Your search keyword '"Mellins, Elizabeth D"' showing total 13 results

1. Increased activation product of complement 4 protein in plasma of individuals with schizophrenia.

Author

Kalinowski, Agnieszka, Liliental, Joanna, Anker, Lauren A., Linkovski, Omer, Culbertson, Collin, Hall, Jacob N., Pattni, Reenal, Sabatti, Chiara, Noordsy, Douglas, Hallmayer, Joachim F., Mellins, Elizabeth D., Ballon, Jacob S., O'Hara, Ruth, Levinson, Douglas F., and Urban, Alexander E.

Published

2021

2. Alternative pathways of osteoclastogenesis in inflammatory arthritis.

Author

Adamopoulos, lannis E. and Mellins, Elizabeth D.

Subjects

*ARTHRITIS, *OSTEOCLASTOGENESIS, *MACROPHAGE colony-stimulating factor, *CELL growth, *INFLAMMATION

Abstract

Osteoclasts are cells of haematopoietic origin that are uniquely specialized to degrade bone. Under physiological conditions, the osteoclastogenesis pathway depends on macrophage colony-stimulating factor 1 (CSF-1, also known as M-CSF) and receptor activator of nuclear factor κB ligand (RANKL). However, an emerging hypothesis is that alternative pathways of osteoclast generation might be active during inflammatory arthritis. In this Perspectives article, we summarize the physiological pathway of osteoclastogenesis and then focus on experimental findings that support the hypothesis that infiltrating inflammatory cells and the cytokine milieu provide multiple routes to bone destruction. The precise identity of osteoclast precursor(s) is not yet known. We propose that myeloid cell differentiation during inflammation could be an important contributor to the differentiation of osteoclast populations and their associated pathologies. Understanding the dynamics of osteoclast differentiation in inflammatory arthritis is crucial for the development of therapeutic strategies for inflammatory joint disease in children and adults. [ABSTRACT FROM AUTHOR]

Published

2015

3. HLA-DO acts as a substrate mimic to inhibit HLA-DM by a competitive mechanism.

Author

Guce, Abigail I, Mortimer, Sarah E, Yoon, Taejin, Painter, Corrie A, Jiang, Wei, Mellins, Elizabeth D, and Stern, Lawrence J

Subjects

HLA class II antigens, MAJOR histocompatibility complex, PROTEIN binding, RADIOLIGAND assay, X-ray crystallography

Abstract

Mammalian class II major histocompatibility (MHCII) proteins bind peptide antigens in endosomal compartments of antigen-presenting cells. The nonclassical MHCII protein HLA-DM chaperones peptide-free MHCII, protecting it against inactivation, and catalyzes peptide exchange on loaded MHCII. Another nonclassical MHCII protein, HLA-DO, binds HLA-DM and influences the repertoire of peptides presented by MHCII proteins. However, the mechanism by which HLA-DO functions is unclear. Here we have used X-ray crystallography, enzyme kinetics and mutagenesis approaches to investigate human HLA-DO structure and function. In complex with HLA-DM, HLA-DO adopts a classical MHCII structure, with alterations near the ? subunit's 310 helix. HLA-DO binds to HLA-DM at the same sites implicated in MHCII interaction, and kinetic analysis showed that HLA-DO acts as a competitive inhibitor. These results show that HLA-DO inhibits HLA-DM function by acting as a substrate mimic, and the findings also limit the possible functional roles for HLA-DO in antigen presentation. [ABSTRACT FROM AUTHOR]

Published

2013

4. Pathogenesis of systemic juvenile idiopathic arthritis: some answers, more questions.

Author

Mellins, Elizabeth D., Macaubas, Claudia, and Grom, Alexei A.

