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4. Minor Genetic Overlap Among Rheumatoid Arthritis, Myocardial Infarction, and Myocardial Infarction Risk Determinants.

Author

Sysojev, Anton Öberg, Alfredsson, Lars, Klareskog, Lars, Askling, Johan, Baecklund, Eva, Björkman, Lena, Kastbom, Alf, Rantapaää‐Dahlqvist, Solbritt, Turesson, Carl, Silberberg, Gilad N., Saevarsdottir, Saedis, Padyukov, Leonid, Magnusson, Patrik K. E., and Westerlind, Helga

Subjects
MYOCARDIAL infarction risk factors, RHEUMATOID arthritis risk factors, GENETICS of rheumatoid arthritis, MYOCARDIAL infarction, RISK assessment, RESEARCH funding, GENOME-wide association studies, CARDIOVASCULAR diseases risk factors, DESCRIPTIVE statistics, CONFIDENCE intervals, SINGLE nucleotide polymorphisms
Abstract

Objective: The aim of this study was to investigate whether a shared genetic susceptibility exists between individuals with rheumatoid arthritis (RA) and individuals with myocardial infarction (MI)—including major MI risk factors—and to quantify the degree of any such overlap. Methods: Genome‐wide association study (GWAS) data for individuals with RA were constructed from a sample of 26,637 Swedish patients with RA and controls without RA. For patients with MI, GWAS data were obtained from a previously published meta‐analysis. Genome‐wide genetic correlation was estimated via linkage disequilibrium score regression. LAVA was employed to estimate local genetic correlations in ~2,500 nonoverlapping loci, including the major histocompatibility complex. The controls without RA were used for reference panel data. We also assessed stratified estimates of both genome‐wide and local genetic correlation based on subsamples of individuals with seropositive RA and those with seronegative RA. Furthermore, genome‐wide genetic correlation was estimated between RA and selected cardiovascular risk factors to elucidate pleiotropic relationships. Results: Following quality control, our GWAS of patients with RA consisted of 25,826 individuas. Genome‐wide genetic correlation between patients with RA and MI was estimated to 0.13 (95% confidence interval –0.03 to 0.29). Six regions exhibited significant local genetic correlation, though none harbored any known risk single‐nucleotide polymorphisms for either of the two traits. Estimates were similar in both individuals with seropositive RA and those with seronegative RA. No statistically significant genetic correlations were observed between RA risk factors and any of the MI risk factors. Conclusion: Our findings indicate that genetic overlap between patients with RA and MI is minor. Furthermore, genetic overlap between RA and MI risk factors seem unlikely to provide a major contribution to the increased risk of MI observed in patients with RA. [ABSTRACT FROM AUTHOR]

Published
2024
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5. A Novel Fluorescent Immuno-Lectin Assay to Identify Osteoarthritis Associated Glycoforms of Lubricin

Author

Afshari, Ali Reza, primary, Thomsson, Kristina A., additional, Höglund, Jennifer, additional, Ryberg, Henrik, additional, Gidwani, Kamlesh, additional, Pettersson, Kim, additional, Rolfson, Ola, additional, Björkman, Lena I, additional, Eisler, Thomas, additional, Schmidt, Tannin A., additional, Jay, Gregory D., additional, and Karlsson, Niclas G., additional

Published
2024
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6. Function and regulation of GPR84 in human neutrophils.

Author

Forsman, Huamei, Dahlgren, Claes, Mårtensson, Jonas, Björkman, Lena, and Sundqvist, Martina

Subjects
LEUCOCYTES, NEUTROPHILS, G protein coupled receptors, SHORT-chain fatty acids, BLOOD circulation, FREE fatty acids
Abstract

