Article
Immunology
Champa Nataraja, Jacqueline Flynn, Wendy Dankers, Melissa Northcott, Wendy Zhu, Rochelle Sherlock, Taylah J. Bennett, Brendan E. Russ, Iolanda Miceli, Mehnaz Pervin, Akshay D'Cruz, James Harris, Eric F. Morand, Sarah A. Jones
Summary: Glucocorticoids are widely used in modern medicine for their ability to suppress immune activation, but they have severe adverse effects. This study found that the GILZ gene plays a crucial role in regulating the expression and action of type I interferon, suggesting that restoring GILZ could be an attractive therapeutic strategy for reducing reliance on glucocorticoids.
JOURNAL OF AUTOIMMUNITY
(2022)
Article
Immunology
Riccardo Papa, Marta Rusmini, Francesca Schena, Elisabetta Traggiai, Maria Cristina Coccia, Roberta Caorsi, Serena Arrigo, Francesco Pasetti, Sara Signa, Patrizia Barone, Giuseppe Santamaria, Giovanni Spirito, Remo Sanges, Diego Vozzi, Andrea Cavalli, Stefano Gustincich, Angelo Ravelli, Marco Gattorno, Isabella Ceccherini, Stefano Volpi
Summary: RAS-associated autoimmune leukoproliferative disease (RALD) is a rare immune dysregulation syndrome caused by somatic gain-of-function mutations of the NRAS or KRAS gene. It can lead to a complex multi-organ autoimmune syndrome, such as hypogammaglobulinemia and hepatopulmonary syndrome.
CLINICAL IMMUNOLOGY
(2021)
Article
Immunology
Nadine Szumilas, Odilia B. J. Corneth, Christian H. K. Lehmann, Heike Schmitt, Svenia Cunz, Jolie G. Cullen, Talyn Chu, Anita Marosan, Attila Mocsai, Vladimir Benes, Dietmar Zehn, Diana Dudziak, Rudi W. Hendriks, Lars Nitschke
Summary: Siglec-H regulates TLR-9-dependent inflammatory responses after virus infections, but not TLR-7 dependent responses. Lack of Siglec-H in pDCs leads to impaired Hck expression and downregulation of chemokine receptor CCR9, affecting pDC function.
FRONTIERS IN IMMUNOLOGY
(2021)
Article
Biochemistry & Molecular Biology
Tao Ming Sim, Siying Jane Ong, Anselm Mak, Sen Hee Tay
Summary: This review discusses the bench to bedside translation of the type I IFN pathway and explores some unresolved issues when selecting SLE patients for treatment with biologics targeting type I IFNs.
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
(2022)
Article
Microbiology
Zhuoran Li, Danfeng Lu, Heng Yang, Zhuoyue Li, Pei Zhu, Jiarui Xie, Defang Liao, Yongtang Zheng, Huachun Li
Summary: NS3 and NS4 of BTV coordinate to counteract IFN-I signaling in the JAK-STAT pathway by directly interacting with STAT1, targeting the SH2 domain of STAT1 to inhibit its phosphorylation. This study confirms the participation of NS3 and NS4 in interfering with IFN-I signaling and reveals a new mechanism used by BTV to evade host innate immune responses.
VETERINARY MICROBIOLOGY
(2021)
Review
Oncology
Yong Liang, Raquibul Hannan, Yang-Xin Fu
Summary: Immune checkpoint inhibitors are successful immunotherapy modalities that enhance CD8(+) T-cell responses. Recent studies have found that cross-priming of conventional type 1 dendritic cells (cDC1) plays a crucial role in initiating CD8(+) T-cell responses during tumor progression, as well as in immunotherapy-mediated reactivation of tumor-specific CD8(+) T cells for tumor regression. Inducing type I IFNs within tumors can overcome innate immune resistance and activate antitumor adaptive immunity.
CLINICAL CANCER RESEARCH
(2021)
Article
Immunology
Emma J. Keller, Neeva B. Patel, Madeline Patt, Jane K. Nguyen, Trine N. Jorgensen
Summary: Research indicates that in SLE patients, IFN alpha beta signaling in B cells leads to splenomegaly, increased populations of activated B cells, germinal center B cells, memory B cells, and plasma blasts/cells, while not affecting the development of glomerulonephritis and immune-complex deposition.