Subjects

*ARTHRITIS, *JUVENILE diseases, *INFLAMMATION, *MONOCYTES, *CYTOKINES, *EPIDEMIOLOGY, *MACROPHAGE activation syndrome

Abstract

Systemic juvenile idiopathic arthritis (sJIA) has long been recognized as unique among childhood arthritides, because of its distinctive clinical and epidemiological features, including an association with macrophage activation syndrome. Here, we summarize research into sJIA pathogenesis. The triggers of disease are unknown, although infections are suspects. Once initiated, sJIA seems to be driven by innate proinflammatory cytokines. Endogenous Toll-like receptor ligands, including S100 proteins, probably synergize with cytokines to perpetuate inflammation. These and other findings support the hypothesis that sJIA is an autoinflammatory condition. Indeed, IL-1 is implicated as a pivotal cytokine, but the source of excess IL-1 activity remains obscure and the role of IL-1 in chronic arthritis is less clear. Another hypothesis is that a form of hemophagocytic lymphohistiocytosis underlies sJIA, with varying degrees of its expression across the spectrum of disease. Alternatively, sJIA with MAS might be a genetically distinct subtype. Yet another hypothesis proposes that inadequate downregulation of immune activation is central to sJIA, supporting evidence for which includes 'alternative activation' of monocyte and macrophages and possible deficiencies in IL-10 and T regulatory cells. Some altered immune phenotypes persist during clinically inactive disease, which suggests that this stage might represent compensated inflammation. Despite much progress being made, many questions remain, providing fertile ground for future research. [ABSTRACT FROM AUTHOR]

Published

2011

5. Medicine on a need-to-know basis.

Author

Busch, Robert, Byrne, Belinda, Gandrud, Laurie, Sears, David, Meyer, Everett, Kattah, Michael, Kurihara, Christine, Haertel, Edward, Parnes, Jane R., and Mellins, Elizabeth D.

Subjects

STUDY & teaching of medicine, SCIENCE education (Graduate), DIABETES, SCIENTISTS, MEDICAL education policy, MEDICINE

Abstract

The article presents a discussion on a introductory medical curricula which focused on the study of diabetes to help overcome educational and institutional barriers that separate aspiring transnational scientists in PhD programs in the world of medicine. It also outlined the evaluation strategies and briefly summarized the results.

Published

2006

6. Author Correction: In vivo clonal expansion and phenotypes of hypocretin-specific CD4+ T cells in narcolepsy patients and controls.

Author

Jiang, Wei, Birtley, James R., Hung, Shu-Chen, Wang, Weiqi, Chiou, Shin-Heng, Macaubas, Claudia, Kornum, Birgitte, Tian, Lu, Huang, Huang, Adler, Lital, Weaver, Grant, Lu, Liying, Ilstad-Minnihan, Alexandra, Somasundaram, Sriram, Ayyangar, Sashi, Davis, Mark M., Stern, Lawrence J., and Mellins, Elizabeth D.

Subjects

T cells, NARCOLEPSY, OREXINS, PHENOTYPES

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper. [ABSTRACT FROM AUTHOR]

Published

2020

7. Paediatric rheumatic diseases: Navigating the transition from paediatric to adult care.

Author

Lawson, Erica F. and Mellins, Elizabeth D.

Subjects

*RHEUMATISM, *ADULT care services, *PEDIATRICS, *QUALITY standards, *PATIENTS, *RHEUMATISM treatment, *COMPARATIVE studies, *CONTINUUM of care, *COST effectiveness, *RESEARCH methodology, *MEDICAL cooperation, *MEDICAL protocols, *RESEARCH, *EVIDENCE-based medicine, *DISEASE management, *PROFESSIONAL practice, *EVALUATION research

Published

2017

8. In vivo clonal expansion and phenotypes of hypocretin-specific CD4+ T cells in narcolepsy patients and controls.

Author

Jiang, Wei, Birtley, James R., Hung, Shu-Chen, Wang, Weiqi, Chiou, Shin-Heng, Macaubas, Claudia, Kornum, Birgitte, Tian, Lu, Huang, Huang, Adler, Lital, Weaver, Grant, Lu, Liying, Ilstad-Minnihan, Alexandra, Somasundaram, Sriram, Ayyangar, Sashi, Davis, Mark M., Stern, Lawrence J., and Mellins, Elizabeth D.

