of pediatric COVID-19 is incomplete, continuous and critical expert opinion and knowledge exchange is helpful.

Published

2021

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

Author

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

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 <30% mosaicism, suggesting a dominant mechanism responsible for the clinical phenotype. Mosaicism was also detected in skin-derived fibroblasts in 3 patients, demonstrating that mutations were not limited to the hematopoietic compartment. All patients had refractory chronic neutropenia, and 3 patients underwent allogeneic hematopoietic cell transplantation. All variants conferred gain of function to TLR8 protein, and immune phenotyping demonstrated a proinflammatory phenotype with activated T cells and elevated serum cytokines associated with impaired B-cell maturation. Differentiation of myeloid cells from patient-derived induced pluripotent stem cells demonstrated increased responsiveness to TLR8. Together, these findings demonstrate that gain-of-function variants in TLR8 lead to a novel childhood-onset IEI with lymphoproliferation, neutropenia, infectious susceptibility, B- and T-cell defects, and in some cases, bone marrow failure. Somatic mosaicism is a prominent molecular mechanism of this new disease.

Published

2021

10. 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

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

Abstract

ObjectiveTo 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.MethodsA 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.ResultsThe 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.ConclusionOur understanding of SARS-CoV-2-related syndromes in the pediatric population continues to evolve. The guidance provided in this "living document" reflects

Published

2020

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

Author

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

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-kappa B 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-Goutieres 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-kappa B 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 (NEM

Published

2020

12. 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

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

Abstract

ObjectiveTo 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.MethodsA 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.ResultsThe 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.ConclusionOur understanding of SARS-CoV-2-related syndromes in the pediatric population continues to evolve. The guidance provided in this "living document" reflects

Published

2020

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

Author

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

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-kappa B 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-Goutieres 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-kappa B 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 (NEM

Published

2020

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

Author

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

Published

2018

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

Author

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

Published

2018

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

Author

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

Published

2018

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

Author

MS Reumatologie/Immunologie/Infectie, Infection & Immunity, Immuno/reuma patientenzorg, Child Health, Aeschlimann, Florence A., Batu, Ezgi D., Canna, Scott W., Go, Ellen, Gül, Ahmet, Hoffmann, Patrycja, Leavis, Helen L., Ozen, Seza, Schwartz, Daniella M., Stone, Deborah L., Van Royen-Kerkhof, Annet, Kastner, Daniel L., Aksentijevich, Ivona, Laxer, Ronald M., MS Reumatologie/Immunologie/Infectie, Infection & Immunity, Immuno/reuma patientenzorg, Child Health, Aeschlimann, Florence A., Batu, Ezgi D., Canna, Scott W., Go, Ellen, Gül, Ahmet, Hoffmann, Patrycja, Leavis, Helen L., Ozen, Seza, Schwartz, Daniella M., Stone, Deborah L., Van Royen-Kerkhof, Annet, Kastner, Daniel L., Aksentijevich, Ivona, and Laxer, Ronald M.

Published

2018