Your search keyword '"Forsman, Huamei"' showing total 33 results

1. Targeting CD38 with monoclonal antibodies disrupts key survival pathways in paediatric Burkitt's lymphoma malignant B cells.

Author

Kläsener, Kathrin, Herrmann, Nadja, Håversen, Liliana, Sundell, Timothy, Sundqvist, Martina, Lundqvist, Christina, Manna, Paul T, Jonsson, Charlotte A, Visentini, Marcella, Ljung Sass, Diana, McGrath, Sarah, Grimstad, Kristoffer, Aranburu, Alaitz, Mellgren, Karin, Fogelstrand, Linda, Forsman, Huamei, Ekwall, Olov, Borén, Jan, Gjertsson, Inger, and Reth, Michael

Subjects

BURKITT'S lymphoma, B cell lymphoma, METABOLIC reprogramming, MEMBRANE proteins, CELL proliferation

Abstract

Objectives: Paediatric Burkitt's lymphoma (pBL) is the most common childhood non‐Hodgkin B‐cell lymphoma. Despite the encouraging survival rates for most children, treating cases with relapse/resistance to current therapies remains challenging. CD38 is a transmembrane protein highly expressed in pBL. This study investigates the effectiveness of CD38‐targeting monoclonal antibodies (mAbs), daratumumab and isatuximab, in impairing crucial cellular processes and survival pathways in pBL malignant cells. Methods: In silico analyses of patient samples, combined with in vitro experiments using the Ramos cell line, were conducted to assess the impact of daratumumab and isatuximab on cellular proliferation, apoptosis and the phosphoinositide 3‐kinase (PI3K) pathway. Results: Isatuximab was found to be more effective than daratumumab in disrupting B‐cell receptor signalling, reducing cellular proliferation and inducing apoptosis. Additionally, isatuximab caused a significant impairment of the PI3K pathway and induced metabolic reprogramming in pBL cells. The study also revealed a correlation between CD38 and MYC expression levels in pBL patient samples, suggesting CD38 involvement in key oncogenic processes. Conclusion: The study emphasises the therapeutic potential of CD38‐targeting mAbs, particularly isatuximab, in pBL. [ABSTRACT FROM AUTHOR]

Published

2024

2. The interaction of innate immune and adaptive immune system.

Author

Wang, Ruyuan, Lan, Caini, Benlagha, Kamel, Camara, Niels Olsen Saraiva, Miller, Heather, Kubo, Masato, Heegaard, Steffen, Lee, Pamela, Yang, Lu, Forsman, Huamei, Li, Xingrui, Zhai, Zhimin, and Liu, Chaohong

Subjects

PATTERN perception receptors, NATURAL immunity, IMMUNE system, B cells, T cells

Abstract

The innate immune system serves as the body's first line of defense, utilizing pattern recognition receptors like Toll‐like receptors to detect pathogens and initiate rapid response mechanisms. Following this initial response, adaptive immunity provides highly specific and sustained killing of pathogens via B cells, T cells, and antibodies. Traditionally, it has been assumed that innate immunity activates adaptive immunity; however, recent studies have revealed more complex interactions. This review provides a detailed dissection of the composition and function of the innate and adaptive immune systems, emphasizing their synergistic roles in physiological and pathological contexts, providing new insights into the link between these two forms of immunity. Precise regulation of both immune systems at the same time is more beneficial in the fight against immune‐related diseases, for example, the cGAS–STING pathway has been found to play an important role in infections and cancers. In addition, this paper summarizes the challenges and future directions in the field of immunity, including the latest single‐cell sequencing technologies, CAR‐T cell therapy, and immune checkpoint inhibitors. By summarizing these developments, this review aims to enhance our understanding of the complexity interactions between innate and adaptive immunity and provides new perspectives in understanding the immune system. [ABSTRACT FROM AUTHOR]

Published

2024

3. Immunoglobulin class‐switch recombination: Mechanism, regulation, and related diseases.

Author

Liu, Jia‐Chen, Zhang, Ke, Zhang, Xu, Guan, Fei, Zeng, Hu, Kubo, Masato, Lee, Pamela, Candotti, Fabio, James, Louisa Katherine, Camara, Niels Olsen Saraiva, Benlagha, Kamel, Lei, Jia‐Hui, Forsman, Huamei, Yang, Lu, Xiao, Wei, Liu, Zheng, and Liu, Chao‐Hong

Subjects

JOB'S syndrome, CYTIDINE deaminase, PRIMARY immunodeficiency diseases, THERAPEUTICS, MULTIPLE myeloma

Abstract

Maturation of the secondary antibody repertoire requires class‐switch recombination (CSR), which switches IgM to other immunoglobulins (Igs), and somatic hypermutation, which promotes the production of high‐affinity antibodies. Following immune response or infection within the body, activation of T cell‐dependent and T cell‐independent antigens triggers the activation of activation‐induced cytidine deaminase, initiating the CSR process. CSR has the capacity to modify the functional properties of antibodies, thereby contributing to the adaptive immune response in the organism. Ig CSR defects, characterized by an abnormal relative frequency of Ig isotypes, represent a rare form of primary immunodeficiency. Elucidating the molecular basis of Ig diversification is essential for a better understanding of diseases related to Ig CSR defects and could provide clues for clinical diagnosis and therapeutic approaches. Here, we review the most recent insights on the diversification of five Ig isotypes and choose several classic diseases, including hyper‐IgM syndrome, Waldenström macroglobulinemia, hyper‐IgD syndrome, selective IgA deficiency, hyper‐IgE syndrome, multiple myeloma, and Burkitt lymphoma, to illustrate the mechanism of Ig CSR deficiency. The investigation into the underlying mechanism of Ig CSR holds significant potential for the advancement of increasingly precise diagnostic and therapeutic approaches. [ABSTRACT FROM AUTHOR]

Published

2024

4. 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

5. Ultra‐high static magnetic fields cause immunosuppression through disrupting B‐cell peripheral differentiation and negatively regulating BCR signaling.