Subjects

IN vivo studies, PHENOTYPES, OREXINS, T cells, NARCOLEPSY

Abstract

Individuals with narcolepsy suffer from abnormal sleep patterns due to loss of neurons that uniquely supply hypocretin (HCRT). Previous studies found associations of narcolepsy with the human leukocyte antigen (HLA)-DQ6 allele and T-cell receptor α (TRA) J24 gene segment and also suggested that in vitro-stimulated T cells can target HCRT. Here, we present evidence of in vivo expansion of DQ6-HCRT tetramer+/TRAJ24+/CD4+ T cells in DQ6+ individuals with and without narcolepsy. We identify related TRAJ24+ TCRαβ clonotypes encoded by identical α/β gene regions from two patients and two controls. TRAJ24-G allele+ clonotypes only expand in the two patients, whereas a TRAJ24-C allele+ clonotype expands in a control. A representative tetramer+/G-allele+ TCR shows signaling reactivity to the epitope HCRT87–97. Clonally expanded G-allele+ T cells exhibit an unconventional effector phenotype. Our analysis of in vivo expansion of HCRT-reactive TRAJ24+ cells opens an avenue for further investigation of the autoimmune contribution to narcolepsy development. T cells from narcolepsy patients were recently reported to recognize hypocretin, a wakefulness-promoting neurohormone, suggesting autoimmune origin of the disease. Here the authors show that hypocretin-specific T cells expand both in healthy controls and in narcolepsy patients, and identify preliminary features that may distinguish them. [ABSTRACT FROM AUTHOR]

Published

2019

9. Synergy between B cell receptor/antigen uptake and MHCII peptide editing relies on HLA-DO tuning.

Author

Jiang, Wei, Adler, Lital N., Macmillan, Henriette, and Mellins, Elizabeth D.

Subjects

B cell receptors, MAJOR histocompatibility complex, ANTIGENS, CELL communication, STOICHIOMETRY, CELL compartmentation

Abstract

B cell receptors and surface-displayed peptide/MHCII complexes constitute two key components of the B-cell machinery to sense signals and communicate with other cell types during antigen-triggered activation. However, critical pathways synergizing antigen-BCR interaction and antigenic peptide-MHCII presentation remain elusive. Here, we report the discovery of factors involved in establishing such synergy. We applied a single-cell measure coupled with super-resolution microscopy to investigate the integrated function of two lysosomal regulators for peptide loading, HLA-DM and HLA-DO. In model cell lines and human tonsillar B cells, we found that tunable DM/DO stoichiometry governs DMfree activity for exchange of placeholder CLIP peptides with high affinity MHCII ligands. Compared to their naïve counterparts, memory B cells with less DMfree concentrate a higher proportion of CLIP/MHCII in lysosomal compartments. Upon activation mediated by high affinity BCR, DO tuning is synchronized with antigen internalization and rapidly potentiates DMfree activity to optimize antigen presentation for T-cell recruitment. [ABSTRACT FROM AUTHOR]

