Formyl peptide receptor 2 as a potential therapeutic target for inflammatory bowel disease

Yang, Wen-sheng; Wang, Jinglin; Wu, Wei; Wang, Guang-fei; Yan, Jun; Liu, Qing; Wu, Xiaoyan; Zhou, Qingtong; Yang, Dehua; Wang, Mingwei; Li, Zhiping

doi:10.1038/s41401-022-00944-0

Cited by 4 publications

(6 citation statements)

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“…Operating through membrane receptors on the cell surface belonging to the FPR family, N-formyl peptides are a driver of migration and activators of different granulocyte functions among which ROS generation is one of the most important. Granulocytes regulated through various receptors are inducers of inflammation and participants of its completion or transition to the chronic stage in pathologies [ 8 , 40 , 41 , 42 , 43 ]. Based on the abovementioned, we assumed that in HFD-consuming ORM the ability of granulocytes to produce ROS in response to activation of FPRs is modified under basic conditions and with the development of acute inflammation.…”

Section: Resultsmentioning

confidence: 99%

“…The WKYMVM signal allowed us to distinguish acute inflammation in controls. This situation can be due to features of binding of peptides with FPRs, receptor expression, state (e.g., desensitization in ORM), or signaling [ 8 , 12 , 48 , 49 , 50 , 51 ]. Next, we analyzed FPR signaling to NADPH-oxidase with the participation of PLC, and PKC, as the main signaling components of these receptors, as well as MAPKs, which fine-tune the activity of the oxidase and participate in pathological processes.…”

Section: Resultsmentioning

confidence: 99%

“…Obese inflammatory conditions in different tissues are triggered and maintained by such epigenetics factors as dietary components (fatty acids including), hypoxia, danger/pathogen-associated molecular patterns (DAMP/PAMPs–LPS, C-type lectins, N-formyl peptides, structure fragments of pathogens, and DNA), and intestinal microbiota (alterations of which can lead to metabolic endotoxemia owing to raised plasma levels of LPS) [ 6 , 7 ]. The inflammatory state evinces increased serum concentrations of C-reactive protein, and is accompanied by an excessive level of proinflammatory cytokines (TNF-α, IL-1β, IL-6, IL-8) and decreased production of regulators with anti-inflammatory properties (IL-10, IL-4, TGF-β, prostaglandin E2, factors controlling Toll-like receptors, and NF-κB signaling) [ 2 , 8 ]. Epigenetic regulation of Toll-like receptors (TLRs–TLR2 and TLR4) via changes in the gut microbiota correlated significantly with body mass index [ 1 ].…”

Section: Introductionmentioning

confidence: 99%

“…Fpr1 and Fpr2, receptors with high- and low-affinity to fMLF, accordingly, are predominantly expressed in mouse neutrophils. Their roles in inflammation are different: FPR1 is considered to be the primary receptor for detection of N-formyl peptides, whereas FPR2 (69% homology to FPR1) can bind to a variety of ligands (formyl peptides, annexin A1, serum amyloid A, lipoxin A4, and others) [ 8 , 9 , 11 ]. FPR2 mediates both inflammatory and anti-inflammatory functions, suggesting ligand-dependent biased signaling; it is considered as a therapeutic target in inflammation, in particular for bowel disease [ 8 ].…”

Section: Introductionmentioning

confidence: 99%

“…Their roles in inflammation are different: FPR1 is considered to be the primary receptor for detection of N-formyl peptides, whereas FPR2 (69% homology to FPR1) can bind to a variety of ligands (formyl peptides, annexin A1, serum amyloid A, lipoxin A4, and others) [ 8 , 9 , 11 ]. FPR2 mediates both inflammatory and anti-inflammatory functions, suggesting ligand-dependent biased signaling; it is considered as a therapeutic target in inflammation, in particular for bowel disease [ 8 ]. Both receptors have been attributed a role in obesity: the FPR1 gene was downregulated in obese humans, and CYBB gene-coding NADPH-oxidase membrane subunit gp91phox was also downregulated in obese humans [ 12 ]; genetic or pharmacological inhibition of Fpr1 increased insulin levels and improved glucose tolerance, dependent upon glucagon-like peptide 1 [ 9 ]; the lack of ALX/FPR2 led to the development of spontaneous obesity, reduced life span, amplified leukocyte dysfunction, and facilitated profound interorgan non-resolving inflammation [ 13 ].…”

Section: Introductionmentioning

confidence: 99%

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Modified Signaling of Membrane Formyl Peptide Receptors in NADPH-Oxidase Regulation in Obesity-Resistant Mice

et al. 2023

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The signaling of membrane receptors is modified in obesity characterized by low-grade inflammation. The obesity-resistant state of organisms is poorly understood. We analyzed the generation of reactive oxygen species (ROS) initiated though membrane formyl peptide receptors (Fpr1, Fpr2) in bone-marrow granulocytes of obesity-resistant mice (ORM). A chemiluminescence assay was used to assess NADPH-oxidase-related intensity of ROS generation. ORM were chosen from animals that received high-fat diets and had metric body parameters as controls (standard diet). High spontaneous ROS production was observed in ORM cells. The EC50 for responses to bacterial or mitochondrial peptide N-formyl-MLF was higher in ORM with and without inflammation vs. the same control groups, indicating an insignificant role of high-affinity Fpr1. Increased responses to synthetic peptide WKYMVM (Fpr2 agonist) were observed in controls with acute inflammation, but they were similar in other groups. Fpr2 was possibly partially inactivated in ORM owing to the inflammatory state. Weakened Fpr1 and Fpr2 signaling via MAPKs was revealed in ORM using specific inhibitors for p38, ERK1/2, and JNK. P38 signaling via Fpr2 was lower in ORM with inflammation. Thus, a high-fat diet modified FPRs’ role and suppressed MAPK signaling in NADPH-oxidase regulation in ORM. This result can be useful to understand the immunological features of obesity resistance.

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