Author

Gu, Heng, Fu, Yufan, Yu, Biao, Luo, Li, Kang, Danqing, Xie, Miaomiao, Jing, Yukai, Chen, Qiuyue, Zhang, Xin, Lai, Juan, Guan, Fei, Forsman, Huamei, Shi, Junming, Yang, Lu, Lei, Jiahui, Du, Xingrong, and Liu, Chaohong

Subjects

B cells, IMMUNOSUPPRESSION, MAGNETIC fields, CELLULAR signal transduction, CELL membranes

Abstract

To increase the imaging resolution and detection capability, the field strength of static magnetic fields (SMFs) in magnetic resonance imaging (MRI) has significantly increased in the past few decades. However, research on the side effects of high magnetic field is still very inadequate and the effects of SMF above 1 T (Tesla) on B cells have never been reported. Here, we show that 33.0 T ultra‐high SMF exposure causes immunosuppression and disrupts B cell differentiation and signaling. 33.0 T SMF treatment resulted in disturbance of B cell peripheral differentiation and antibody secretion and reduced the expression of IgM on B cell membrane, and these might be intensity dependent. In addition, mice exposed to 33.0 T SMF showed inhibition on early activation of B cells, including B cell spreading, B cell receptor clustering and signalosome recruitment, and depression of both positive and negative molecules in the proximal BCR signaling, as well as impaired actin reorganization. Sequencing and gene enrichment analysis showed that SMF stimulation also affects splenic B cells' transcriptome and metabolic pathways. Therefore, in the clinical application of MRI, we should consider the influence of SMF on the immune system and choose the optimal intensity for treatment. [ABSTRACT FROM AUTHOR]

Published

2023

6. 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

7. The allosterically modulated FFAR2 is transactivated by signals generated by other neutrophil GPCRs.

Author

Lind, Simon, Granberg, Kenneth L., Forsman, Huamei, and Dahlgren, Claes

Subjects

NEUTROPHILS, G protein coupled receptors, PURINERGIC receptors, PLATELET activating factor, FREE fatty acids, G proteins, CELL membranes

Abstract

Positive allosteric modulators for free fatty acid receptor 2 (FFAR2/GPR43), that affect receptor function through binding to two distinct allosteric binding sites, were used to determine the correlation between the responses induced in neutrophils by two distinct activation modes; FFAR2 was activated either by the orthosteric agonist propionate or by a receptor transactivation mechanism that activated FFAR2 from the cytosolic side of the neutrophil plasma membrane by signals generated by the neutrophil PAFR (receptor for platelet activating factor), P2Y2R (receptor for ATP), FPR1 (receptor for fMLF) and FPR2 (receptor for WKYMVM). We show that the transactivation signals that activate FFAR2 in the absence of any orthosteric agonist were generated downstream of the signaling G protein that couple to PAFR and P2Y2R. This transactivation of allosterically modulated FFAR2s, by signals generated by PAFR/P2Y2R, represents a novel mechanism by which a G protein coupled receptor can be activated. Weak correlations were obtained when the FFAR2 activity was induced by the transactivation signals generated by PAFRs and P2Y2Rs were compared with the FFAR2 activity induced by the orthosteric agonist propionate. Comparison of the responses for each allosteric modulator revealed that the ratio values, calculated from the peak values of the ATP and propionate responses, varied from 0.2 to 1. Depending on the allosteric modulator, the response induced by the two different mechanisms (orthosteric activation and receptor transactivation, respectively), was equal or the propionate response was more pronounced. Importantly, we conclude that FFAR2 activation from outside (orthosteric activation) and inside (receptor cross-talk/transactivation) can be selectively affected by an allosteric FFAR2 modulator. [ABSTRACT FROM AUTHOR]

Published

2023

8. 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

9. Phenol-soluble modulin α and β display divergent roles in mice with staphylococcal septic arthritis.

Author

Hu, Zhicheng, Kopparapu, Pradeep Kumar, Ebner, Patrick, Mohammad, Majd, Lind, Simon, Jarneborn, Anders, Dahlgren, Claes, Schultz, Michelle, Deshmukh, Meghshree, Pullerits, Rille, Nega, Mulugeta, Nguyen, Minh-Thu, Fei, Ying, Forsman, Huamei, Götz, Friedrich, and Jin, Tao

Subjects

INFECTIOUS arthritis, STAPHYLOCOCCAL diseases, PHORBOL esters, PEPTIDE receptors, NICOTINAMIDE adenine dinucleotide phosphate, MICE, STAPHYLOCOCCUS aureus

Abstract

Phenol-soluble modulin α (PSMα) is identified as potent virulence factors in Staphylococcus aureus (S. aureus) infections. Very little is known about the role of PSMβ which belongs to the same toxin family. Here we compared the role of PSMs in S. aureus-induced septic arthritis in a murine model using three isogenic S. aureus strains differing in the expression of PSMs (Newman, Δpsmα, and Δpsmβ). The effects of PSMs on neutrophil NADPH-oxidase activity were determined in vitro. We show that the PSMα activates neutrophils via the formyl peptide receptor (FPR) 2 and reduces their NADPH-oxidase activity in response to the phorbol ester PMA. Despite being a poor neutrophil activator, PSMβ has the ability to reduce the neutrophil activating effect of PSMα and to partly reverse the effect of PSMα on the neutrophil response to PMA. Mice infected with S. aureus lacking PSMα had better weight development and lower bacterial burden in the kidneys compared to mice infected with the parental strain, whereas mice infected with bacteria lacking PSMβ strain developed more severe septic arthritis accompanied with higher IL-6 and KC. We conclude that PSMα and PSMβ play distinct roles in septic arthritis: PSMα aggravates systemic infection, whereas PSMβ protects arthritis development. Phenol-soluble modulin α and β display divergent roles in staphylococcal infection and its associated septic arthritis - whereas PSMα is a virulence factor for neutrophils that worsens infection, PSMβ protects from the development of septic arthritis. [ABSTRACT FROM AUTHOR]