FRONTIERS IN IMMUNOLOGY
(2021)
Article
Fisheries
Rodrigo Guabiraba, Damaris Ribeiro Rodrigues, Paul T. Manna, Melanie Chollot, Vincent Saint-Martin, Sascha Trapp, Marisa Oliveira, Clare E. Bryant, Brian J. Ferguson
Summary: The innate immune response relies on the ability of host cells to detect and respond to microbial nucleic acids. Toll-like receptors (TLRs) play a crucial role in this process by distinguishing self from non-self. This study focused on TLR21, an avian TLR that recognizes bacterial DNA motifs. The findings suggest that avian TLR21 shares similar activation mechanisms to mammalian TLR9, highlighting the conservation of nucleic acid sensing mechanisms across species.
DEVELOPMENTAL AND COMPARATIVE IMMUNOLOGY
(2024)
Article
Virology
Jing Xiong, Yanjun Jiang, Jinru Zhang, Yanmeng Chen, Yuan Hu
Summary: This study found that CK1α can interact with IFNAR1 during HBV infection, increasing the abundance of IFNAR1 by reducing ubiquitination levels. Additionally, CK1α promotes the JAK-STAT signaling pathway triggered by IFN-α, enhancing its antiviral effects against HBV replication.
Article
Immunology
Gloria Yiu, Tue Kruse Rasmussen, Brandon L. Tsai, Vivian K. Diep, David J. Haddon, Jennifer Tsoi, Gopika D. Miller, Begona Comin-Anduix, Bent Deleuran, Gay M. Crooks, Paul J. Utz
Summary: This study investigates the role of interferon (IFN) signaling in systemic lupus erythematosus (SLE). The results show a correlation between IFN signaling and clinical manifestations as well as immune factors in SLE, suggesting potential targets for future therapeutic approaches.
FRONTIERS IN IMMUNOLOGY
(2022)
Article
Virology
Gennaro Iaconis, Ben Jackson, Kay Childs, Mark Boyce, Stephen Goodbourn, Neil Blake, Miren Iturriza-Gomara, Julian Seago
Summary: This study reveals that the rotavirus NSP1 protein can antagonize the induction of type III and type I interferons, and it is an effective inhibitor of IRF-1, which helps in evading antiviral immunity in the intestinal epithelium.
Article
Multidisciplinary Sciences
Alexandra M. Moore, Lei Zhou, Jing Cui, Luyi Li, Nanping Wu, Alice Yu, Soumya Poddar, Keke Liang, Evan R. Abt, Stephanie Kim, Razmik Ghukasyan, Nooneh Khachatourian, Kristina Pagano, Irmina Elliott, Amanda M. Dann, Rana Riahi, Thuc Le, David W. Dawson, Caius G. Radu, Timothy R. Donahue
Summary: Emerging evidence suggests that intratumoral interferon signaling can trigger targetable vulnerabilities in PDAC by reducing NAD levels through up-regulating NAD-consuming enzymes. This sensitizes PDAC cells to NAMPT inhibition, leading to decreased cell proliferation and invasion in vitro, as well as suppression of tumor growth and metastases in vivo.
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
(2021)
Article
Biochemistry & Molecular Biology
Linyuan Feng, Wanwei Li, Xiaowen Li, Xiaotian Li, Yanhong Ran, Xiaoping Yang, Zemin Deng, Hongjian Li
Summary: Signaling desensitization plays a crucial role in limiting the duration and intensity of signal transduction. This study demonstrates that NMI enhances STAT1 phosphorylation and IFNγ-induced immune responses by sequestering UBC9 and blocking STAT1 sumoylation. NMI also facilitates the translocation of UBC9 from the nucleus to the cytoplasm, inhibiting STAT1 sumoylation. This research reveals the importance of NMI in modulating IFNγ signaling through a desensitization mechanism.
Article
Virology
Jiangwei Song, Yitong Guo, Dan Wang, Rong Quan, Jing Wang, Jue Liu
Summary: The Seneca Valley virus (SVV) inhibits the type I interferon (IFN) response by degrading STAT1, STAT2, and IRF9, and cleaving STAT2, which leads to impaired IFN-stimulated gene activity. Additionally, SVV blocks the nuclear import of STAT1 and STAT2 by degrading karyopherin 1, thereby evading the host immune response.