Human neutrophils are components of the innate immune system and are the most abundant white blood cells in the circulation. They are professional phagocytes and express several G protein‐coupled receptors (GPCRs), which are essential for proper neutrophil functions. So far, the two formyl peptide receptors, FPR1 and FPR2, have been the most extensively studied group of neutrophil GPCRs, but recently, a new group, the free fatty acid (FFA) receptors, has attracted growing attention. Neutrophils express two FFA receptors, GPR84 and FFA2, which sense medium‐ and short‐chain fatty acids respectively, and display similar activation profiles. The exact pathophysiological role of GPR84 is not yet fully understood, but it is generally regarded as a pro‐inflammatory receptor that mediates neutrophil activation. In this review, we summarize current knowledge of how GPR84 affects human neutrophil functions and discuss the regulatory mechanisms that control these responses, focusing on the similarities and differences in comparison to the two FPRs and FFA2. LINKED ARTICLES: This article is part of a themed issue GPR84 Pharmacology. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v181.10/issuetoc [ABSTRACT FROM AUTHOR]

Published
2024
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7. Genome-wide investigation of persistence with methotrexate treatment in early rheumatoid arthritis.

Author

Sysojev, Anton Öberg, Saevarsdottir, Saedis, Diaz-Gallo, Lina-Marcela, Silberberg, Gilad N, Alfredsson, Lars, Klareskog, Lars, Baecklund, Eva, Björkman, Lena, Kastbom, Alf, Rantapää-Dahlqvist, Solbritt, Turesson, Carl, Jonsdottir, Ingileif, Stefansson, Kari, Frisell, Thomas, Padyukov, Leonid, Askling, Johan, and Westerlind, Helga

Subjects
CHRONIC disease risk factors, RHEUMATOID arthritis risk factors, GENETICS of rheumatoid arthritis, INFECTION risk factors, RISK assessment, GENOME-wide association studies, EARLY medical intervention, RESEARCH funding, RHEUMATOID arthritis, METHOTREXATE, TREATMENT effectiveness, ANTIRHEUMATIC agents, DESCRIPTIVE statistics, RELATIVE medical risk, SINGLE nucleotide polymorphisms
Abstract

Objectives To investigate the influence of genetic factors on persistence with treatment of early RA with MTX monotherapy. Methods We conducted a genome-wide association study (GWAS) in a sample of 3902 Swedish early-RA patients initiating MTX in DMARD monotherapy as their first-ever DMARD. The outcome, short- and long-term MTX treatment persistence, was defined as remaining on MTX at 1 and at 3 years, respectively, with no additional DMARDs added. As genetic predictors, we investigated individual SNPs, and then calculated a polygenic risk score (PRS) based on SNPs associated with RA risk. The SNP-based heritability of persistence was estimated overall and by RA serostatus. Results No individual SNP reached genome-wide significance (P  < 5 × 10−8), either for persistence at 1 year or at 3 years. The RA PRS was not significantly associated with MTX treatment persistence at 1 year [relative risk (RR) = 0.98 (0.96–1.01)] or at 3 years [RR = 0.96 (0.93–1.00)]. The heritability of MTX treatment persistence was estimated to be 0.45 (0.15–0.75) at 1 year and 0.14 (0–0.40) at 3 years. The results in seropositive RA were comparable with those in the analysis of RA overall, while heritability estimates and PRS RRs were attenuated towards the null in seronegative RA. Conclusion Despite being the largest GWAS on an MTX treatment outcome to date, no genome-wide significant associations were detected. The modest heritability observed, coupled with the broad spread of suggestively associated loci, indicate that genetic influence is of polygenic nature. Nevertheless, MTX monotherapy persistence was lower in patients with a greater genetic disposition, per the PRS, towards RA. [ABSTRACT FROM AUTHOR]

Published
2024
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10. Genome-wide investigation of persistence with methotrexate treatment in early rheumatoid arthritis

Author

Sysojev, Anton Öberg, primary, Saevarsdottir, Saedis, additional, Diaz-Gallo, Lina-Marcela, additional, Silberberg, Gilad N, additional, Alfredsson, Lars, additional, Klareskog, Lars, additional, Baecklund, Eva, additional, Björkman, Lena, additional, Kastbom, Alf, additional, Rantapää-Dahlqvist, Solbritt, additional, Turesson, Carl, additional, Jonsdottir, Ingileif, additional, Stefansson, Kari, additional, Frisell, Thomas, additional, Padyukov, Leonid, additional, Askling, Johan, additional, and Westerlind, Helga, additional

Published
2023
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12. Severe chronic non-bacterial osteomyelitis in combination with total MPO deficiency and responsiveness to TNFα inhibition.