Published

2022

10. The Two Formyl Peptide Receptors Differently Regulate GPR84-Mediated Neutrophil NADPH Oxidase Activity.

Author

Mårtensson, Jonas, Sundqvist, Martina, Manandhar, Asmita, Ieremias, Loukas, Zhang, Linjie, Ulven, Trond, Xie, Xin, Björkman, Lena, and Forsman, Huamei

Published

2021

11. Functional selective FPR1 signaling in favor of an activation of the neutrophil superoxide generating NOX2 complex.

Author

Lind, Simon, Dahlgren, Claes, Holmdahl, Rikard, Olofsson, Peter, and Forsman, Huamei

Subjects

SUPEROXIDES, PEPTIDE receptors, REACTIVE oxygen species, SMALL molecules, NEUTROPHILS

Abstract

The formyl peptide receptors FPR1 and FPR2 are abundantly expressed by neutrophils, in which they regulate proinflammatory tissue recruitment of inflammatory cells, the production of reactive oxygen species (ROS), and resolution of inflammatory reactions. The unique dual functionality of the FPRs makes them attractive targets to develop FPR‐based therapeutics as novel anti‐inflammatory treatments. The small compound RE‐04‐001 has earlier been identified as an inducer of ROS in differentiated HL60 cells but the precise target and the mechanism of action of the compound was has until now not been elucidated. In this study, we reveal that RE‐04‐001 specifically targets and activates FPR1, and the concentrations needed to activate the neutrophil NADPH‐oxidase was very low (EC50 ∼1 nM). RE‐04‐001 was also found to be a neutrophil chemoattractant, but when compared to the prototype FPR1 agonist N‐formyl‐Met‐Leu‐Phe (fMLF), the concentrations required were comparably high, suggesting that signaling downstream of the RE‐04‐001‐activated‐FPR1 is functionally selective. In addition, the RE‐04‐001‐induced response was strongly biased toward the PLC‐PIP2‐Ca2+ pathway and ERK1/2 activation but away from β‐arrestin recruitment. Compared to the peptide agonist fMLF, RE‐04‐001 is more resistant to inactivation by the MPO‐H2O2‐halide system. In summary, this study describes RE‐04‐001 as a novel small molecule agonist specific for FPR1, which displays a biased signaling profile that leads to a functional selective activating of human neutrophils. RE‐04‐001 is, therefore, a useful tool, not only for further mechanistic studies of the regulatory role of FPR1 in inflammation in vitro and in vivo, but also for developing FPR1‐specific drug therapeutics. [ABSTRACT FROM AUTHOR]

Published

2021

12. Porphyromonas gingivalis Produce Neutrophil Specific Chemoattractants Including Short Chain Fatty Acids.

Author

Dahlstrand Rudin, Agnes, Khamzeh, Arsham, Venkatakrishnan, Vignesh, Persson, Tishana, Gabl, Michael, Savolainen, Otto, Forsman, Huamei, Dahlgren, Claes, Christenson, Karin, and Bylund, Johan

Subjects

PORPHYROMONAS gingivalis, FATTY acids, BACTERIAL metabolism, NEUTROPHILS, FREE fatty acids, MACROPHAGES, PERIODONTAL disease

Abstract

Neutrophil migration from blood to tissue-residing microbes is governed by a series of chemoattractant gradients of both endogenous and microbial origin. Periodontal disease is characterized by neutrophil accumulation in the gingival pocket, recruited by the subgingival biofilm consisting mainly of gram-negative, anaerobic and proteolytic species such as Porphyromonas gingivalis. The fact that neutrophils are the dominating cell type in the gingival pocket suggests that neutrophil-specific chemoattractants are released by subgingival bacteria, but characterization of chemoattractants released by subgingival biofilm species remains incomplete. In the present study we characterized small (< 3 kDa) soluble chemoattractants released by growing P. gingivalis , and show that these are selective for neutrophils. Most neutrophil chemoattractant receptors are expressed also by mononuclear phagocytes, the free fatty acid receptor 2 (FFAR2) being an exception. In agreement with the selective neutrophil recruitment, the chemotactic activity found in P. gingivalis supernatants was mediated in part by a mixture of short chain fatty acids (SCFAs) that are recognized by FFAR2, and other leukocytes (including monocytes) did not respond to SCFA stimulation. Although SCFAs, produced by bacterial fermentation of dietary fiber in the gut, has previously been shown to utilize FFAR2, our data demonstrate that the pronounced proteolytic metabolism employed by P. gingivalis (and likely also other subgingival biofilm bacteria associated with periodontal diseases) may result in the generation of SCFAs that attract neutrophils to the gingival pocket. This finding highlights the interaction between SCFAs and FFAR2 in the context of P. gingivalis colonization during periodontal disease, but may also have implications for other inflammatory pathologies involving proteolytic bacteria. [ABSTRACT FROM AUTHOR]

Published

2021

13. Functional selective ATP receptor signaling controlled by the free fatty acid receptor 2 through a novel allosteric modulation mechanism.

Author

Lind, Simon, Holdfeldt, André, Mårtensson, Jonas, Sundqvist, Martina, Björkman, Lena, Forsman, Huamei, and Dahlgren, Claes

Published

2019

14. 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

15. Neutrophil priming that turns natural FFA2R agonists into potent activators of the superoxide generating NADPH‐oxidase.