JOURNAL OF VIROLOGY
(2023)
Article
Gastroenterology & Hepatology
Jiazeng Sun, Guanhui Wu, Florentin Pastor, Naimur Rahman, Wen-Hung Wang, Zhengtao Zhang, Philippe Merle, Lijian Hui, Anna Salvetti, David Durantel, Danzhou Yang, Ourania Andrisani
Summary: The study demonstrates that RNA helicase DDX5 plays a crucial role in regulating STAT1 translation by resolving a G-quadruplex structure in the 5' UTR of STAT1 mRNA, and is essential for IFN response. The absence of DDX5 correlates with reduced STAT1 expression and weakened anti-viral effect of IFN-alpha in HBV-infected cells, highlighting the importance of DDX5 in controlling the dynamic range of IFN response.
Article
Immunology
Annika Wiedemann, Marie Lettau, Ina Wirries, Annemarie Jungmann, Abdulrahman Salhab, Gilles Gasparoni, Henrik E. Mei, Carsten Perka, Joern Walter, Andreas Radbruch, Andreia C. Lino, Thomas Doerner
Summary: The study revealed distinct characteristics of IgA(+) BMPC in response to BCR stimulation, showing higher sensitivity to changes in the checkpoint molecule PD-1 compared to other PC subsets regardless of CD19 expression. This indicates that IgA(+) BMPC may have different regulatory functions independent of their phenotypic heterogeneity based on CD19 expression.
FRONTIERS IN IMMUNOLOGY
(2021)
Article
Immunology
Annika Wiedemann, Marie Lettau, Sarah Y. Weissenberg, Ana-Luisa Stefanski, Eva-Vanessa Schrezenmeier, Hector Rincon-Arevalo, Karin Reiter, Tobias Alexander, Falk Hiepe, Andreia C. Lino, Thomas Dorner
Summary: The study revealed reduced BTLA expression on CD27(-)IgD(+) naive B cells from SLE patients, associated with disease activity, and impaired function. BTLA engagement was found to control CpG/TLR9 activation limiting plasmablast and B cell memory induction, but these functions were compromised in SLE B cells. Inhibition of SYK mimicked the effects of BTLA activity in vitro, suggesting a potential therapeutic principle for SLE.
FRONTIERS IN IMMUNOLOGY
(2021)
Article
Immunology
Hector Rincon-Arevalo, Mira Choi, Ana-Luisa Stefanski, Fabian Halleck, Ulrike Weber, Franziska Szelinski, Bernd Jahrsdorfer, Hubert Schrezenmeier, Carolin Ludwig, Arne Sattler, Katja Kotsch, Alexander Potekhin, Yidan Chen, Gerd R. Burmester, Kai-Uwe Eckardt, Gabriela Maria Guerra, Pawel Durek, Frederik Heinrich, Marta Ferreira-Gomes, Andreas Radbruch, Klemens Budde, Andreia C. Lino, Mir-Farzin Mashreghi, Eva Schrezenmeier, Thomas Doerner
Summary: Patients with kidney failure are at increased risk for SARS-CoV-2 infection, making effective vaccination critical. However, studies have found significantly impaired antibody responses to the BNT162b2 vaccine in kidney transplant recipients and dialysis patients, leading to insufficient immune responses.
SCIENCE IMMUNOLOGY
(2021)
Review
Rheumatology
Franziska Szelinski, Andreia C. Lino, Thomas Doerner
Summary: Recent insights into altered B cell distribution in systemic lupus erythematosus (SLE) have provided new understanding of B cell abnormalities and their role in immune protection, especially in the context of therapeutic targeting with advanced treatment experiences. The key role of B cell requirements in connection with T cells during SARS-Cov2 infection and vaccination emphasizes the importance of considering preservation of protection in targeting pathogenic B cells.
CURRENT OPINION IN RHEUMATOLOGY
(2022)
Article
Immunology
Hector Rincon-Arevalo, Arman Aue, Jacob Ritter, Franziska Szelinski, Dmytro Khadzhynov, Daniel Zickler, Luisa Stefanski, Andreia C. Lino, Sixten Koerper, Kai-Uwe Eckardt, Hubert Schrezenmeier, Thomas Doerner, Eva Schrezenmeier
Summary: Investigating the interferon signaling pathway in immune cells of COVID-19 patients revealed an upregulation of STAT1 and IRF9 in both mild and severe cases, as well as enhanced phosphorylation of STAT1 in severe cases. This dysbalanced JAK/STAT signaling may lead to insufficient transcription of interferon stimulated response elements (ISRE), suggesting a potential predictive biomarker for targeted interferon pathway treatments.