Author

Sundqvist, Martina, Christenson, Karin, Wekell, Per, Björnsdottir, Halla, Rudin, Agnes Dahlstrand, Sanchez Klose, Felix P., Kallinich, Tilmann, Welin, Amanda, Björkman, Lena, Bylund, Johan, Karlsson-Bengtsson, Anna, and Berg, Stefan

Subjects
TERMINATION of treatment, OSTEOMYELITIS, ANTI-inflammatory agents, ETIOLOGY of diseases, REACTIVE oxygen species, GENETIC disorders
Abstract

We describe a female patient suffering from severe chronic non-bacterial osteomyelitis (CNO) with systemic inflammation and advanced malnutrition and complete deficiency of myeloperoxidase (MPO). CNO is a rare autoinflammatory bone disorder associated with dysregulation of the innate immune system. MPO deficiency is a genetic disorder with partial or complete absence of the phagocyte peroxidase MPO. MPO deficiency has no established clinical phenotype but reports indicate increased susceptibility to infection and chronic inflammation. The patient's symptoms began at 10 years of age with pain in the thighs, systemic inflammation and malnutrition. She was diagnosed with CNO at 14 years of age. Treatment with nonsteroidal anti-inflammatory drugs, corticosteroids, bisphosphonates or IL1-receptor antagonists (anakinra) did not relieve the symptoms. However, the patient responded instantly and recovered from her clinical symptoms when treated with TNFα blockade (adalimumab). Three years after treatment initiation adalimumab was withdrawn, resulting in rapid symptom recurrence. When reintroducing adalimumab, the patient promptly responded and went into remission. In addition to clinical and laboratory profiles, neutrophil functions (reactive oxygen species, ROS; neutrophil extracellular traps, NETs; degranulation; apoptosis; elastase activity) were investigated both in a highly inflammatory state (without treatment) and in remission (on treatment). At diagnosis, neither IL1β, IL6, nor TNFα was significantly elevated in serum, but since TNFα blockade terminated the inflammatory symptoms, the disease was likely TNFα-driven. All neutrophil parameters were normal both during treatment and treatment withdrawal, except for MPO-dependent intracellular ROS- and NET formation. The role of total MPO deficiency for disease etiology and severity is discussed. [ABSTRACT FROM AUTHOR]

Published
2023
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17. Truncated lubricin glycans in osteoarthritis stimulate the synoviocyte secretion of VEGFA, IL-8, and MIP-1α: Interplay between O-linked glycosylation and inflammatory cytokines

Author

Huang, Shan, primary, Thomsson, Kristina A., additional, Jin, Chunsheng, additional, Ryberg, Henrik, additional, Das, Nabangshu, additional, Struglics, André, additional, Rolfson, Ola, additional, Björkman, Lena I., additional, Eisler, Thomas, additional, Schmidt, Tannin A., additional, Jay, Gregory D., additional, Krawetz, Roman, additional, and Karlsson, Niclas G., additional

Published
2022
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18. The ketone body acetoacetate activates human neutrophils through FFAR2.

