Identification of Peptides That Antagonize Formyl Peptide Receptor-Like 1-Mediated Signaling

et al. 2009

Exp Mol Med

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In this study, we observed that lysophosphatidylglycerol (LPG) completely inhibited a formyl peptide receptor like-1 (FPRL1) agonist (MMK-1)-stimulated chemotactic migration in human phagocytes, such as neutrophils and monocytes. LPG also dramatically inhibited IL-1β production by another FPRL1 agonist serum amyloid A (SAA) in human phagocytes. However, LPG itself induced intracellular calcium increase and superoxide anion production in human phagocytes. Keeping in mind that phagocytes migration and IL-1β production by FPRL1 are important for the induction of inflammatory response, our data suggest that LPG can be regarded as a useful material for the modulation of inflammatory response induced by FPRL1 activation.

Section: Discussionmentioning

confidence: 99%

Lysophosphatidylglycerol inhibits formyl peptide receptor like-1-stimulated chemotactic migration and IL-1β production from human phagocytes

Shim

et al. 2009

Exp Mol Med

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“…However, some GPCR groups do codesensitize via single receptor activation for reasons, like receptor oligomerization, sequestration, and others (20). To solve this problem, we used the antagonizing peptide, WRW4, which does not activate but does bind FPRL1 (16). Desensitization events between two GPCRs usually occur via agonist-induced receptor activation (20).…”

Section: Discussionmentioning

confidence: 99%

“…Ligand-binding analysis was performed as previously described (16). Briefly, FPRL1/RBL cells were seeded at 1 ϫ 10 5 cells/well onto a 24-well plate and cultured overnight.…”

Section: Ligand-binding Analysismentioning

confidence: 99%

Pituitary Adenylate Cyclase-Activating Polypeptide 27 Is a Functional Ligand for Formyl Peptide Receptor-Like 1

Lee

The Journal of Immunology

et al. 2006

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Although the neuropeptide pituitary adenylate cyclase-activating polypeptide (PACAP) has been implicated in the regulation of several immune responses, its target receptors and signaling mechanisms have yet to be fully elucidated in immune cells. In this study, we found that PACAP27, but not PACAP38, specifically stimulated intracellular calcium mobilization and ERK phosphorylation in human neutrophils. Moreover, formyl peptide receptor-like 1 (FPRL1) was identified as a PACAP27 receptor, and PACAP27 was found to selectively stimulate intracellular calcium increase in FPRL1-transfected rat basophile leukocytes-2H3 cell lines. In addition, PACAP27-induced calcium increase and ERK phosphorylation were specifically inhibited by an FPRL1 antagonist, Trp-Arg-Trp-Trp-Trp-Trp (WRW4), thus supporting the notion that PACAP27 acts on FPRL1. In terms of the functional role of PACAP27, we found that the peptide stimulated CD11b surface up-regulation and neutrophil chemotactic migration, and that these responses were completely inhibited by WRW4. The interaction between PACAP27 and FPRL1 was analyzed further using truncated PACAPs and chimeric PACAPs using vasoactive intestinal peptide, and the C-terminal region of PACAP27 was found to perform a vital function in the activation of FPRL1. Taken together, our study suggests that PACAP27 activates phagocytes via FPRL1 activation, and that this results in proinflammatory behavior, involving chemotaxis and the up-regulation of CD11b.

“…FPRL1 Since F2L has been reported to induce the chemotactic migration of mouse neutrophils via FPR2 (mouse counterpart of human FPRL1) [15], we tested whether F2L stimulates the chemotactic migration of HUVECs via FPRL1, with the aid of an FPRL1-selective antagonist (WRW 4 ) [18]. The F2L-induced HUVEC chemotaxis was completely inhibited by WRW 4 (Fig.…”

Section: F2l-induced Huvec Chemotactic Migration Is Mediated Bymentioning

confidence: 99%

F2L, a peptide derived from heme‐binding protein, inhibits LL‐37‐induced cell proliferation and tube formation in human umbilical vein endothelial cells

Lee

et al. 2007

FEBS Letters

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F2L, a peptide derived from heme-binding protein, was originally identified as an endogenous ligand for formyl peptide receptor-like (FPRL)2. Previously, we reported that F2L inhibits FPR and FPRL1-mediated signaling in neutrophils. Since endothelial cells express functional FPRL1, we examined the effect of F2L on LL-37 (an FPRL1 agonist)-induced signaling in human umbilical vein endothelial cells (HUVECs). F2L stimulated the chemotactic migration in HUVECs. However, F2L inhibited FPRL1 activity, resulting in the inhibition of cell proliferation and tube formation induced by LL-37 in HUVECs. We suggest that F2L will potentially be useful in the study of FPRL1 signaling and the development of drugs to treat diseases involving the FPRL1 in the vascular system.