Author

Mårtensson, Jonas, Holdfeldt, André, Sundqvist, Martina, Gabl, Michael, Kenakin, Terry P., Björkman, Lena, Forsman, Huamei, and Dahlgren, Claes

Subjects

NADPH oxidase, FREE fatty acids, NEUTROPHILS, ACETANILIDE, ACETATES

Abstract

Acetate, an agonist for the free fatty acid receptor 2 (FFA2R/GPR43), triggers an increase in the cytosolic concentration of free Ca2+ in neutrophils without any assembly of the superoxide generating NADPH‐oxidase. We show that the phenylacetamide compound 58 (Cmp 58; (S)‐2‐(4‐chlorophenyl)‐3,3‐dimethyl‐N‐(5‐phenylthiazol‐2‐yl)butanamide), lacking a direct activating effect on neutrophils, acts as a positive FFA2R modulator that turns acetate into a potent activating agonist that triggers an assembly of the NADPH‐oxidase. The NADPH‐oxidase activity could be further increased in neutrophils treated with the pro‐inflammatory cytokine TNF‐α. Many neutrophil chemoattractant receptors are stored in secretory organelles but no FFA2R mobilization was induced in neutrophils treated with TNF‐α. The receptor selectivity was demonstrated through the inhibition of the neutrophil response induced by the combined action of acetate and Cmp 58 by the FFA2R antagonist CATPB. Receptor modulators that positively co‐operate with natural FFA2R agonists and prime neutrophils in their response to such agonists, may serve as good tools for further unraveling the physiological functions of FFA2R and its involvement in various diseases. In this study, we show that neutrophils primed with a presumed allosteric FFA2R modulator produce increased amounts of reactive oxygen species when activated by receptor specific agonists. Allosteric modulation of FFA2R, a novel receptor selective mechanism, primes neutrophils to produce increased amounts of reactive oxygen species. [ABSTRACT FROM AUTHOR]

Published

2018

16. Lack of Receptor for Advanced Glycation End Products Leads to Less Severe Staphylococcal Skin Infection but More Skin Abscesses and Prolonged Wound Healing.

Author

Na, Manli, Mohammad, Majd, Fei, Ying, Wang, Wanzhong, Holdfeldt, André, Forsman, Huamei, Ali, Abukar, Pullerits, Rille, and Jin, Tao

Subjects

RECEPTOR for advanced glycation end products (RAGE), STAPHYLOCOCCUS aureus infections, STAPHYLOCOCCAL diseases, SKIN infections, ABSCESS treatment, ANIMAL models of wound healing, VACCINATION, THERAPEUTICS

Abstract

Background: Lack of receptor for advanced glycation end products (RAGE) ameliorates several infections including Staphylococcus aureus pneumonia. We sought to investigate the role of RAGE in staphylococcal skin infection in mice.Methods: Wild-type (WT) and RAGE deficient (RAGE-/-) mice were subcutaneously inoculated with S. aureus SH1000 strain in abscess-forming dose or necrotic dose. Clinical signs of dermatitis, along with histopathological changes, were compared between the groups.Results: The skin lesion size was smaller in RAGE-/- mice. Infected RAGE-/- mice expressed lower proinflammatory cytokines in local skins compared to control mice. Low dose of bacteria caused more abscess formation in RAGE-/- mice compared to skin necrosis that was more often observed in WT mice. As a result of more abscess formation, the wound healing was prolonged in RAGE-/- mice. Importantly, RAGE-/- mice had lower bacterial loads in the skin than controls, which is correlated with higher local levels of myeloperoxidase before skin infection. In vitro, enhanced phagocytic capacity of neutrophils and macrophages obtained from RAGE-/- mice compared to control mice was observed.Conclusions: RAGE deficiency up-regulates phagocytic capacity of phagocytes, resulting in lower bacterial burden in local skin and milder skin lesions in mice with staphylococcal skin infection. [ABSTRACT FROM AUTHOR]

Published

2018

17. Formyl Peptide Receptors in Mice and Men: Similarities and Differences in Recognition of Conventional Ligands and Modulating Lipopeptides.

Author

Winther, Malene, Dahlgren, Claes, and Forsman, Huamei

Subjects

LIGANDS (Biochemistry), LIPOPEPTIDE antibiotics, LABORATORY mice, ALLOSTERIC proteins, INFLAMMATORY bowel diseases

Abstract

Abstract: The pattern recognition formyl peptide receptors (FPRs) belong to the class of G‐protein‐coupled receptors (GPCRs), the largest group of cell surface receptors involved in a range of physiological processes and pathologies. The FPRs have regulatory function in the initiation as well as resolution of inflammatory reactions, making them highly interesting as targets for drug development. Recent research in the GPCR/FPR fields has uncovered novel receptor biology concepts, including biased signalling/functional selectivity, allosteric modulation, receptor reactivation and receptor cross‐talk. When it comes to allosteric modulators, ‘tailor‐made’ lipopeptides (pepducins and lipopeptoids) represent a novel concept of GPCR/FPR regulation. This MiniReview is focused on the basis for recognition of conventional ligands and immunomodulating lipopeptides, novel allosteric modulators for the FPRs, receptors that are highly expressed by both human and mouse neutrophils. The FPRs play key roles in host defence against microbial infections, tissue homeostasis and the initiation as well as resolution of inflammation but there are both similarities and differences in ligand recognition between mice and men. Thus, identification and functional characterization of activating and inhibiting ligands should provide insights into future design of FPR‐based animal models of human diseases and development of therapeutics for treating inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2018

18. Formyl peptide derived lipopeptides disclose differences between the receptors in mouse and men and call the pepducin concept in question.

Author

Winther, Malene, Holdfeldt, André, Sundqvist, Martina, Rajabkhani, Zahra, Gabl, Michael, Bylund, Johan, Dahlgren, Claes, and Forsman, Huamei

Subjects

LIPOPEPTIDE antibiotics, AMINO acid sequence, G protein coupled receptors, NEUTROPHILS, IMMUNOMODULATORS

Abstract

A pepducin is a lipopeptide containing a peptide sequence that is identical to one of the intracellular domains of the G-protein coupled receptor (GPCR) assumed to be the target. Neutrophils express two closely related formyl peptide receptors belonging to the family of GPCRs; FPR1 and FPR2 in human and their respective orthologue Fpr1 and Fpr2 in mouse. By applying the pepducin concept, we have earlier identified FPR2 activating pepducins generated from the third intracellular loop of FPR2. The third intracellular loop of FPR2 differs in two amino acids from that of FPR1, seven from Fpr2 and three from Fpr1. Despite this, we found that pepducins generated from FPR1, FPR2, Fpr1 and Fpr2 all targeted FPR2 in human neutrophils and Fpr2 in mouse, but with different modulating outcomes. Whereas the FPR1/Fpr1 derived pepducins inhibited the FPR2 function in human neutrophils, they activated Fpr2 in mouse. The FPR2 derived pepducin activated FPR2/Fpr2, whereas the pepducin generated from Fpr2 inhibited both FPR2 and Fpr2. In summary, our data demonstrate that pepducins generated from the third intracellular loop of human FPR1/2 and mouse Fpr1/2, all targeted FPR2 in human and Fpr2 in mouse. With respect to the modulating outcomes, pepducin inhibitors identified for FPR2 are in fact activators for Fpr2 in mouse neutrophils. Our data thus questions the validity of pepducin concept regarding their receptor selectivity but supports the notion that FPR2/Fpr2 may recognize a lipopeptide molecular pattern, and highlight the differences in ligand recognition profile between FPR2 and its mouse orthologue Fpr2. [ABSTRACT FROM AUTHOR]

Published

2017

19. Reactivation of Gαi‐coupled formyl peptide receptors is inhibited by Gαq‐selective inhibitors when induced by signals generated by the platelet‐activating factor receptor.

