Serum amyloid A opposes lipoxin A<sub>4</sub>to mediate glucocorticoid refractory lung inflammation in chronic obstructive pulmonary disease

Bozinovski, Steven; Uddin, Mohib; Vlahos, Ross; Thompson, Michelle; McQualter, Jonathan L.; Merritt, Anne-Sophie; Wark, Peter; Hutchinson, Ana; Irving, Louis; Levy, Bruce D.; Anderson, Gary P.

doi:10.1073/pnas.1109382109

Cited by 142 publications

(224 citation statements)

References 34 publications

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“…The anti-inflammatory and proresolving actions of these novel peptides are in line with the actions displayed by the potent antiinflammatory and proresolving mediators LXA 4 and AT-LXA 4 that are both FPR2/ALX agonists (14,39). Notably, it has recently been demonstrated in that serum amyloid A, another FPR2/ALX may blunt the anti-inflammatory actions of LXA 4 , which, in turn, may mediate glucocorticoid refractory lung inflammation in patients with chronic obstructive pulmonary disease (39).…”

Section: Discussionmentioning

confidence: 61%

“…Notably, it has recently been demonstrated in that serum amyloid A, another FPR2/ALX may blunt the anti-inflammatory actions of LXA 4 , which, in turn, may mediate glucocorticoid refractory lung inflammation in patients with chronic obstructive pulmonary disease (39). These findings further underscore the complexity of ligand-receptor interactions mediated by FPR2/ALX that may lead to the activation of specific signaling pathways, ultimately resulting in functionally distinct cellular responses.…”

Section: Discussionmentioning

confidence: 81%

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Proresolving and Tissue-Protective Actions of Annexin A1–Based Cleavage-Resistant Peptides Are Mediated by Formyl Peptide Receptor 2/Lipoxin A4 Receptor

Dalli

Consalvo²,

Ray³

et al. 2013

The Journal of Immunology

109

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Endogenous mechanisms regulating the host response during inflammation resolution are critical in ensuring disposal of noxious stimuli and return to homeostasis. In this article, we engineered novel Annexin A1 (AnxA1)–based peptides, AnxA12–50, that displayed specific binding to the AnxA1 receptor (formyl peptide receptor 2/Lipoxin A4 receptor [FPR2/ALX]; IC50 ∼4 nM). Intravenous administration of AnxA12–50 markedly reduced (>60%) leukocyte adhesion to postcapillary venules in wild type and Fpr1−/−, but not Fpr2/Alx−/−, mice. Generation of a metabolically stable form of this peptide (CR-AnxA12–50), engineered by substituting a cleavage site shared by human proteinase 3 and neutrophil elastase, yielded an agonist that was resistant to neutrophil-mediated cleavage and displayed enhanced proresolving actions: accelerated resolution of self-limited inflammation and enhanced macrophage efferocytosis after sterile injury, when compared with AnxA12–50. These actions were retained with human primary leukocytes where CR-AnxA12–50 decreased neutrophil–endothelial interactions (∼25–45%), and stimulated neutrophil apoptosis and macrophage efferocytosis (∼45%). In murine cardiac ischemia/reperfusion injury, CR-AnxA12–50 elicited tissue-protective actions reducing infarct size (∼60%) and incidence of 24-h death. These results identify AnxA12–50 and CR-AnxA12–50 as FPR2/ALX agonists that harness the proresolving actions of AnxA1, and thus may represent therapeutic tools for treatment of inflammatory conditions.

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Section: Discussionmentioning

confidence: 61%

Section: Discussionmentioning

confidence: 81%

Proresolving and Tissue-Protective Actions of Annexin A1–Based Cleavage-Resistant Peptides Are Mediated by Formyl Peptide Receptor 2/Lipoxin A4 Receptor

Dalli

Consalvo²,

Ray³

et al. 2013

The Journal of Immunology

109

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“…It is noteworthy that, whereas LXA 4 did not affect the ALX conformational change promoted by AnxA1, SAA did reduce this response, thus providing a molecular explanation for the antagonistic properties of SAA and AnxA1 (25).…”

Section: Discussionmentioning

confidence: 98%

Ligand-specific conformational change of the G-protein–coupled receptor ALX/FPR2 determines proresolving functional responses