Author

Mårtensson, Jonas, Björkman, Lena, Lind, Simon, Viklund, Moa Bjerhem, Zhang, Linjie, Gutierrez, Saray, Dahlgren, Claes, Sundqvist, Martina, Xie, Xin, and Forsman, Huamei

Subjects
KETONES, NEUTROPHILS, SHORT-chain fatty acids, FREE fatty acids, CELL migration
Abstract

Neutrophils express many surface receptors that sense environmental changes. One such sensor is FFAR2 (free fatty acid receptor 2), a receptor that detects gut microbiota-derived short-chain fatty acids. As such, FFAR2 has been regarded as a molecular link between metabolism and inflammation. Our recent studies on FFAR2, using its endogenous agonist propionate in combination with allosteric modulators, have identified several novel aspects of FFAR2 regulation. A recent study has also identified the ketone body acetoacetate as an endogenous ligand for mouse FFAR2. Whether human FFAR2 also recognizes acetoacetate and how this recognition modulates human neutrophil functions has not been investigated. In this study, we found that acetoacetate can induce a decrease of cAMP and translocation of β-arrestin in cells overexpressing FFAR2. In addition, we show that similar to propionate, FFAR2-specific allosteric modulators enhance acetoacetate-induced transient rise in cytosolic calcium, production of reactive oxygen species, and cell migration in human neutrophils. In summary, we demonstrate that human neutrophils recognize the ketone body acetoacetate through FFAR2. Thus, our data further highlight the key role of FFAR2 in inflammation and metabolism. [ABSTRACT FROM AUTHOR]

Published
2023
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19. G protein coupled pattern recognition receptors expressed in neutrophils: Recognition, activation/modulation, signaling and receptor regulated functions.

Author

Dahlgren, Claes, Lind, Simon, Mårtensson, Jonas, Björkman, Lena, Wu, Yanling, Sundqvist, Martina, and Forsman, Huamei

Subjects
G proteins, PATTERN perception receptors, G protein coupled receptors, LEUCOCYTES, NEUTROPHILS, ALLOSTERIC regulation
Abstract

Summary: Neutrophils, the most abundant white blood cell in human blood, express receptors that recognize damage/microbial associated pattern molecules of importance for cell recruitment to sites of inflammation. Many of these receptors belong to the family of G protein coupled receptors (GPCRs). These receptor‐proteins span the plasma membrane in expressing cells seven times and the down‐stream signaling rely in most cases on an activation of heterotrimeric G proteins. The GPCRs expressed in neutrophils recognize a number of structurally diverse ligands (activating agonists, allosteric modulators, and inhibiting antagonists) and share significant sequence homologies. Studies of receptor structure and function have during the last 40 years generated important information on GPCR biology in general; this knowledge aids in the overall understanding of general pharmacological principles, governing regulation of neutrophil function and inflammatory processes, including novel leukocyte receptor activities related to ligand recognition, biased/functional selective signaling, allosteric modulation, desensitization, and reactivation mechanisms as well as communication (receptor transactivation/cross‐talk) between GPCRs. This review summarizes the recent discoveries and pharmacological hallmarks with focus on some of the neutrophil expressed pattern recognition GPCRs. In addition, unmet challenges, including recognition by the receptors of diverse ligands and how biased signaling mediate different biological effects are described/discussed. [ABSTRACT FROM AUTHOR]

Published
2023
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22. The level of synovial human VEGFA, IL-8 and MIP-1α correlate with truncation of lubricin glycans in osteoarthritis

Author

Huang, Shan, primary, Thomsson, Kristina A., additional, Jin, Chunsheng, additional, Ryberg, Henrik, additional, Das, Nabangshu, additional, Struglics, André, additional, Rolfson, Ola, additional, Björkman, Lena I, additional, Eisler, Thomas, additional, Schmidt, Tannin A., additional, Jay, Gregory D., additional, Krawetz, Roman, additional, and Karlsson, Niclas G., additional

Published
2021
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25. Decrease of core 2 O-glycans on synovial lubricin in osteoarthritis reduces galectin-3 mediated crosslinking

Author

Flowers, Sarah A., primary, Thomsson, Kristina A., additional, Ali, Liaqat, additional, Huang, Shan, additional, Mthembu, Yolanda, additional, Regmi, Suresh C., additional, Holgersson, Jan, additional, Schmidt, Tannin A., additional, Rolfson, Ola, additional, Björkman, Lena I., additional, Sundqvist, Martina, additional, Karlsson-Bengtsson, Anna, additional, Jay, Gregory D., additional, Eisler, Thomas, additional, Krawetz, Roman, additional, and Karlsson, Niclas G., additional