Published

2019

10. Proceedings of the 2016 Childhood Arthritis and Rheumatology Research Alliance (CARRA) Scientific Meeting

Author

Fotis, Lampros, Shaikh, Nur, Baszis, Kevin, French, Anthony, Tarr, Phillip, Grevich, Sriharsha, Lee, Peggy, Ringold, Sarah, Leroux, Brian, Leahey, Hannah, Yuasa, Megan, Foster, Jessica, Sokolove, Jeremy, Lahey, Lauren, Robinson, William, Newsom, Joshua, Stevens, Anne, Karasawa, Rie, Tamaki, Mayumi, Tanaka, Megumi, Sato, Toshiko, Yudoh, Kazuo, Jarvis, James N., Moncrieffe, Halima, Bennett, Mark F., Tsoras, Monica, Luyrink, Lorie, Xu, Huan, Prahalad, Sampath, Morris, Paula, Dare, Jason, Nigrovic, Peter A., Rosenkranz, Margalit, Becker, Mara, O’Neil, Kathleen M., Griffin, Thomas, Lovell, Daniel J., Grom, Alexei A., Medvedovic, Mario, Thompson, Susan D., Zhu, Lisha, Jiang, Kaiyu, Wong, Laiping, Buck, Michael J, Chen, Yanmin, Brungs, Laura, Liu, Tao, Wang, Ting, Jarvis, James N, Alsaeid, Khaled, Alfailakawi, Jasim, Alenezi, Hamid, Alsaeed, Hazim, Beukelman, Tim, Natter, Marc, Ilowite, Norm, Mieszkalski, Kelly, Burrell, Grendel, Best, Brian, Bristow, Helen, Carr, Shannon, Dennos, Anne, Kaufmann, Rachel, Kimura, Yukiko, Schanberg, Laura, Blier, Peter R., Boneparth, Alexis, Wenderfer, Scott E., Moorthy, L. Nandini, Radhakrishna, Suhas M., Sagcal-Gironella, Anna Carmela P., von Scheven, Emily, Gedik, Kader Cetin, Siddique, Salma, Aguiar, Cassyanne L., Erkan, Doruk, Cohen, Ezra, Lee, Yvonne, Dossett, Michelle, Mehta, Darshan, Davis, Roger, Gilbert, Mileka, Goilav, Beatrice, Meidan, Esra, Hsu, Joyce, Chua, Anabelle, Ardoin, Stacy, Von Scheven, Emily, Ruth, Natasha M., Hui-Yuen, Joyce, Bermudez, Liza, Cook, Ashlea, Imundo, Lisa, Starr, Amy, Eichenfield, Andrew, Askanase, Anca, Janow, Ginger, Schanberg, Laura E., Setoguchi, Soko, Hasselblad, Victor, Mellins, Elizabeth D., Schneider, Rayfel, Beukelman, Timothy, Morgan, Esi, Graham, T. Brent, Ibarra, Maria, Ruas, Yonit Sterba, Klein-Gitelman, Marisa, Onel, Karen, Punaro, Marilynn, Toib, Dana, Van Mater, Heather, Weiss, Jennifer E., Weiss, Pamela F., Kwok, Timothy S. H., Bisaillon, Jacinthe, Smith, Christine, Brosseau, Lucie, Stinson, Jennifer, Huber, Adam M., Duffy, Ciaran M., April, Karine Toupin, Lewandowski, Laura B., Scott, Christiaan, Li, Suzanne C., Torok, Kathryn S., Rabinovich, C. Egla, Hong, Sandy D., Becker, Mara L, Dedeoglu, Fatma, Ibarra, Maria F., Ferguson, Polly J, Fuhbrigge, Rob C., Stewart, Katie G., Pope, Elena, Laxer, Ronald M., Mason, Thomas G., Higgins, Gloria C., Li, Xiaohu, Punaro, Marilynn G., Tomlinson, George, Pullenayegum, Eleanor, Matelski, John, Feldman, Brian M., Manthiram, Kalpana, Correa, Hernan, Edwards, Kathryn, Oberle, Edward J., Bayer, Michelle, Co, Dominic O., Baris, Hatice Ezgi, Chiu, Yvonne, Huber, Adam, Kim, Susan, Orandi, Amir B., Baszis, Kevin W., Dharnidharka, Vikas, Hoeltzel, Mark F., Reed, Ann, Goh, Y. Ingrid, Schnabel, Anja, Range, Ursula, Hahn, Gabriele, Siepmann, Timo, Berner, Reinhard, Hedrich, Christian Michael, Stevens, Brandi, Li, Suzanne, Hershey, Nicole, Curran, Megan, Higgins, Gloria, Moore, Katharine, Rabinovich, Egla, Stevens, Anne M., Connelly, Mark, Luca, Nadia, Spiegel, Lynn, Tsimicalis, Argerie, Luca, Stephanie, Tajuddin, Naweed, Berard, Roberta, Barsalou, Julia, Campillo, Sarah, Dancey, Paul, Duffy, Ciaran, Feldman, Brian, Johnson, Nicole, McGrath, Patrick, Shiff, Natalie, Tse, Shirley, Tucker, Lori, Victor, Charles, Lalloo, Chitra, Harris, Lauren, Cafazzo, Joseph, Laxer, Ronald, Bullock, Danielle R., Vehe, Richard K., Zhang, Lei, Correll, Colleen K., Ganguli, Suhas, Shenberger, Max, Korumilli, Ritesh, Gottlieb, Beth, Rodriguez, Martha, de Ranieri, Deirdre, Wagner-Weiner, Linda, Tesher, Melissa, Wojcicki, Elizabeth Roth, Maletta, Kristyn L., Malloy, Marsha, Thomson, Sarah, Olson, Judyann C., Sule, Sangeeta, Rubinstein, Tamar B., Okamura, Daryl M., Chua, Annabelle, Greenbaum, Laurence A., Lane, Jerome C., Ardoin, Stacy P., Woo, Jennifer M. P., Malloy, Marsha M., Jegers, James A., Hahn, Dustin J., Hintermeyer, Mary K., Martinetti, Stacey M., Heckel, Gretchen R., and Roth-Wojcicki, Elizabeth L.