Cooray

Gobbetti

Montero‐Melendez

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

252

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Formyl-peptide receptor type 2 (FPR2), also called ALX (the lipoxin A4 receptor), conveys the proresolving properties of lipoxin A 4 and annexin A1 (AnxA1) and the proinflammatory signals elicited by serum amyloid protein A and cathelicidins, among others. We tested here the hypothesis that ALX might exist as homo-or heterodimer with FPR1 or FPR3 (the two other family members) and operate in a ligand-biased fashion. Coimmunoprecipitation and bioluminescence resonance energy transfer assays with transfected HEK293 cells revealed constitutive dimerization of the receptors; significantly, AnxA1, but not serum amyloid protein A, could activate ALX homodimers. A p38/MAPK-activated protein kinase/heat shock protein 27 signaling signature was unveiled after AnxA1 application, leading to generation of IL-10, as measured in vitro (in primary monocytes) and in vivo (after i.p. injection in the mouse). The latter response was absent in mice lacking the ALX ortholog. Using a similar approach, ALX/FPR1 heterodimerization evoked using the panagonist peptide Ac2-26, identified a JNK-mediated proapoptotic path that was confirmed in primary neutrophils. These findings provide a molecular mechanism that accounts for the dual nature of ALX and indicate that agonist binding and dimerization state contribute to the conformational landscape of FPRs.inflammation | leukocyte | resolution signaling G -protein-coupled receptors (GPCRs) constitute a large family of cell surface receptors that share structural characteristics and perform pivotal biological functions, transducing signals from hormones, autacoids, and chemokines. The human GPCR termed "ALX/FPR2" (formyl peptide receptor type 2 or lipoxin A 4 receptor, hereafter referred to as "ALX") is a unique GPCR, shown to convey signals induced by proteins, peptides, and lipid ligands (1). ALX belongs to a small family of receptors that is also activated by formylated peptides, short amino acid sequences with an N-terminal formyl group released by pathogenic and commensal bacteria, as well as by mitochondria upon cell damage. There are three human FPRs and they are termed FPR1, ALX, and FPR3 (2). In view of their different nature and potential engagement with a large number endogenous and exogenous ligands, elucidation of FPR functions may reveal important biological pathways.ALX is an unconventional receptor for the diversity of its agonists and because it can convey contrasting biological signals. The proresolving and anti-inflammatory properties of the protein annexin A1 (AnxA1) and the lipid lipoxin A 4 (LXA 4 ), which include neutrophil apoptosis and macrophage efferocytosis, are mediated by this receptor, as shown using pharmacological approaches (1, 3) and more recently with knockout mouse models (4). At the same time, the proinflammatory responses elicited by the cathelicidin-associated antimicrobial peptide LL-37 and serum amyloid protein A (SAA) are also mediated by ALX, which modulates leukocyte activation, recruitment to the site of inflammation, and lifespan (5-7). Moreover,...

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“…LXA 4 is a potent stimulus for macrophage phagocytosis (32). Additionally, LXA 4 inhibits neutrophil transepithelial migration (33) and airway epithelial proinflammatory mediator expression in an ALX/FPR2-dependent manner (33,34). LXA 4 also displays mucosal protection by stimulating ZO-1 expression and transepithelial electrical resistance in human airway epithelial cells (35).…”

Section: Discussionmentioning

confidence: 99%

Human Mesenchymal Stem (Stromal) Cells Promote the Resolution of Acute Lung Injury in Part through Lipoxin A4

Fang

Abbott

Cheng

et al. 2015

The Journal of Immunology

Self Cite

137

123

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Previous studies demonstrated that bone marrow–derived mesenchymal stem (stromal) cells (MSCs) reduce the severity of acute lung injury in animal models and in an ex vivo perfused human lung model. However, the mechanisms by which MSCs reduce lung injury are not well understood. In the present study, we tested the hypothesis that human MSCs promote the resolution of acute lung injury in part through the effects of a specialized proresolving mediator lipoxin A4 (LXA4). Human alveolar epithelial type II cells and MSCs expressed biosynthetic enzymes and receptors for LXA4. Coculture of human MSCs with alveolar epithelial type II cells in the presence of cytomix significantly increased the production of LXA4 by 117%. The adoptive transfer of MSCs after the onset of LPS-induced acute lung injury (ALI) in mice led to improved survival (48 h), and blocking the LXA4 receptor with WRW4, a LXA4 receptor antagonist, significantly reversed the protective effect of MSCs on both survival and the accumulation of pulmonary edema. LXA4 alone improved survival in mice, and it also significantly decreased the production of TNF-α and MIP-2 in bronchoalveolar lavage fluid. In summary, these experiments demonstrated two novel findings: human MSCs promote the resolution of lung injury in mice in part through the proresolving lipid mediator LXA4, and LXA4 itself should be considered as a therapeutic for acute respiratory distress syndrome.

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Serum amyloid A opposes lipoxin A₄to mediate glucocorticoid refractory lung inflammation in chronic obstructive pulmonary disease

Cited by 142 publications

References 34 publications

Proresolving and Tissue-Protective Actions of Annexin A1–Based Cleavage-Resistant Peptides Are Mediated by Formyl Peptide Receptor 2/Lipoxin A4 Receptor

Proresolving and Tissue-Protective Actions of Annexin A1–Based Cleavage-Resistant Peptides Are Mediated by Formyl Peptide Receptor 2/Lipoxin A4 Receptor

Ligand-specific conformational change of the G-protein–coupled receptor ALX/FPR2 determines proresolving functional responses

Human Mesenchymal Stem (Stromal) Cells Promote the Resolution of Acute Lung Injury in Part through Lipoxin A4

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Serum amyloid A opposes lipoxin A4to mediate glucocorticoid refractory lung inflammation in chronic obstructive pulmonary disease

Cited by 142 publications

References 34 publications

Proresolving and Tissue-Protective Actions of Annexin A1–Based Cleavage-Resistant Peptides Are Mediated by Formyl Peptide Receptor 2/Lipoxin A4 Receptor

Proresolving and Tissue-Protective Actions of Annexin A1–Based Cleavage-Resistant Peptides Are Mediated by Formyl Peptide Receptor 2/Lipoxin A4 Receptor

Ligand-specific conformational change of the G-protein–coupled receptor ALX/FPR2 determines proresolving functional responses

Human Mesenchymal Stem (Stromal) Cells Promote the Resolution of Acute Lung Injury in Part through Lipoxin A4

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Serum amyloid A opposes lipoxin A₄to mediate glucocorticoid refractory lung inflammation in chronic obstructive pulmonary disease