Author

Holdfeldt, André, Dahlstrand Rudin, Agnes, Gabl, Michael, Rajabkhani, Zahra, König, Gabriele M., Kostenis, Evi, Dahlgren, Claes, and Forsman, Huamei

Subjects

PEPTIDE receptors, G proteins, G protein coupled receptors, CROSSTALK

Abstract

Signals generated by the Gαq‐coupled PAF receptor reactivate Gαi‐coupled FPRs. Formyl peptide receptor (FPR)–desensitized neutrophils display increased production/release of superoxide (O2−) when activated by platelet‐activating factor (PAF), a priming of the response achieved through a unique receptor crosstalk mechanism. The aim of this study was to determine the effect of an inhibitor selective for small, heterotrimeric G proteins belonging to the Gαq subclass on that receptor crosstalk. We show that signals generated by FPRs and the PAF receptor (PAFR) induce activation of the neutrophil O2−, producing NADPH‐oxidase, and that response was sensitive to Gαq inhibition in cells activated by PAF, but no inhibition was obtained in cells activated by FPR agonists. Signaling in naive neutrophils is terminated fairly rapidly, and the receptors become homologously desensitized. The downstream sensitivity to Gαq inhibition in desensitized cells displaying increased production/release of O2− through the PAFR receptor crosstalk mechanism also comprised the reactivation of the FPRs, and the activation signals were redirected from the PAFR to the desensitized/reactivated FPRs. The Gαq‐dependent activation signals generated by the PAFRs activate the Gαi‐coupled FPRs, a receptor crosstalk that represents a novel pathway by which G protein‐coupled receptors can be regulated and signaling can be turned on and off. [ABSTRACT FROM AUTHOR]

Published

2017

20. Phenol-soluble Modulin α Peptide Toxins from Aggressive Staphylococcus aureus Induce Rapid Formation of Neutrophil Extracellular Traps through a Reactive Oxygen Species-Independent Pathway.

Author

Björnsdottir, Halla, Rudin, Agnes Dahlstrand, Klose, Felix P., Elmwall, Jonas, Welin, Amanda, Stylianou, Marios, Christenson, Karin, Urban, Constantin F., Forsman, Huamei, Dahlgren, Claes, Karlsson, Anna, and Bylund, Johan

Subjects

STAPHYLOCOCCUS aureus, BACTERIAL toxins, REACTIVE oxygen species

Abstract

Neutrophils have the ability to capture and kill microbes extracellularly through the formation of neutrophil extracellular traps (NETs). These are DNA and protein structures that neutrophils release extracellularly and are believed to function as a defense mechanism against microbes. The classic NET formation process, triggered by, e.g., bacteria, fungi, or by direct stimulation of protein kinase C through phorbol myristate acetate, is an active process that takes several hours and relies on the production of reactive oxygen species (ROS) that are further modified by myeloperoxidase (MPO). We show here that NET-like structures can also be formed by neutrophils after interaction with phenol-soluble modulin α (PSMα) that are cytotoxic membrane-disturbing peptides, secreted from community-acquired methicillin-resistant Staphylococcus aureus (CA-MRSA). The PSMα-induced NETs contained the typical protein markers and were able to capture microbes. The PSMα-induced NET structures were disintegrated upon prolonged exposure to DNase-positive S. aureus but not on exposure to DNase-negative Candida albicans. Opposed to classic NETosis, PSMα-triggered NET formation occurred very rapidly, independently of ROS or MPO, and was also manifest at 4°C. These data indicate that rapid NETs release may result from cytotoxic membrane disturbance by PSMα peptides, a process that may be of importance for CA-MRSA virulence. [ABSTRACT FROM AUTHOR]

Published

2017

21. Formylated MHC Class Ib Binding Peptides Activate Both Human and Mouse Neutrophils Primarily through Formyl Peptide Receptor 1.

Author

Winther, Malene, Holdfeldt, André, Gabl, Michael, Wang, Ji Ming, Forsman, Huamei, and Dahlgren, Claes

Subjects

MAJOR histocompatibility complex, FORMYLATION, CARRIER proteins, NEUTROPHILS, PEPTIDE receptors, MOLECULAR recognition

Abstract

Two different immune recognition systems have evolved in parallel to recognize peptides starting with an N-formylated methionine, and recognition similarities/differences between these two systems have been investigated. A number of peptides earlier characterized in relation to the H2-M3 complex that presents N-formylated peptides to cytotoxic T cells, have been characterized in relation to the formyl peptide receptors expressed by phagocytic neutrophils in both men (FPRs) and mice (Fprs). FPR1/Fpr1 was identified as the preferred receptor for all fMet-containing peptides examined, but there was no direct correlation between H2-M3 binding and the neutrophil activation potencies. Similarly, there was no direct correlation between the activities induced by the different peptides in human and mouse neutrophils, respectively. The formyl group was important in both H2-M3 binding and FPR activation, but FPR2 was the preferred receptor for the non-formylated peptide. The structural requirements differed between the H2-M3 and FPR/Fpr recognition systems and these data suggest that the two recognition systems have different evolutionary traits. [ABSTRACT FROM AUTHOR]