Subjects

Rheumatology, Immunology and Allergy, Pediatrics, Perinatology, and Child Health, Meeting Abstracts

Abstract

Table of Contents P1 Serologic evidence of gut-driven systemic inflammation in juvenile idiopathic arthritis Lampros Fotis, Nur Shaikh, Kevin Baszis, Anthony French, Phillip Tarr P2 Oral health and anti-citrullinated peptide antibodies (ACPA) in juvenile idiopathic arthritis Sriharsha Grevich, Peggy Lee, Sarah Ringold, Brian Leroux, Hannah Leahey, Megan Yuasa, Jessica Foster, Jeremy Sokolove, Lauren Lahey, William Robinson, Joshua Newsom, Anne Stevens P3 Novel autoantigens for endothelial cell antibodies in pediatric rheumatic diseases identified by proteomics Rie Karasawa, Mayumi Tamaki, Megumi Tanaka, Toshiko Sato, Kazuo Yudoh, James N. Jarvis P4 Transcriptional profiling reveals monocyte signature associated with JIA patient poor response to methotrexate Halima Moncrieffe, Mark F. Bennett, Monica Tsoras, Lorie Luyrink, Huan Xu, Sampath Prahalad, Paula Morris, Jason Dare, Peter A. Nigrovic, Margalit Rosenkranz, Mara Becker, Kathleen M. O’Neil, Thomas Griffin, Daniel J. Lovell, Alexei A. Grom, Mario Medvedovic, Susan D. Thompson P5 A multi-dimensional genomic map for polyarticular juvenile idiopathic arthritis Lisha Zhu, Kaiyu Jiang, Laiping Wong, Michael J Buck, Yanmin Chen, Halima Moncrieffe, Laura Brungs, Tao Liu, Ting Wang, James N Jarvis P6 Tocilizumab for treatment of children with refractory JIA Khaled Alsaeid, Jasim Alfailakawi, Hamid Alenezi, Hazim Alsaeed P7 Clinical characteristics of the initial patients enrolled in the Childhood Arthritis and Rheumatology Research Alliance (CARRA) Registry Tim Beukelman, Marc Natter, Norm Ilowite, Kelly Mieszkalski, Grendel Burrell, Brian Best, Helen Bristow, Shannon Carr, Anne Dennos, Rachel Kaufmann, Yukiko Kimura, Laura Schanberg P8 Comparative performance of small and large clinical centers in a comprehensive pediatric rheumatology disease registry Peter R Blier P9 Clinical characteristics of children with membranous lupus nephritis: The Childhood Arthritis and Rheumatology Research Alliance Legacy Registry Alexis Boneparth, Scott E. Wenderfer, L. Nandini Moorthy, Suhas M. Radhakrishna, Anna Carmela P. Sagcal-Gironella, Emily von Scheven P10 Rituximab use in pediatric lupus anticoagulant hypoprothrombinemia syndrome - a two center experience Kader Cetin Gedik, Salma Siddique, Cassyanne L. Aguiar, Doruk Erkan P11 Predictors of complementary and alternative medicine use and response in children with musculoskeletal conditions Ezra Cohen, Yvonne Lee, Michelle Dossett, Darshan Mehta, Roger Davis P12 Comparison of pediatric rheumatology and nephrology survey results for the treatment of refractory proliferative lupus nephritis and renal flare in juvenile SLE Mileka Gilbert, Beatrice Goilav, Esra Meidan, Joyce Hsu, Alexis