Glucose homeostasis is impaired in mice deficient in the neuropeptide 26RFa (QRFP)

El-Mehdi, Mouna; Takhlidjt, Saloua; Khiar, Fayrouz; Prévost, Gaëtan; Rego, Jean-Luc do; Rego, Jean–Claude do; Bénani, Alexandre; Nédélec, Emmanuelle; Godefroy, David; Arabo, Arnaud; Lefranc, Benjamin; Leprince, Jérôme; Anouar, Youssef; Chartrel, Nicolas; Picot, Marie Christine

doi:10.1136/bmjdrc-2019-000942

Cited by 15 publications

(17 citation statements)

References 31 publications

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“…Primeaux ( Takayasu et al, 2006 ) has shown that, after 3 weeks on a high-fat (55%) diet, consumption increased the concentration of preproQRFP mRNA in the VHM/ARC, but not in the LHA. In contrast, Beck et al ( El-Mehdi et al, 2020 ) have shown that the expression of 26RFa/QRFP was undetectable in Long-Evans rats fed on a high-fat diet, yet in the control group (30% fat) the expression was lower than in the low-fat (5%) diet group. Nevertheless, the application of a caloric restriction diet for 10 weeks in B6 mice resulted in no changes in the expression of 26RFa and GPR103 ( Méquinion et al, 2017 ).…”

Section: Neuropeptide 26rfamentioning

confidence: 89%

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New Peptides as Potential Players in the Crosstalk Between the Brain and Obesity, Metabolic and Cardiovascular Diseases

2021

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According to the World Health Organization report published in 2016, 650 million people worldwide suffer from obesity, almost three times more than in 1975. Obesity is defined as excessive fat accumulation which may impair health with non-communicable diseases such as diabetes, cardiovascular diseases (hypertension, coronary artery disease, stroke), and some cancers. Despite medical advances, cardiovascular complications are still the leading causes of death arising from obesity. Excessive fat accumulation is caused by the imbalance between energy intake and expenditure. The pathogenesis of this process is complex and not fully understood, but current research is focused on the role of the complex crosstalk between the central nervous system (CNS), neuroendocrine and immune system including the autonomic nervous system, adipose tissue, digestive and cardiovascular systems. Additionally, special attention has been paid to newly discovered substances: neuropeptide 26RFa, preptin, and adropin. It was shown that the above peptides are synthesized both in numerous structures of the CNS and in many peripheral organs and tissues, such as the heart, adipose tissue, and the gastrointestinal tract. Recently, particular attention has been paid to the role of the presented peptides in the pathogenesis of obesity, metabolic and cardiovascular system diseases. This review summarizes the role of newly investigated peptides in the crosstalk between brain and peripheral organs in the pathogenesis of obesity, metabolic, and cardiovascular diseases.

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Section: Neuropeptide 26rfamentioning

confidence: 89%

“…Recently, the QRFP system is a popular target for research on metabolic homeostasis, glucose and lipid metabolism, pancreas function, and obesity ( Mulumba et al, 2010 , 2015 ; Méquinion et al, 2017 ; Prévost et al, 2019a , b ; El-Mehdi et al, 2020 ).…”

Section: Neuropeptide 26rfamentioning

confidence: 99%

New Peptides as Potential Players in the Crosstalk Between the Brain and Obesity, Metabolic and Cardiovascular Diseases

2021

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“…The QRFPR gene (also known as GPR103 gene) encodes a G-protein-coupled receptor that is expressed in brain, urinary bladder, thyroid gland, human pancreatic β-cells, and so on. 21 Recent data indicate that QRFPR and its ligand QRFP are key regulators of glucose homeostasis 22 by increasing insulin sensitivity and insulin secretion, 23 , 24 as well as preventing pancreatic β-cells death and apoptosis. 25 Besides, a locus on chromosome 4q27 that is approximately 625kb downstream the QRFPR gene was reported to be associated with a number of autoimmune diseases.…”

Section: Discussionmentioning

confidence: 99%

Associations of GWAS-Supported Non-MHC Genes with Autoimmune Thyroiditis in Patients with Type 1 Diabetes