Published
2020
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30. Increased CD11b and Decreased CD62L in Blood and Airway Neutrophils from Long-Term Smokers with and without COPD

Author

Stockfelt, Marit, primary, Christenson, Karin, additional, Andersson, Anders, additional, Björkman, Lena, additional, Padra, Médea, additional, Brundin, Bettina, additional, Ganguly, Koustav, additional, Asgeirsdottir, Helga, additional, Lindén, Sara, additional, Qvarfordt, Ingemar, additional, Bylund, Johan, additional, and Lindén, Anders, additional

Published
2020
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31. Core-2 O-glycans are required for galectin-3 interaction with the osteoarthritis related protein lubricin

Author

Flowers, Sarah A., primary, Thomsson, Kristina A., additional, Ali, Liaqat, additional, Huang, Shan, additional, Mthembu, Yolanda, additional, Regmi, Suresh C., additional, Holgersson, Jan, additional, Schmidt, Tannin A., additional, Rolfson, Ola, additional, Björkman, Lena I, additional, Sundqvist, Martina, additional, Karlsson, Anna, additional, Jay, Gregory D., additional, Eisler, Thomas, additional, Krawetz, Roman, additional, and Karlsson, Niclas G., additional

Published
2019
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34. Cathepsin g degrades synovial fluid lubricin: relevance for osteoarthritis pathogenesis

Author

Huang, Shan, primary, Thomsson, Kristina A., additional, Jin, Chunsheng, additional, Alweddi, Sally, additional, Struglics, André, additional, Rolfson, Ola, additional, Björkman, Lena I, additional, Kalamajski, Sebastian, additional, Schmidt, Tannin A., additional, Jay, Gregory D., additional, Krawetz, Roman, additional, Karlsson, Niclas G., additional, and Eisler, Thomas, additional

Published
2019
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35. Data on the NADPH-oxidase activity induced by WKYMVm and galectin-3 in bone marrow derived and exudated neutrophils isolated from four different mouse strains

Author

Björkman, Lena, Forsman, Huamei, and Önnheim, Karin

Subjects
Neutrophils, Mouse strain, Galectin-3, lcsh:R858-859.7, Formyl peptide receptor agonist, lcsh:Computer applications to medicine. Medical informatics, lcsh:Science (General), NADPH-oxidase, Data Article, lcsh:Q1-390
Abstract

Neutrophils are the key players in inflammatory reactions and the release of superoxide through the NADPH-oxidase upon neutrophil activation contributes to bacterial clearance and surrounding tissue damage. Here we describe data on the mouse neutrophil NADPH-oxidase activation induced by the mouse formyl peptide receptor (Fpr) agonist WKYMVm and galectin-3. Neutrophils isolated from bone marrow, peritoneal exudated, and in vitro TNFα primed bone marrow neutrophils from four different laboratory strains (C57BL/6, DBA/1, BALB/c and NMRI) were used. Both Fpr agonist and galectin-3 activated neutrophils to release superoxide. No differences were observed in the amounts of superoxide released from neutrophils derived from four different strains.

Published
2017

39. The neutrophil subset defined by CD177 expression is preferentially recruited to gingival crevicular fluid in periodontitis.

Author

Dahlstrand Rudin, Agnes, Amirbeagi, Firoozeh, Davidsson, Lisa, Khamzeh, Arsham, Thorbert Mros, Sara, Thulin, Pontus, Welin, Amanda, Björkman, Lena, Christenson, Karin, and Bylund, Johan

Subjects
GINGIVAL fluid, PERIODONTITIS, SYNOVIAL fluid, CELL membranes, NEUTROPHILS
Abstract