Boneparth, Anabelle Chua, Stacy Ardoin, Scott E. Wenderfer, Emily Von Scheven, Natasha M. Ruth P13 Transitioning lupus patients from pediatric to adult rheumatology Joyce Hui-Yuen, Kader Cetin Gedik, Liza Bermudez, Ashlea Cook, Lisa Imundo, Amy Starr, Andrew Eichenfield, Anca Askanase P14 The systemic juvenile idiopathic arthritis cohort of the Childhood Arthritis & Rheumatology Research Alliance Registry Ginger Janow, Laura E. Schanberg, Soko Setoguchi, Victor Hasselblad, Elizabeth D. Mellins, Rayfel Schneider, Yukiko Kimura, The CARRA Legacy Registry Investigators P15 Results of the pilot study of the Childhood Arthritis and Rheumatology Research Alliance (CARRA) consensus treatment plans for new-onset systemic juvenile idiopathic arthritis Yukiko Kimura, Sriharsha Grevich, Timothy Beukelman, Esi Morgan, T Brent Graham, Maria Ibarra, Yonit Sterba Ruas, Marisa Klein-Gitelman, Karen Onel, Sampath Prahalad, Marilynn Punaro, Sarah Ringold, Dana Toib, Heather Van Mater, Jennifer E. Weiss, Pamela F. Weiss, Kelly Mieszkalski, Laura E. Schanberg P16 A systemic review of pain relief modalities in juvenile idiopathic arthritis: First step in developing a novel decision support intervention Timothy S. H. Kwok, Jacinthe Bisaillon, Christine Smith, Lucie Brosseau, Jennifer Stinson, Adam M. Huber, Ciaran M. Duffy, Karine Toupin April P17 Barriers and facilitators to care retention for pediatric systemic lupus erythematous patients in South Africa: A qualitative study Laura B Lewandowski, Christiaan Scott P18 Evaluating the feasibility of conducting comparative effectiveness studies in juvenile Localized Scleroderma (jLS) Suzanne C. Li, Kathryn S. Torok, C. Egla Rabinovich, Sandy D. Hong, Mara L Becker, Fatma Dedeoglu, Maria F. Ibarra, Polly J Ferguson, Rob C. Fuhbrigge, Katie G. Stewart, Elena Pope, Ronald M. Laxer, Thomas G. Mason, Gloria C. Higgins, Xiaohu Li, Marilynn G. Punaro, George Tomlinson, Eleanor Pullenayegum, John Matelski, Laura Schanberg, Brian M. Feldman P19 Tonsillar histology in patients with periodic fever, aphthous stomatitis, pharyngitis, adenitis (PFAPA) syndrome Kalpana Manthiram, Hernan Correa, Kathryn Edwards P20 Clinical course of juvenile dermatomyositis presenting as skin predominant disease Edward J. Oberle, Michelle Bayer, Dominic O. Co, Hatice Ezgi Baris, Yvonne Chiu, Adam Huber, Susan Kim P21 A Survey of musculoskeletal ultrasound practices of pediatric rheumatologists in North America Edward J Oberle, Timothy Beukelman P22 Assessment, classification and treatment of calcinosis as a complication of juvenile dermatomyositis: A survey of pediatric rheumatologists by the Childhood Arthritis and Rheumatology Research Alliance Amir B. Orandi, Kevin W. Baszis, Vikas Dharnidharka, Mark F. Hoeltzel, for the CARRA JDM Committee P23 CARRA dermatomyositis CTP pilot study Ann