EUROPEAN JOURNAL OF IMMUNOLOGY
(2022)
Article
Immunology
Andrea Cossarizza, Hyun-Dong Chang, Andreas Radbruch, Sergio Abrignani, Richard Addo, Muebeccel Akdis, Immanuel Andrae, Francesco Andreata, Francesco Annunziato, Eduardo Arranz, Petra Bacher, Sudipto Bari, Vincenzo Barnaba, Joana Barros-Martins, Dirk Baumjohann, Cristian G. Beccaria, David Bernardo, Dominic A. Boardman, Jessica Borger, Chotima Boettcher, Leonie Brockmann, Marie Burns, Dirk H. Busch, Garth Cameron, Ilenia Cammarata, Antonino Cassotta, Yinshui Chang, Fernando Gabriel Chirdo, Eleni Christakou, Luka Cicin-Sain, Laura Cook, Alexandra J. Corbett, Rebecca Cornelis, Lorenzo Cosmi, Martin S. Davey, Sara De Biasi, Gabriele De Simone, Genny del Zotto, Michael Delacher, Francesca Di Rosa, James Di Santo, Andreas Diefenbach, Jun Dong, Thomas Doerner, Regine J. Dress, Charles-Antoine Dutertre, Sidonia B. G. Eckle, Pascale Eede, Maximilien Evrard, Christine S. Falk, Markus Feuerer, Simon Fillatreau, Aida Fiz-Lopez, Marie Follo, Gemma A. Foulds, Julia Froebel, Nicola Gagliani, Giovanni Galletti, Anastasia Gangaev, Natalio Garbi, Jose Antonio Garrote, Jens Geginat, Nicholas A. Gherardin, Lara Gibellini, Florent Ginhoux, Dale I. Godfrey, Paola Gruarin, Claudia Haftmann, Leo Hansmann, Christopher M. Harpur, Adrian C. Hayday, Guido Heine, Daniela Carolina Hernandez, Martin Herrmann, Oliver Hoelsken, Qing Huang, Samuel Huber, Johanna E. Huber, Jochen Huehn, Michael Hundemer, William Y. K. Hwang, Matteo Iannacone, Sabine M. Ivison, Hans-Martin Jaeck, Peter K. Jani, Baerbel Keller, Nina Kessler, Steven Ketelaars, Laura Knop, Jasmin Knopf, Hui-Fern Koay, Katja Kobow, Katharina Kriegsmann, H. Kristyanto, Andreas Krueger, Jenny F. Kuehne, Heike Kunze-Schumacher, Pia Kvistborg, Immanuel Kwok, Daniela Latorre, Daniel Lenz, Megan K. Levings, Andreia C. Lino, Francesco Liotta, Heather M. Long, Enrico Lugli, Katherine N. MacDonald, Laura Maggi, Mala K. Maini, Florian Mair, Calin Manta, Rudolf Armin Manz, Mir-Farzin Mashreghi, Alessio Mazzoni, James McCluskey, Henrik E. Mei, Fritz Melchers, Susanne Melzer, Dirk Mielenz, Leticia Monin, Lorenzo Moretta, Gabriele Multhoff, Luis Enrique Munoz, Miguel Munoz-Ruiz, Franziska Muscate, Ambra Natalini, Katrin Neumann, Lai Guan Ng, Antonia Niedobitek, Jana Niemz, Larissa Nogueira Almeida, Samuele Notarbartolo, Lennard Ostendorf, Laura J. Pallett, Amit A. Patel, Gulce Itir Percin, Giovanna Peruzzi, Marcello Pinti, A. Graham Pockley, Katharina Pracht, Immo Prinz, Irma Pujol-Autonell, Nadia Pulvirenti, Linda Quatrini, Kylie M. Quinn, Helena Radbruch, Hefin Rhys, Maria B. Rodrigo, Chiara Romagnani, Carina Saggau, Shimon Sakaguchi, Federica Sallusto, Lieke Sanderink, Inga Sandrock, Christine Schauer, Alexander Scheffold, Hans U. Scherer, Matthias Schiemann, Frank A. Schildberg, Kilian Schober, Janina Schoen, Wolfgang Schuh, Thomas Schueler, Axel R. Schulz, Sebastian Schulz, Julia Schulze, Sonia Simonetti, Jeeshan Singh, Katarzyna M. Sitnik, Regina Stark, Sarah Starossom, Christina Stehle, Franziska Szelinski, Leonard Tan, Attila Tarnok, Julia Tornack, Timothy I. M. Tree, Jasper J. P. van Beek, Willem van de Veen, Klaas van Gisbergen, Chiara Vasco, Nikita A. Verheyden, Anouk von Borstel, Kirsten A. Ward-Hartstonge, Klaus Warnatz, Claudia Waskow, Annika Wiedemann, Anneke Wilharm, James Wing, Oliver Wirz, Jens Wittner, Jennie H. M. Yang, Juhao Yang
Summary: The third edition of Flow Cytometry Guidelines provides comprehensive information on phenotypes and functional assays of major human and murine immune cell subsets, as well as clinical sample analysis and applications in various diseases. It also includes expert tips, tricks, and pitfalls to avoid, making it an essential handbook for researchers.