Published

2016

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

Subjects

NEUTROPHILS, CHEMICAL agonists, FREE fatty acids, TUMOR necrosis factors, CYTOSKELETON

Abstract

Ligands with improved potency and selectivity for free fatty acid receptor 2 (FFA2R) have become available, and we here characterize the neutrophil responses induced by one such agonist (Cmp1) and one antagonist (CATPB). Cmp1 triggered an increase in the cytosolic concentration of Ca2+, and the neutrophils were then desensitized to Cmp1 and to acetate, a naturally occurring FFA2R agonist. The antagonist CATPB selectively inhibited responses induced by Cmp1 or acetate. The activated FFA2R induced superoxide anion secretion at a low level in naive blood neutrophils. This response was largely increased by tumor necrosis factor alpha (TNF-α) in a process associated with a recruitment of easily mobilizable granules, but neutrophils recruited to an aseptic inflammation in vivo were nonresponding. Superoxide production induced by Cmp1 was increased in latrunculin A-treated neutrophils, but no reactivation of desensitized FFA2R was induced by this drug, suggesting that the cytoskeleton is not directly involved in terminating the response. The functional and regulatory differences between the receptors that recognize short-chain fatty acids and formylated peptides, respectively, imply different roles of these receptors in the orchestration of inflammation and confirm the usefulness of a selective FFA2R agonist and antagonist as tools for the exploration of the precise role of the FFA2R. [ABSTRACT FROM AUTHOR]

Published

2016

23. A neutrophil inhibitory pepducin derived from FPR1 expected to target FPR1 signaling hijacks the closely related FPR2 instead.

Author

Winther, Malene, Gabl, Michael, Welin, Amanda, Dahlgren, Claes, and Forsman, Huamei

Subjects

NEUTROPHILS, FORMYL peptide receptors, CELLULAR signal transduction, G protein coupled receptors, SUPEROXIDES, ANTI-inflammatory agents

Abstract

Pepducins constitute a unique class of G-protein coupled receptor (GPCR) modulating lipopeptides. Pepducins with inhibitory effects on neutrophils could potentially be developed into anti-inflammatory pharmaceuticals. A pepducin with a peptide sequence identical to the third intracellular loop of FPR1 was found to inhibit neutrophil functions including granule mobilization and superoxide production. This FPR1-derived pepducin selectively inhibited signaling and cellular responses through FPR2, but not FPR1 as expected. Binding to the neutrophil surface of a conventional FPR2 agonist is also inhibited. The fatty acid is essential for inhibition and pepducins with shorter peptides lose in potency. In summary, a pepducin designed to target FPR1 was found to hijack FPR2 and potently inhibit neutrophil functions. [ABSTRACT FROM AUTHOR]

Published

2015

24. A Pepducin Derived from the Third Intracellular Loop of FPR2 Is a Partial Agonist for Direct Activation of This Receptor in Neutrophils But a Full Agonist for Cross-Talk Triggered Reactivation of FPR2.

Author

Gabl, Michael, Winther, Malene, Skovbakke, Sarah Line, Bylund, Johan, Dahlgren, Claes, and Forsman, Huamei

Subjects

NEUTROPHILS, SIGNAL processing, G protein coupled receptors, SOCIALIZATION agents, PEPTIDE receptors

Abstract

We recently described a novel receptor cross-talk mechanism in neutrophils, unique in that the signals generated by the PAF receptor (PAFR) and the ATP receptor (P2Y2R) transfer formyl peptide receptor 1 (FPR1) from a desensitized (non-signaling) state back to an actively signaling state (Forsman H et al., PLoS One, 8:e60169, 2013; Önnheim K, et al., Exp Cell Res, 323∶209, 2014). In addition to the G-protein coupled FPR1, neutrophils also express the closely related receptor FPR2. In this study we used an FPR2 specific pepducin, proposed to work as an allosteric modulator at the cytosolic signaling interface, to determine whether the cross-talk pathway is utilized also by FPR2. The pepducin used contains a fatty acid linked to a peptide sequence derived from the third intracellular loop of FPR2, and it activates as well as desensensitizes this receptor. We now show that neutrophils desensitized with the FPR2-specific pepducin display increased cellular responses to stimulation with PAF or ATP. The secondary PAF/ATP induced response was sensitive to FPR2-specific inhibitors, disclosing a receptor cross-talk mechanism underlying FPR2 reactivation. The pepducin induced an activity in naïve cells similar to that of a conventional FPR2 agonist, but with lower potency (partial efficacy), meaning that the pepducin is a partial agonist. The PAF- or ATP-induced reactivation was, however, much more pronounced when neutrophils had been desensitized to the pepducin as compared to cells desensitized to conventional agonists. The pepducin should thus in this respect be classified as a full agonist. In summary, we demonstrate that desensitized FPR2 can be transferred back to an actively signaling state by receptor cross-talk signals generated through PAFR and P2Y2R, and the difference in agonist potency with respect to pepducin-induced direct receptor activation and cross-talk reactivation of FPR2 puts the concept of functional selectivity in focus. [ABSTRACT FROM AUTHOR]

Published

2014

25. The role of total and cartilage-specific estrogen receptor alpha expression for the ameliorating effect of estrogen treatment on arthritis.

Author

Engdahl, Cecilia, Börjesson, Anna E., Forsman, Huamei F., Andersson, Annica, Stubelius, Alexandra, Krust, Andree, Chambon, Pierre, Islander, Ulrika, Ohlsson, Claes, Carlsten, Hans, and Lagerquist, Marie K.

Published

2014

26. Reactivation of Desensitized Formyl Peptide Receptors by Platelet Activating Factor: A Novel Receptor Cross Talk Mechanism Regulating Neutrophil Superoxide Anion Production.