Reed, Adam Huber, George Tomlinson, Eleanor Pullenayegum, John Matelski, Y. Ingrid Goh, Laura Schanberg, Brian M. Feldman P24 Unexpectedly high incidences and prolonged disease activity in children with chronic non-bacterial osteomyelitis (CNO) as compared to bacterial osteomyelitis Anja Schnabel, Ursula Range, Gabriele Hahn, Timo Siepmann, Reinhard Berner, Christian Michael Hedrich P25 Juvenile systemic sclerosis cohort within the Childhood Arthritis and Rheumatology Research Alliance (CARRA) Legacy Registry: Follow up characteristics Brandi Stevens, Kathryn S. Torok, Suzanne Li, Nicole Hershey, Megan Curran, Gloria Higgins, Katharine Moore, Egla Rabinovich, Anne M. Stevens, for the CARRA Registry Investigators P26 Development and usability testing of an iPad and desktop psycho-educational game for children with Juvenile Idiopathic Arthritis and their parents Jennifer Stinson, Mark Connelly, Adam Huber, Nadia Luca, Lynn Spiegel, Argerie Tsimicalis, Stephanie Luca, Naweed Tajuddin, Roberta Berard, Julia Barsalou, Sarah Campillo, Paul Dancey, Ciaran Duffy, Brian Feldman, Nicole Johnson, Patrick McGrath, Natalie Shiff, Shirley Tse, Lori Tucker, Charles Victor P27 iCanCopeTM: User-centred design and development of a smartphone app to support self-management for youth with arthritis pain Jennifer Stinson, Chitra Lalloo, Lauren Harris, Joseph Cafazzo, Lynn Spiegel, Brian Feldman, Nadia Luca, Ronald Laxer P28 Accessing pediatric rheumatology care: Despite barriers, few parents prefer telemedicine Danielle R. Bullock, Richard K. Vehe, Lei Zhang, Colleen K. Correll1 P29 Exploration of factors contributing to time to achieve clinically inactive disease (CID) in juvenile idiopathic arthritis (JIA): A preliminary report Suhas Ganguli, Max Shenberger, Ritesh Korumilli, Beth Gottlieb P30 Pediatric rheumatology referral patterns: Presenting complaints of new patients at a large, urban academic center Martha Rodriguez, Deirdre de Ranieri, Karen Onel, Linda Wagner-Weiner, Melissa Tesher P31 Quality improvement (QI) initiatives in childhood systemic lupus erythematosus (cSLE) Elizabeth Roth Wojcicki, Kristyn L. Maletta, Dominic O. Co, Marsha Malloy, Sarah Thomson, Judyann C. Olson P32 Proliferative lupus nephritis in juvenile SLE: Support from the pediatric nephrology community for the definitions of responsiveness and flare in the 2012 consensus treatment plans Scott E. Wenderfer, Mileka Gilbert, Joyce Hsu, Sangeeta Sule, Tamar B. Rubinstein, Beatrice Goilav, Daryl M. Okamura, Annabelle Chua, Laurence A. Greenbaum, Jerome C. Lane, Emily von Scheven, Stacy P. Ardoin, Natasha M. Ruth P33 The steroid taper app: Making of a mobile app Jennifer M. P. Woo, Marsha M. Malloy, James A. Jegers, Dustin J. Hahn, Mary K. Hintermeyer, Stacey M. Martinetti, Gretchen R. Heckel, Elizabeth L. Roth-Wojcicki, Dominic O. Co