EUROPEAN JOURNAL OF IMMUNOLOGY
(2021)
Article
Urology & Nephrology
Eva Schrezenmeier, Hector Rincon-Arevalo, Ana-Luisa Stefanski, Alexander Potekhin, Henriette Staub-Hohenbleicher, Mira Choi, Friederike Bachmann, Vanessa Pross, Charlotte Hammett, Hubert Schrezenmeier, Carolin Ludwig, Bernd Jahrsdoerfer, Andreia C. Lino, Kai-Uwe Eckardt, Katja Kotsch, Thomas Doerner, Klemens Budde, Arne Sattler, Fabian Halleck
Summary: The study found that 36% of kidney transplant recipients showed seroconversion after receiving a third dose of vaccine, highlighting the need for individual humoral monitoring and continued efforts to adapt vaccination protocols for immunosuppressed individuals. The quantitative and qualitative changes in cellular immunity associated with seroconversion emphasize the importance of modified vaccination approaches for this at-risk group.
JOURNAL OF THE AMERICAN SOCIETY OF NEPHROLOGY
(2021)
Article
Rheumatology
Ana-Luisa Stefanski, Hector Rincon-Arevalo, Eva Schrezenmeier, Kirsten Karberg, Franziska Szelinski, Jacob Ritter, Bernd Jahrsdoerfer, Hubert Schrezenmeier, Carolin Ludwig, Arne Sattler, Katja Kotsch, Yidan Chen, Anne Claussnitzer, Hildrun Haibel, Fabian Proft, Gabriela Guerra, Pawel Durek, Frederik Heinrich, Marta Ferreira-Gomes, Gerd R. Burmester, Andreas Radbruch, Mir-Farzin Mashreghi, Andreia C. Lino, Thomas Doerner
Summary: Patients with autoimmune inflammatory rheumatic diseases receiving rituximab (RTX) therapy require a minimum of 10 B cells per microliter in the peripheral circulation to mount an appropriate immune response to SARS-CoV-2 vaccination. Functionally relevant B cell depletion results in impaired interferon-gamma secretion by spike-specific CD4 T cells.
ARTHRITIS & RHEUMATOLOGY
(2022)
Article
Rheumatology
Manuel Graf, Sae Lim von Stuckrad, Akinori Uruha, Jens Klotsche, Lydia Zorn-Pauly, Nadine Unterwalder, Thomas Buttgereit, Martin Krusche, Christian Meisel, Gerd R. Burmester, Falk Hiepe, Robert Biesen, Tilmann Kallinich, Werner Stenzel, Udo Schneider, Thomas Rose
Summary: The objective of this study was to evaluate the expression of SIGLEC1 on monocytes as a biomarker for type I interferon activity in idiopathic inflammatory myopathies (IIM). The results showed that SIGLEC1 could distinguish between active and inactive disease and correlated with disease activity longitudinally. SIGLEC1 was also found to be useful for monitoring disease activity and response to treatment in patients with juvenile and adult dermatomyositis.
Review
Dermatology
Van Duc Dang, Ana-Luisa Stefanski, Andreia C. Lino, Thomas Doerner
Summary: B lymphocytes have a critical role in immunity, and in autoimmune diseases, they can exhibit both pathogenic and protective functions. Understanding the different subsets of B cells with these functions can facilitate the development of more specific and personalized therapies.
JOURNAL OF INVESTIGATIVE DERMATOLOGY
(2022)
Article
Immunology
Ana-Luisa Stefanski, Hector Rincon-Arevalo, Eva Schrezenmeier, Kirsten Karberg, Franziska Szelinski, Jacob Ritter, Yidan Chen, Bernd Jahrsdoerfer, Carolin Ludwig, Hubert Schrezenmeier, Andreia C. Lino, Thomas Doerner
Summary: By analyzing the B cell and T cell data before receiving rituximab (RTX) treatment, it is possible to predict the response to vaccination in patients with autoimmune inflammatory rheumatic diseases. The study found that B cells of vaccination responders in the RTX group were mainly naive and transitional cells, while vaccination non-responders had a higher proportion of plasmablasts and double negative B cells. There was also a positive correlation between neutralizing antibodies and B cells expressing HLA-DR and CXCR5, and an inverse correlation with CD95 and CD21low expression. Adequate repopulation of the naive B cell compartment after RTX therapy and expression of exhaustion markers both affect vaccination response.