Author

Forsman, Huamei, Önnheim, Karin, Andréasson, Emil, Christenson, Karin, Karlsson, Anna, Bylund, Johan, and Dahlgren, Claes

Subjects

FORMYL peptide receptors, PLATELET activating factor, NEUTROPHILS, MICROBIOLOGY, CELLULAR signal transduction, COMMUNICABLE diseases, REGULATOR of G-protein-signaling proteins, PHARMACEUTICAL chemistry

Abstract

Neutrophils express different chemoattractant receptors of importance for guiding the cells from the blood stream to sites of inflammation. These receptors communicate with one another, a cross talk manifested as hierarchical, heterologous receptor desensitization. We describe a new receptor cross talk mechanism, by which desensitized formyl peptide receptors (FPRdes) can be reactivated. FPR desensitization is induced through binding of specific FPR agonists and is reached after a short period of active signaling. The mechanism that transfers the receptor to a non-signaling desensitized state is not known, and a signaling pathway has so far not been described, that transfers FPRdes back to an active signaling state. The reactivation signal was generated by PAF stimulation of its receptor (PAFR) and the cross talk was uni-directional. LatrunculinA, an inhibitor of actin polymerization, induced a similar reactivation of FPRdes as PAF while the phosphatase inhibitor CalyculinA inhibited reactivation, suggesting a role for the actin cytoskeleton in receptor desensitization and reactivation. The activated PAFR could, however, reactivate FPRdes also when the cytoskeleton was disrupted prior to activation. The receptor cross talk model presented prophesies that the contact on the inner leaflet of the plasma membrane that blocks signaling between the G-protein and the FPR is not a point of no return; the receptor cross-talk from the PAFRs to the FPRdes initiates an actin-independent signaling pathway that turns desensitized receptors back to a signaling state. This represents a novel mechanism for amplification of neutrophil production of reactive oxygen species. [ABSTRACT FROM AUTHOR]

Published

2013

27. Galectin 3 aggravates joint inflammation and destruction in antigen-induced arthritis.

Author

Forsman, Huamei, Islander, Ulrika, Andréasson, Emil, Andersson, Annica, Önnheim, Karin, Karlström, Alexandra, Sävman, Karin, Magnusson, Mattias, Brown, Kelly L., and Karlsson, Anna

Subjects

ANALYSIS of variance, ANIMAL experimentation, ARTHRITIS, FLOW cytometry, INFLAMMATION, MICE, RESEARCH funding, STATISTICS

Abstract

The article presents a study to investigate the influence of galectin 3 deficiency in a murine model of arthritis. Wild-type (WT) and galectin 3–deficient (galectin 3&sup–/–;) mice were subjected to antigen-induced arthritis (AIA), and the concentration of serum cytokines, antigen-specific antibodies and cellular IL-17 responses were examined. Galectin 3&sup–/–; mice showed a relatively greater suppression in joint inflammation and bone erosion, thereby suggesting that galectin 3 plays a pathogenic role in the development and progression of AIA.

Published

2011

28. Negative regulation of Toll-like receptor signaling plays an essential role in homeostasis of the intestine.

Author

Biswas, Amlan, Wilmanski, Jeanette, Forsman, Huamei, Hrncir, Tomas, Hao, Liming, Tlaskalova-Hogenova, Helena, and Kobayashi, Koichi S.

Abstract

A healthy intestinal tract is characterized by controlled homeostasis due to the balanced interaction between commensal bacteria and the host mucosal immune system. Human and animal model studies have supported the hypothesis that breakdown of this homeostasis may underlie the pathogenesis of inflammatory bowel diseases. However, it is not well understood how intestinal microflora stimulate the intestinal mucosal immune system and how such activation is regulated. Using a spontaneous, commensal bacteria-dependent colitis model in IL-10-deficient mice, we investigated the role of TLR and their negative regulation in intestinal homeostasis. In addition to IL-10 [ABSTRACT FROM AUTHOR]

Published

2011

29. The FPR2-induced rise in cytosolic calcium inhuman neutrophils relies on an emptying ofintracellular calcium stores and is inhibited by agelsolin-derived PIP2-binding peptide.

Author

Forsman, Huamei and Dahlgren, Claes

Subjects

INTRACELLULAR calcium, NEUTROPHILS, G proteins, CELL receptors, CELLULAR signal transduction, CHEMICAL agonists

Abstract

Background: The molecular basis for neutrophil recognition of chemotactic peptides is their binding to specific Gprotein- coupled cell surface receptors (GPCRs). Human neutrophils express two pattern recognition GPCRs, FPR1 and FPR2, which belong to the family of formyl peptide receptors. The high degree of homology between these two receptors suggests that they share many functional and signal transduction properties, although they exhibit some differences with respect to signaling. The aims of this study were to determine whether FPR2 triggers a unique signal that allows direct influx of extracellular calcium without the emptying of intracellular calcium stores, and whether the gelsolin-derived PIP2-binding peptide, PBP10, selectively inhibits FPR2-mediated transient rise in intracellular Ca2+. Results: The transient rise in intracellular Ca2+ induced by agonists for FPR1 or FPR2 in human neutrophils occurred also in the presence of a chelator of Ca2+ (EGTA). PBP10 inhibited not only FPR2-induced oxidase activity, but also the transient rise in intracellular Ca2+. Conclusions: Ca2+ signaling mediated via FPR2 follows the same route as FPR1, which involves initial emptying of the intracellular stores. PBP10 inhibits selectively the signals generated by FPR2, both with respect to NADPH-oxidase activity and the transient rise in intracellular Ca2+ induced by agonist exposure. [ABSTRACT FROM AUTHOR]

Published

2010

30. Tumour necrosis factor (TNF)-α primes murine neutrophils when triggered via formyl peptide receptor-related sequence 2, the murine orthologue of human formyl peptide receptor-like 1, through a process involving the type I TNF receptor and subcellular granule mobilization

Author

Önnheim, Karin, Bylund, Johan, Boulay, Francois, Dahlgren, Claes, and Forsman, Huamei

Subjects

TUMOR necrosis factors, NEUTROPHILS, REACTIVE oxygen species, MICROBIAL invasiveness, CELLULAR immunity