In recent years, the concept of distinct subpopulations of human neutrophils has attracted much attention. One bona fide subset marker, exclusively expressed by a proportion of circulating neutrophils in a given individual, and therefore dividing neutrophils in two distinct subpopulations, is the glycoprotein CD177. CD177 is expressed on the plasma and granule membranes of 0–100% of circulating neutrophils depending on the donor. Several in vitro studies have linked CD177 to neutrophil transmigration, yet very few have looked at the role of CD177 for tissue recruitment in vivo. We investigate whether the CD177+ and CD177– neutrophil subsets differ in their propensity to migrate to both aseptic‐ and microbe‐triggered inflamed human tissues. Microbe‐triggered neutrophil migration was evaluated in samples of gingival crevicular fluid (GCF) from patients with periodontitis, whereas neutrophil migration to aseptic inflammation was evaluated in synovial fluid from patients with inflammatory arthritis, as well as in exudate from experimental skin chambers applied on healthy donors. We found that the proportion of CD177+ neutrophils was significantly higher in GCF from patients with periodontitis, as compared to blood from the same individuals. Such accumulation of CD177+ neutrophils was not seen in the two models of aseptic inflammation. Moreover, the proportion of CD177+ neutrophils in circulation was significantly higher in the periodontitis patient group, as compared to healthy donors. Our data indicate that the CD177+ neutrophil subset is preferentially recruited to the gingival crevice of periodontitis patients, and may imply that this subtype is of particular importance for situations of microbe‐driven inflammation. [ABSTRACT FROM AUTHOR]

Published
2021
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40. The two neutrophil members of the formylpeptide receptor family activate the NADPH-oxidase through signals that differ in sensitivity to a gelsolin derived phosphoinositide-binding peptide

Author

Karlsson Jennie, Karlsson Anna, Janmey Paul, Björkman Lena, Fu Huamei, Movitz Charlotta, and Dahlgren Claes

Subjects
Cytology, QH573-671
Abstract

Abstract Background The formylpeptide receptor family members FPR and FPRL1, expressed in myeloid phagocytes, belong to the G-protein coupled seven transmembrane receptor family (GPCRs). They share a high degree of sequence similarity, particularly in the cytoplasmic domains involved in intracellular signaling. The established model of cell activation through GPCRs states that the receptors isomerize from an inactive to an active state upon ligand binding, and this receptor transformation subsequently activates the signal transducing G-protein. Accordingly, the activation of human neutrophil FPR and FPRL1 induces identical, pertussis toxin-sensitive functional responses and a transient increase in intracellular calcium is followed by a secretory response leading to mobilization of receptors from intracellular stores, as well as a release of reactive oxygen metabolites. Results We report that a cell permeable ten amino acid peptide (PBP10) derived from the phosphatidylinositol 4,5-bisphosphate (PIP2) binding region of gelsolin (an uncapper of actin filaments) blocks granule mobilization as well as secretion of oxygen radicals. The inhibitory effect of PBP10 is, however, receptor specific and affects the FPRL1-, but not the FPR-, induced cellular response. The transient rise in intracellular calcium induced by the active receptors is not affected by PBP10, suggesting that the blockage occurs in a parallel, novel signaling pathway used by FPRL1 to induce oxygen radical production and secretion. Also the FPR can activate neutrophils through a PBP10-sensitive signaling pathway, but this signal is normally blocked by the cytoskeleton. Conclusions This study demonstrates that the two very closely related chemoattractant receptors, FPR and FPRL1, use distinct signaling pathways in activation of human neutrophils. The PIP2-binding peptide PBP10 selectively inhibits FPRL1-mediated superoxide production and granule mobilization. Furthermore, the activity of this novel PBP10 sensitive pathway in neutrophils is modulated by the actin cytoskeleton network.

Published
2004
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41. Lubricin binds cartilage proteins, cartilage oligomeric matrix protein, fibronectin and collagen II at the cartilage surface

Author

Flowers, Sarah A., Zieba, Agata, Örnros, Jessica, Jin, Chunsheng, Rolfson, Ola, Björkman, Lena I., Eisler, Thomas, Kalamajski, Sebastian, Kamali-Moghaddam, Masood, and Karlsson, Niclas G.