11. HLA associations in inflammatory arthritis: emerging mechanisms and clinical implications.

Author

Busch, Robert, Kollnberger, Simon, and Mellins, Elizabeth D.

Subjects

*DISEASE risk factors, *MACROPHAGE activation syndrome, *RHEUMATOID arthritis, *JUVENILE idiopathic arthritis, *ARTHRITIS, *RHEUMATISM

Abstract

Our understanding of the mechanisms underlying HLA associations with inflammatory arthritis continues to evolve. Disease associations have been refined, and interactions of HLA genotype with other genes and environmental risk factors in determining disease risk have been identified. This Review provides basic information on the genetics and molecular function of HLA molecules, as well as general features of HLA associations with disease. Evidence is discussed regarding the various peptide-dependent and peptide-independent mechanisms by which HLA alleles might contribute to the pathogenesis of three types of inflammatory arthritis: rheumatoid arthritis, spondyloarthritis and systemic juvenile idiopathic arthritis. Also discussed are HLA allelic associations that shed light on the genetic heterogeneity of inflammatory arthritides and on the relationships between adult and paediatric forms of arthritis. Clinical implications range from improved diagnosis and outcome prediction to the possibility of using HLA associations in developing personalized strategies for the treatment and prevention of these diseases. [ABSTRACT FROM AUTHOR]

Published

2019

12. pH-susceptibility of HLA-DO tunes DO/DM ratios to regulate HLA-DM catalytic activity.

Author

Jiang, Wei, Strohman, Michael J., Somasundaram, Sriram, Ayyangar, Sashi, Hou, Tieying, Wang, Nan, and Mellins, Elizabeth D.

Subjects

PEPTIDE analysis, PROTEIN analysis, HLA histocompatibility antigens, HISTOCOMPATIBILITY class I antigens, HISTOCOMPATIBILITY, IMMUNOLOGICAL tolerance

Abstract

The peptide-exchange catalyst, HLA-DM, and its inhibitor, HLA-DO control endosomal generation of peptide/class II major histocompatibility protein (MHC-II) complexes; these complexes traffic to the cell surface for inspection by CD4+ T cells. Some evidence suggests that pH influences DO regulation of DM function, but pH also affects the stability of polymorphic MHC-II proteins, spontaneous peptide loading, DM/MHC-II interactions and DM catalytic activity, imposing challenges on approaches to determine pH effects on DM-DO function and their mechanistic basis. Using optimized biochemical methods, we dissected pH-dependence of spontaneous and DM-DO-mediated class II peptide exchange and identified an MHC-II allele-independent relationship between pH, DO/DM ratio and efficient peptide exchange. We demonstrate that active, free DM is generated from DM-DO complexes at late endosomal/lysosomal pH due to irreversible, acid-promoted DO destruction rather than DO/DM molecular dissociation. Any soluble DM that remains in complex with DO stays inert. pH-exposure of DM-DO in cell lysates corroborates such a pH-regulated mechanism, suggesting acid-activated generation of functional DM in DO-expressing cells. [ABSTRACT FROM AUTHOR]

Published

2015

13. Oligoarticular and polyarticular JIA: epidemiology and pathogenesis.

Author

Macaubas, Claudia, Nguyen, Khoa, Milojevic, Diana, Park, Jane L., and Mellins, Elizabeth D.

Subjects

*ARTHRITIS, *ETIOLOGY of diseases, *RHEUMATOID arthritis, *GENETICS, *TUMOR necrosis factors

Abstract

Juvenile idiopathic arthritis (JIA) refers to a group of chronic childhood arthropathies of unknown etiology, currently classified into subtypes primarily on the basis of clinical features. Research has focused on the hypothesis that these subtypes arise through distinct etiologic pathways. In this Review, we discuss four subtypes of JIA: persistent oligoarticular, extended oligoarticular, rheumatoid-factor-positive polyarticular and rheumatoid-factor-negative polyarticular. These subtypes differ in prevalence between ethnic groups and are associated with different HLA alleles. Non-HLA genetic risk factors have also been identified, some of which reveal further molecular differences between these subtypes, while others suggest mechanistic overlap. Investigations of immunophenotypes also provide insights into subtype differences: adaptive immunity seems to have a prominent role in both polyarticular and oligoarticular JIA, and the more-limited arthritis observed in persistent oligoarticular JIA as compared with extended oligoarticular JIA may reflect more-potent immunoregulatory T-cell activity in the former. Tumor necrosis factor seems to be a key mediator of both polyarticular and oligoarticular JIA, especially in the extended oligoarticular subtype, although elevated levels of other cytokines are also observed. Limited data on monocytes, dendritic cells, B cells, natural killer T cells and neutrophils suggest that the contributions of these cells differ across subtypes of JIA. Within each subtype, however, common pathways seem to drive joint damage. [ABSTRACT FROM AUTHOR]

Published

2009