Abstract

Neutrophil granulocytes play an important role in innate host defence against microbial invasions and they are also the key effector cells in mediating host tissue damage. These functions often rely on the production of reactive oxygen species (ROS) from the membrane-bound NADPH-oxidase system. The magnitude of ROS production varies depending on the state of the cells, i.e. resting or primed. Many priming agents as well as potent NADPH-oxidase activators have been identified and characterized for human neutrophils. The cytokine tumour necrosis factor (TNF)-α is one prominent example of a priming agent and the synthetic hexapeptide WKYMVm is an agonist that triggers an activation of the NADPH-oxidase of human neutrophils through two members of the formyl peptide family of receptors, formyl peptide receptor (FPR) and FPR-like 1 (FPRL1). This peptide also activates murine neutrophils but the precise receptor involved has not been previously characterized. We show in this study that WKYMVm activates stably transfected HL60 cells expressing murine formyl peptide receptor-related sequence 2 (Fpr-rs2) and that activation of murine neutrophils with WKYMVm is blocked by an FPRL1-specific antagonist. WKYMVm is thus an agonist for Fpr-rs2 and we suggest that this receptor is in fact the mouse orthologue of FPRL1. In addition, we show that the WKYMVm response in murine neutrophils can be primed by TNF-α and this priming process involves mobilization of subcellular granules. The results obtained using neutrophils derived from TNF receptor type I (TNFRI)-deficient animals suggest that TNF-α exerts its priming effect via the TNFRI. [ABSTRACT FROM AUTHOR]

Published

2008

31. Functional characteristics of circulating granulocytes in severe congenital neutropenia caused by ELANE mutations.

Author

Liu, Qiao, Sundqvist, Martina, Li, Wenyan, Holdfeldt, André, Zhang, Liang, Björkman, Lena, Bylund, Johan, Dahlgren, Claes, Wang, Cai, Zhao, Xiaodong, and Forsman, Huamei

Subjects

PROGENITOR cells, BONE marrow, EOSINOPHILS, NEUTROPENIA, GRANULOCYTES

Abstract

Background: Neutrophils and eosinophils are multifunctional granulocytes derived from common myelocytic-committed progenitor cells. Severe congenital neutropenia 1 (SCN1) caused by ELANE mutations is a rare disease characterized by very low numbers of circulating neutrophils. Little is known about the functional characteristics of the SCN1 granulocytes, except that eosinophilia has been noticed in both bone marrow and peripheral blood. In this study, we profiled the number and function of granulocytes in patients suffering from SCN1.Methods: Nine patients diagnosed with SCN1 were enrolled in this study and absolute counts of eosinophils and neutrophils from bone marrow aspirates and peripheral blood samples were analysed. In addition, Ficoll-Paque enriched granulocytes from patients and healthy controls were analysed for specific eosinophil and neutrophil markers using flow cytometry and for NADPH-oxidase activity-profile by chemiluminescence.Results: Our data demonstrate a skewed granulocyte population in SCN1 patients dominated by eosinophils in both bone marrow and peripheral blood. The latter was detected only by blood smear examination, but not by automated blood analysers. Furthermore, we show that the SCN1 eosinophils exerted normal production of reactive oxygen species generated by the NADPH-oxidase, however the response was profoundly different from that of healthy control neutrophils.Conclusions: SCN1 patients with ELANE mutations suffer from neutropenia yet display eosinophilia in the bone marrow and blood, as revealed by smear examination but not by automatic blood analysers. The SCN1 eosinophils are functionally normal regarding production of reactive oxygen species (ROS). However, the ROS profile produced by eosinophils differs drastically from that of neutrophils isolated from the same blood donor, implying that the eosinophilia in SCN1 cannot compensate for the loss of neutrophils regarding ROS-mediated functions. [ABSTRACT FROM AUTHOR]

Published

2019

32. The Human Neutrophil Subsets Defined by the Presence or Absence of OLFM4 Both Transmigrate into Tissue In Vivo and Give Rise to Distinct NETs In Vitro.

Author

Welin, Amanda, Amirbeagi, Firoozeh, Christenson, Karin, Björkman, Lena, Björnsdottir, Halla, Forsman, Huamei, Dahlgren, Claes, Karlsson, Anna, and Bylund, Johan

Subjects

NEUTROPHILS, HETEROGENEITY, BIOMARKERS, OLFACTOMEDIN, CELL migration, APOPTOSIS, GHRELIN receptors, EXTRACELLULAR space

Abstract

Neutrophil heterogeneity was described decades ago, but it could not be elucidated at the time whether the existence of different neutrophil subsets had any biological relevance. It has been corroborated in recent years that neutrophil subsets, defined by differential expression of various markers, are indeed present in human blood, calling for renewed attention to this question. The expression of the granule protein olfactomedin 4 (OLFM4) has been suggested to define two such neutrophil subsets. We confirm the simultaneous presence of one OLFM4-positive and one OLFM4-negative neutrophil subpopulation as well as the localization of the protein to specific granules. In vitro, these neutrophil subsets displayed equal tendency to undergo apoptosis and phagocytose bacteria. In addition, the subpopulations were recruited equally to inflammatory sites in vivo, and this was true both in an experimental model of acute inflammation and in naturally occurring pathological joint inflammation. In line with its subcellular localization, only limited OLFM4 release was seen upon in vivo transmigration, and release through conventional degranulation required strong secretagogues. However, extracellular release of OLFM4 could be achieved upon formation of neutrophil extracellular traps (NETs) where it was detected only in a subset of the NETs. Although we were unable to demonstrate any functional differences between the OLFM4-defined subsets, our data show that different neutrophil subsets are present in inflamed tissue in vivo. Furthermore, we demonstrate NETs characterized by different markers for the first time, and our results open up for functions of OLFM4 itself in the extracellular space through exposure in NETs. [ABSTRACT FROM AUTHOR]

Published

2013

33. Reply.

Author

Forsman, Huamei, Islander, Ulrika, and Karlsson, Anna

Subjects

BREAST tumors, HEART failure, GENETICS of rheumatoid arthritis, THYROID gland tumors, GENETIC polymorphisms, GENETICS

Abstract

A response by Huamei Forsman and colleagues is presented to a letter to the editor about their article "Galectin 3 aggravates joint inflammation and destruction in antigen-induced arthritis" in the February 2011 issue.

Published

2011