Subjects
Cartilage, Articular, Male, musculoskeletal diseases, Medicin och hälsovetenskap, lcsh:R, lcsh:Medicine, Cartilage Oligomeric Matrix Protein, musculoskeletal system, Immunohistochemistry, Medical and Health Sciences, Article, Fibronectins, Mice, Animals, Humans, lcsh:Q, Collagen, lcsh:Science, Aged, Glycoproteins
Abstract

Lubricin, a heavily O-glycosylated protein, is essential for boundary lubrication of articular cartilage. Strong surface adherence of lubricin is required given the extreme force it must withstand. Disulfide bound complexes of lubricin and cartilage oligomeric matrix protein (COMP) have recently been identified in arthritic synovial fluid suggesting they may be lost from the cartilage surface in osteoarthritis and inflammatory arthritis. This investigation was undertaken to localise COMP-lubricin complexes within cartilage and investigate if other cartilage proteins are involved in anchoring lubricin to the joint. Immunohistochemical analysis of human cartilage biopsies showed lubricin and COMP co-localise to the cartilage surface. COMP knockout mice, however, presented with a lubricin layer on the articular cartilage leading to the further investigation of additional lubricin binding mechanisms. Proximity ligation assays (PLA) on human cartilage biopsies was used to localise additional lubricin binding partners and demonstrated that lubricin bound COMP, but also fibronectin and collagen II on the cartilage surface. Fibronectin and collagen II binding to lubricin was confirmed and characterised by solid phase binding assays with recombinant lubricin fragments. Overall, COMP, fibronectin and collagen II bind lubricin, exposed on the articular cartilage surface suggesting they may be involved in maintaining essential boundary lubrication.

Published
2017

43. Similarities and differences between the responses induced in human phagocytes through activation of the medium chain fatty acid receptor GPR84 and the short chain fatty acid receptor FFA2R

Author

Sundqvist, Martina, primary, Christenson, Karin, additional, Holdfeldt, André, additional, Gabl, Michael, additional, Mårtensson, Jonas, additional, Björkman, Lena, additional, Dieckmann, Regis, additional, Dahlgren, Claes, additional, and Forsman, Huamei, additional

Published
2018
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46. The Neutrophil Response Induced by an Agonist for Free Fatty Acid Receptor 2 (GPR43) Is Primed by Tumor Necrosis Factor Alpha and by Receptor Uncoupling from the Cytoskeleton but Attenuated by Tissue Recruitment

Author

Björkman, Lena, primary, Mårtensson, Jonas, additional, Winther, Malene, additional, Gabl, Michael, additional, Holdfeldt, André, additional, Uhrbom, Martin, additional, Bylund, Johan, additional, Højgaard Hansen, Anders, additional, Pandey, Sunil K., additional, Ulven, Trond, additional, Forsman, Huamei, additional, and Dahlgren, Claes, additional

Published
2016
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47. Neutrophil recruitment to inflamed joints can occur without cellular priming.

Author

Björkman, Lena, Davidsson, Lisa, Mårtensson, Jonas, Welin, Amanda, Forsman, Huamei, Karlsson, Anna, Dahlgren, Claes, Christenson, Karin, Amirbeagi, Firoozeh, and Bylund, Johan

Subjects
NEUTROPHIL immunology, SYNOVIAL fluid, CELL membranes, JOINTS (Anatomy), NEUTROPHILS, INTEGRINS
Abstract

