Your search keyword '"Björkman, Lena"' showing total 8 results

1. 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

2. 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

3. 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

4. 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

5. A simple skin blister technique for the study of in vivo transmigration of human leukocytes.

Author

Davidsson, Lisa, Björkman, Lena, Christenson, Karin, Alsterholm, Mikael, Movitz, Charlotta, Thorén, Fredrik B., Karlsson, Anna, Welin, Amanda, and Bylund, Johan

Subjects

*DERMIS, *LEUCOCYTES, *CELL migration, *BLOOD circulation, *INFLAMMATION, *OLFACTOMEDIN, *DISEASES

Abstract

Abstract: The study of human leukocytes is almost exclusively conducted using cells isolated from peripheral blood. This is especially true for neutrophils, despite the fact that these cells are of main (pathological) importance in extravascular tissues upon e.g., infection and/or tissue damage. The journey from circulation to tissue is typically associated with a number of cellular changes, making the cells primed, or hyper-responsive, and in many aspects distinct from the cells present in circulation. Models to obtain in vivo transmigrated leukocytes from human tissue are available, but not widely used. We describe here an easy-to-use model for the study of local inflammation, stemming from limited tissue damage, which can be used to isolate viable and functional leukocytes. The model is based on the generation of aseptic skin blisters, formed by the application of negative pressure, and allows for investigations of the cellular infiltrate as well as of soluble mediators present in the exudate. We believe that this method, combined with modern analysis equipment suitable for small volumes and cell numbers, could be of great use for increasing our understanding of the nature and function of leukocytes that have left circulation and transmigrated to inflamed tissues. [Copyright &y& Elsevier]

Published

2013

6. 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

Abstract

A nonactivating allosteric modulator of free fatty acid receptor 2 (FFA2R, also called GPCR 43) turns both propionate (an orthosteric FFA2R agonist) and ATP (an agonist for the purinergic P2Y2 receptor), into potent activating ligands that trigger an assembly of the superoxide-generating neutrophil NADPH oxidase. The ATP-induced activation requires the participation of FFA2R, and the signaling is biased toward oxidase activation, leaving the ATP-induced rise in intracellular Ca2+ unaffected. No NADPH oxidase activity was induced by ATP when propionate replaced the allosteric modulator. Signaling downstream of propionate-activated FFA2Rs was insensitive to Gαq inhibition, but the crosstalk activation involving both FFA2R and P2Y2R relied on Gαq signaling. The receptor crosstalk, by which allosterically modulated FFA2Rs communicate with P2Y2Rs and generate NADPH oxidase activating signals downstream of Gαq, represent a novel mechanism by which GPCR activities can be regulated from inside the plasma membrane. Further, the finding that an allosteric FFA2R modulator sensitizes not only the response induced by orthosteric FFA2R agonists, but also the response induced by ATP (P2Y2R-specific agonist) and formyl peptide receptor-specific agonists, violates the receptor restriction characteristics normally defining the selectivity of allosteric GPCR modulators. [ABSTRACT FROM AUTHOR]

Published

2019

7. A methodological approach to studies of desensitization of the formyl peptide receptor: Role of the read out system, reactive oxygen species and the specific agonist used to trigger neutrophils

Author

Karlsson, Jennie, Bylund, Johan, Movitz, Charlotta, Björkman, Lena, Forsman, Huamei, and Dahlgren, Claes

Subjects

*NEUTROPHILS, *PEPTIDES, *CELL receptors, *G proteins, *REACTIVE oxygen species, *ANNEXINS, *SERUM albumin, *PEROXIDASE

Abstract

Abstract: Neutrophil accumulation at an inflammatory site or an infected tissue is dependent on the recognition of chemotactic peptides that bind to G-protein coupled receptors (GPCRs) exposed on the surface of the inflammatory cells. A GPCR activated by a chemoattractant quickly becomes refractory to further stimulation by ligands using the same receptor. This desensitization phenomenon has been used frequently to characterize new receptor agonists and to determine receptor hierarchies. In this study we show that desensitization patterns differ depending on what read out systems are used to follow neutrophil activity. When monitoring release of superoxide, neutrophils were readily desensitized against repeated stimulations with the prototypical agonist formylmethionyl-leucyl-phenylalanine (fMLF). In contrast, neutrophils were not desensitized for fMLF when cell activity was determined by intracellular calcium ([Ca2+]i). The difference observed was dependent on inactivation of the agonist in one read out system but not in the other, and we suggest several different solutions to the problem. Agonist inactivation occurs through a myeloperoxidase (MPO)/hydrogen peroxide catalyzed reaction, and the problem could be avoided by using a FACS based technique to measure the change in [Ca2+]i, by the use of an agonist insensitive to the MPO/hydrogen peroxide-system or, by adding an MPO inhibitor or a scavenger that removes either superoxide/hydrogen peroxide or the MPO-derived metabolites. [Copyright &y& Elsevier]

Published

2010

8. Interdependent allosteric free fatty acid receptor 2 modulators synergistically induce functional selective activation and desensitization in neutrophils.

Author

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

Subjects

*FREE fatty acids, *RALOXIFENE, *CALCIUM ions, *ALLOSTERIC regulation, *G protein coupled receptors

Abstract

The non-activating allosteric modulator AZ1729, specific for free fatty acid receptor 2 (FFAR2), transfers the orthosteric FFAR2 agonists propionate and the P2Y 2 R specific agonist ATP into activating ligands that trigger an assembly of the neutrophil superoxide generating NADPH-oxidase. The homologous priming effect on the propionate response and the heterologous receptor cross-talk sensitized ATP response mediated by AZ1729 are functional characteristics shared with Cmp58, another non-activating allosteric FFAR2 modulator. In addition, AZ1729 also turned Cmp58 into a potent activator of the superoxide generating neutrophil NADPH-oxidase, and in agreement with the allosteric modulation concept, the effect was reciprocal in that Cmp58 turned AZ1729 into a potent activating allosteric agonist. The activation signals down-stream of FFAR2 when stimulated by the two interdependent allosteric modulators were biased in that, unlike for orthosteric agonists, the two complementary modulators together triggered an activation of the NADPH-oxidase, but not any transient rise in the cytosolic concentration of free calcium ions (Ca2+). Furthermore, following AZ1729/Cmp58 activation, the signaling by the desensitized FFAR2s was functionally selective in that the orthosteric agonist propionate could still induce a transient rise in intracellular Ca2+. The novel neutrophil activation and receptor down-stream signaling pattern mediated by the two cross-sensitizing allosteric FFAR2 modulators represent a new regulatory mechanism that controls receptor signaling. • The agonist occupied ATP receptor P2Y 2 R activates allosterically modulated FFAR2s. • Activation of FFAR2s by allosteric modulators without any orthosteric agonist • Biased receptor signaling induced by two interdependent allosteric modulators. • New regulatory mechanisms for control of GPCR-signaling [ABSTRACT FROM AUTHOR]

Published

2020