FRONTIERS IN IMMUNOLOGY
(2022)
Article
Immunology
Van Duc Dang, Elodie Mohr, Franziska Szelinski, Tuan Anh Le, Jacob Ritter, Timo Hinnenthal, Ana-Luisa Stefanski, Eva Schrezenmeier, Soeren Ocvirk, Christian Hipfl, Sebastian Hardt, Qingyu Cheng, Falk Hiepe, Max Loehning, Thomas Doerner, Andreia C. Lino
Summary: A large-scale protein screening identified twelve new molecules specifically expressed by murine ASCs, with stable expression of CD39, CD81, CD130, and CD326 offering improved resolution for ASC identification. Further analysis revealed a subpopulation of ASC in autoimmunity expressing high levels of CD39 and CD326.
FRONTIERS IN IMMUNOLOGY
(2022)
Article
Immunology
Ana-Luisa Stefanski, Hector Rincon-Arevalo, Eva Schrezenmeier, Kirsten Karberg, Franziska Szelinski, Jacob Ritter, Yidan Chen, Christian Meisel, Bernd Jahrsdoerfer, Carolin Ludwig, Hubert Schrezenmeier, Andreia C. Lino, Thomas Doerner
Summary: Durable vaccine-mediated immunity relies on the generation of long-lived plasma cells and memory B cells, differentiating upon germinal center reactions. SARS-CoV-2 mRNA vaccination induces a strong germinal center response in healthy volunteers, but limited data is available about response longevity upon rituximab treatment. This study evaluated humoral and cellular responses upon third vaccination in rheumatoid arthritis patients who initially mounted anti-spike SARS-CoV-2 antibodies after primary vaccination and were later exposed to rituximab. The results showed that rituximab-treated patients had lower levels of anti-SARS-CoV-2 antibodies after the third vaccination but similar neutralizing capacity compared to healthy controls. Despite a significant reduction in B cells, the induction of IgG+ memory B cells was observed in rituximab-treated patients. Only rituximab-treated patients showed a high amount of IgA+ memory B cells and IgA+ plasmablasts after the third vaccination. TNF-secretion and the generation of effector memory CD4 spike-specific T cells were significantly boosted upon the third vaccination. Based on pre-existing affinity matured memory B cells, rituximab-treated patients had a persistent but atypical germinal center immune response accompanied by boosted spike-specific memory CD4 T cells upon SARS-CoV-2 recall vaccination.
FRONTIERS IN IMMUNOLOGY
(2022)
Article
Chemistry, Medicinal
Jakob Hoeppner, Vincent Casteleyn, Robert Biesen, Thomas Rose, Wolfram Windisch, Gerd Ruediger Burmester, Elise Siegert
Summary: This observational study aimed to investigate the potential of Sialic Acid-Binding Ig-like Lectin 1 (SIGLEC-1) as a biomarker for disease phenotype, therapeutic response, and differential diagnosis in Systemic Sclerosis (SSc). The results showed that SIGLEC-1 expression on monocytes in SSc patients was higher than healthy controls but lower than patients with other rheumatic diseases. SIGLEC-1 expression was associated with reduced forced expiratory volume, but not with fibrotic or vascular disease manifestations. SIGLEC-1 remained stable over time and was independent of changes in immunosuppressive therapy. Therefore, SIGLEC-1 can be used to differentiate SSc from other connective tissue diseases, but not as a biomarker for SSc disease manifestations or activity.
Article
Medicine, Research & Experimental
Tuan Anh Le, Van Trung Chu, Andreia C. Lino, Eva Schrezenmeier, Christopher Kressler, Dania Hamo, Klaus Rajewsky, Thomas Doerner, Van Duc Dang
Summary: Gene editing using CRISPR-Cas9 technology in human B cells can help identify gene regulatory networks and therapeutic targets for autoimmune diseases. Targeting IRF4, PRDM1, and XBP1 genes severely impairs B cell survival and plasma cell differentiation. This method provides a new avenue for studying gene functions and identifying plasma cell regulators.
MOLECULAR THERAPY-NUCLEIC ACIDS
(2022)