Liang

et al. 2021

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Purpose A genome-wide association study (GWAS) in Caucasian population identified five non-MHC genes ( PHTF1, PTPN22, MAGI3, BCL2L15 , and QRFPR ) associated with risk of the co-occurrence of autoimmune thyroid diseases (AITD) and type 1 diabetes (T1D). The aim of this study is to replicate these associations with AITD in patients with T1D in Chinese Han population. Patients and Methods A case–control study was designed. Five single-nucleotide polymorphisms (SNPs) PHTF1 rs1111695, PTPN22 rs1217407, MAGI3 rs2153977, BCL2L15 rs2358994, and QRFPR rs7679475 were genotyped in 489 patients with T1D. Associations between genotypes and AITD risk were analyzed with logistic regression model. Results AITD occurred in 159 (32.5%) patients. When adjusting multiple factors by logistic regression, QRFPR rs7679475 was significantly associated with an increased risk of AITD in T1D patients in codominant model (G/G vs A/A, OR 2.93; 95% CI 1.44–5.96; P = 0.003), dominant model (G/A-G/G vs A/A, OR 1.81; 95% CI 1.17–2.79; P = 0.007) and recessive model (G/G vs A/A-G/A, OR 2.28; 95% CI 1.17–4.43; P = 0.015). Furthermore, we found a significant interaction between rs7679475 and female ( P interaction = 0.005). In silico analysis indicated that rs7679475 is located in histone modification marked region and can change the binding of regulatory motifs. Conclusion Our results suggested that QRFPR rs7679475 may influence the risk of AITD in patients with T1D in Chinese Han population, and this effect may be modulated by sex.

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“…N-methylation of Phe 22 (LV-2066, 25) and Phe 26 (LV-2242, 27) nullified the activity of the parent compound (EC 50 > 10 µM, Table 2) revealing the critical role of the corresponding NHs in forming an H-bond with the hQRFPR pocket residues or another residue of the peptide, whereas N-methylation of Phe 24 (LV-2233, 26) did not impair the whole activity of LV-2021 (1). The corresponding Tic-containing analogs (28)(29)(30) did not totally confirm these data since [Tic 24 ]26RFa (20)(21)(22)(23)(24)(25)(26) (20)(21)(22)(23)(24)(25)(26) (LV-2211, 28) was 5-fold more potent than 26RFa (20)(21)(22)(23)(24)(25)(26) (LV-2021, 1) (Figure 3D). It is thus also plausible that the structural constraint induced by the Tic 22 residue may keep the side chain in a favorable conformation for receptor activation, which was less accessible by free rotation in the native Phe side chain.…”

Section: Impact Of Modifications Of Each Phenylalanine Residuementioning

confidence: 98%

“…There is also evidence that 26RFa and/or QRFP regulate several other neuroendocrine and cognitive functions including reproduction [ 17 , 18 ], anxiety [ 19 ], memory [ 20 ], cardiovascular activity [ 8 ] and nociceptive transmission [ 21 , 22 , 23 ], some of which depend, at least in part, on off-target interaction with QRFPR-related receptors [ 24 , 25 ]. In addition, recent data reveal that the 26RFa/QRFPR system controls glucose homeostasis at the periphery by increasing insulin sensitivity and inhibiting hepatic glucose production [ 26 , 27 , 28 , 29 ]. Thus, QRFPR positions as an attractive target for the development of innovative drugs.…”

Section: Introductionmentioning

confidence: 99%

Point-Substitution of Phenylalanine Residues of 26RFa Neuropeptide: A Structure-Activity Relationship Study

et al. 2021

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26RFa is a neuropeptide that activates the rhodopsin-like G protein-coupled receptor QRFPR/GPR103. This peptidergic system is involved in the regulation of a wide array of physiological processes including feeding behavior and glucose homeostasis. Herein, the pharmacological profile of a homogenous library of QRFPR-targeting peptide derivatives was investigated in vitro on human QRFPR-transfected cells with the aim to provide possible insights into the structural determinants of the Phe residues to govern receptor activation. Our work advocates to include in next generations of 26RFa(20–26)-based QRFPR agonists effective substitutions for each Phe unit, i.e., replacement of the Phe22 residue by a constrained 1,2,3,4-tetrahydroisoquinoline-3-carboxylic acid moiety, and substitution of both Phe24 and Phe26 by their para-chloro counterpart. Taken as a whole, this study emphasizes that optimized modifications in the C-terminal part of 26RFa are mandatory to design selective and potent peptide agonists for human QRFPR.

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Glucose homeostasis is impaired in mice deficient in the neuropeptide 26RFa (QRFP)

Cited by 15 publications

References 31 publications

New Peptides as Potential Players in the Crosstalk Between the Brain and Obesity, Metabolic and Cardiovascular Diseases

New Peptides as Potential Players in the Crosstalk Between the Brain and Obesity, Metabolic and Cardiovascular Diseases

Associations of GWAS-Supported Non-MHC Genes with Autoimmune Thyroiditis in Patients with Type 1 Diabetes

Point-Substitution of Phenylalanine Residues of 26RFa Neuropeptide: A Structure-Activity Relationship Study

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