Recruitment of neutrophils from blood to tissues is a cardinal event in inflammation during which neutrophils switch from a resting, naive state to a preactivated, primed phenotype; the priming process is characterized by alterations in the composition of cell surface adhesins, for example, shedding of l‐selectin and mobilization of granule‐stored integrins to the cell surface. Ligation of chemotactic receptors and interactions with the endothelial lining are established triggers of neutrophil priming and in line with this, in vivo transmigrated neutrophils obtained from tissues are typically highly primed. We here characterize the priming of neutrophils brought about by in vivo recruitment from blood to inflamed joints by the analyses of synovial fluid and blood from patients with inflammatory arthritis. For comparisons, we used controlled in vivo models of neutrophil transmigration to skin of healthy subjects. In contrast to the residing view and in vivo transmigrated neutrophils from skin models, neutrophils from synovial fluid were often surprisingly resting and phenotypically very similar to naive cells isolated from peripheral blood; synovial fluid cells often retained l‐selectin and had undergone minimal up‐regulation of integrin receptors. In complete agreement with our in vivo findings, cell‐free synovial fluid was potently chemotactic without triggering alteration of surface receptors also in vitro. We conclude that tissue recruitment of neutrophils does not by default trigger l‐selectin shedding and granule mobilization, and the chemoattractant(s) guiding neutrophils to synovial fluid apparently operate without inducing cellular priming. [ABSTRACT FROM AUTHOR]

Published
2019
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48. Neutrophils from patients with SAPHO syndrome show no signs of aberrant NADPH oxidase-dependent production of intracellular reactive oxygen species

Author

Wekell, Per, primary, Björnsdottir, Halla, additional, Björkman, Lena, additional, Sundqvist, Martina, additional, Christenson, Karin, additional, Osla, Veronica, additional, Berg, Stefan, additional, Fasth, Anders, additional, Welin, Amanda, additional, Bylund, Johan, additional, and Karlsson, Anna, additional

Published
2016
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49. The Role Of Serum Amyloid A In Inflammatory Disease - Proinflammatory Mediator Or Inert Biomarker?

Author

Björkman, Lena

Subjects
rheumatoid arthritis, neutrophils, serum amyloid A
Abstract

Neutrophils are phagocytes of the innate immune system with prominent roles in host defense and are also believed to be important in autoimmune diseases such as rheumatoid arthritis (RA) by accumulating in inflamed joints and contribute to tissues destruction. Neutrophils differentiate in the bone-marrow and are mature cells when entering circulation with a cytoplasm packed with granules that contain toxic substances in addition to receptors that can be up-regulated to the cell surface during activation. Migration into the affected tissue is directed by mediators from the inflamed site which guides neutrophils along a chemotactic gradient and transfers the cell from resting- into a primed state. The inflammatory process triggers a systemic acute phase response characterized by the production of acute phase proteins (APP). The most prominent APP is serum amyloid A (SAA), the concentration of which can increase thousand fold in response to infection, aseptic inflammation or trauma. Patients with RA often have chronically elevated SAA in blood and joints and SAA has been implicated in the pathogenesis of RA. Recombinant SAA (rSAA) has been suggested to possess proinflammatory activities and act as a chemoattractant for neutrophils via a receptor called FPR2. A peptide (PBP10) with intracellular inhibitory activity was shown to allow discrimination between neutrophil signals mediated by FPR2 and the closely related FPR1. Next, the receptor specificity for rSAA was studied by use of PBP10 and another FPR2 specific inhibitor WRW4. rSAA affinity for FPR2 in transfected cell lines was corroborated and rSAA indeed activated primary human neutrophils. However, FPR2 was not responsible for mediating activation of primary human neutrophils by rSAA. Next, proinflammatory activity of rSAA was compared to that of endogenous SAA in circulation of RA patients. Using a sensitive marker for neutrophil activation in peripheral blood, endogenous SAA in circulation lacked proinflammatory activity and thus differed functionally from rSAA. Synovial neutrophils from patients with inflammatory arthritis and elevated SAA in joint fluid were next studied with respect to activation status. Synovial neutrophils displayed a surprisingly resting phenotype despite having transmigrated from peripheral blood to a compartment with endogenous SAA. Endogenous SAA, both in circulation and in joints, lack the proinflammatory properties present in the recombinant molecule. Key-words: neutrophils, serum amyloid A, rheumatoid arthritis ISBN: 978-91-628-8050-7

Published
2010

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