Prolonged signalling and trafficking of the bradykinin B2 receptor stimulated with the amphibian peptide maximakinin: Insight into the endosomal inactivation of kinins

Bawolak, Marie‐Thérèse; Roy, Caroline; Gera, Lajos; Marceau, François

doi:10.1016/j.phrs.2011.11.004

Cited by 19 publications

(36 citation statements)

References 29 publications

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“…The recycling of B 2 R-GFP is conveniently assessed 3 h after stimulation with BK, a fragile peptide that is rapidly cleared by different pathways in both the serum-containing culture medium and in endosomes [5] (Fig. 6, top …”

Section: Effect Of Cytochalasin D On the Recycling Processmentioning

confidence: 99%

“…Thus, the B 2 R combines with either type of non-visual -arrestins and the ligand-B 2 R--arrestin complex gets translocated into endosomes [1,2]. The fusion protein B 2 Rgreen fluorescent protein (B 2 R-GFP) -arrestins conjugated to fluorescent proteins and BK sequences that were extended with fluorophores were instrumental in modeling the BK-induced endocytosis, but also its recycling to the cell surface and the persistence of the ternary agonistreceptor--arrestin complexes in intracellular structures [3][4][5] (and literature cited herein).…”

Section: Introductionmentioning

confidence: 99%

“…However, the BK-stimulated B 2 Rs are essentially completely recycled to the cell surface as a function of time, unless the agonist has an altered structure that confers resistance to proteolytic breakdown. In this case, the length of the B 2 R internalization and the duration of signaling are remarkably prolonged, and the secondary down-regulation of the receptors becomes prominent [2,5].…”

Section: Introductionmentioning

confidence: 99%

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Inhibitory effects of cytoskeleton disrupting drugs and GDP-locked Rab mutants on bradykinin B2 receptor cycling

Charest‐Morin

Fortin

Lodge

et al. 2013

Pharmacological Research

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The bradykinin (BK) B 2 receptor (B 2 R) is G protein coupled and phosphorylated upon agonist stimulation; its endocytosis and recycling are documented. We assessed the effect of drugs that affect the cytoskeleton on B 2 R cycling. These drugs were targeted to tubulin (paclitaxel, or the novel combretastatin A-4 mimetic 3,4,5-trimethoxyphenyl-4-(2-oxoimidazolidin-1-yl)benzenesulfonate Consistent with the displacement of cargo along specific cytoskeletal elements, Rab5-associated progression of the endocytosed BK B 2 R follows microtubules toward their (-)end, while its recycling progresses along actin fibers to the cell surface. However, tubulin ligands do not suppress the tested desensitization or resensitization mechanisms of the B 2 R.

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Section: Effect Of Cytochalasin D On the Recycling Processmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Inhibitory effects of cytoskeleton disrupting drugs and GDP-locked Rab mutants on bradykinin B2 receptor cycling

Charest‐Morin

Fortin

Lodge

et al. 2013

Pharmacological Research

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“…Of interest is that only the leucine residue substitution at position 8 of BK would cause such an astonishing function loss. Leucine 1 is a common substitution occurred in BRPs, compared with valine substation at position 1, it normally exhibits moderate agonistic effect of BK [26]. As the fact that Leu8-BK was reported as a BK receptor antagonist [27], we performed further experiments to examine whether RAP-L1, T6-BK and its analogue RAP-L1, T6, L8-BK could inhibit BK-induced relax on rat tail artery smooth muscle, the results revealed that, as expected, RAP-L1, T6-BK did not show BK inhibition property (Figure S1), but RAP-L1, T6, L8-BK significantly reduced BK relaxation activity on rat tail artery nearly 50% in the concentration range 10 −8 M–10 −5 M. These data suggested that although this novel BRP has a three residues -RAP- extension and leucine 1, threonine 6 substitutions, the leucine 8 still plays the essential and dominant role in reversing the BK’s effect.…”

Section: Discussionmentioning

confidence: 99%

Ex Vivo Smooth Muscle Pharmacological Effects of a Novel Bradykinin-Related Peptide, and Its Analogue, from Chinese Large Odorous Frog, Odorrana livida Skin Secretions

Xiang

Wang

et al. 2016

Toxins

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Bradykinin-related peptides (BRPs) are one of the most extensively studied frog secretions-derived peptide families identified from many amphibian species. The diverse primary structures of BRPs have been proven essential for providing valuable information in understanding basic mechanisms associated with drug modification. Here, we isolated, identified and characterized a dodeca-BRP (RAP-L1, T6-BK), with primary structure RAPLPPGFTPFR, from the skin secretions of Chinese large odorous frogs, Odorrana livida. This novel peptide exhibited a dose-dependent contractile property on rat bladder and rat ileum, and increased the contraction frequency on rat uterus ex vivo smooth muscle preparations; it also showed vasorelaxant activity on rat tail artery smooth muscle. In addition, the analogue RAP-L1, T6, L8-BK completely abolished these effects on selected rat smooth muscle tissues, whilst it showed inhibition effect on bradykinin-induced rat tail artery relaxation. By using canonical antagonist for bradykinin B1 or B2 type receptors, we found that RAP-L1, T6-BK -induced relaxation of the arterial smooth muscle was very likely to be modulated by B2 receptors. The analogue RAP-L1, T6, L8-BK further enhanced the bradykinin inhibitory activity only under the condition of co-administration with HOE140 on rat tail artery, suggesting a synergistic inhibition mechanism by which targeting B2 type receptors.

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“…Endosomal BK degradation obligatorily precedes the dissociation of β-arrestins from the B 2 R and receptor recycling to the cell surface, as shown by several inactivation-resistant B 2 R agonists that promote the persistence of this intracellular complex for at least 12 h and prolonged signaling [6,7]. Fluorophore conjugated analogs (carboxyfluorescein-or AlexaFluor-350-ε-aminocaproyl-BK) model the intracellular inactivation of the kinin, notably because the inhibitor of the proton pump V-ATPase, bafilomycin A1, prevents the time-dependent disappearance of the fluorescent peptides in endosomes of B 2 Rexpressing cells [8,9].…”

Section: Introductionmentioning

confidence: 99%

Vasopeptidase-activated latent ligands of the histamine receptor-1

Gera

Roy²,

Charest‐Morin³

et al. 2013

International Immunopharmacology

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Whether peptidases present in vascular cells can activate prodrugs active on vascular cells has been tested with 2 potential latent ligands of the histamine H 1 receptor (H 1 R). First, a peptide consisting of the antihistamine cetirizine (CTZ) condensed at the N-terminus of ε-aminocaproyl-bradykinin (εACA-BK) was evaluated for an antihistamine activity that could be revealed by degradation of the peptide part of the molecule. CTZ-εACA-BK had a submicromolar affinity for the BK B 2 receptor (B 2 R; IC 50 of 590 nM, [ The human umbilical vein contractility assay responded to L-alanyl-histamine (EC 50 54.7 µM), but the APN inhibitor amastatin massively (17-fold) reduced its apparent potency. Amastatin did not influence the potency of histamine as a contractile agent. One of the 2 tested latent H 1 R ligands, Lalanyl-histamine, supported the feasibility of pro-drug activation by vascular ectopeptidases.

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Prolonged signalling and trafficking of the bradykinin B2 receptor stimulated with the amphibian peptide maximakinin: Insight into the endosomal inactivation of kinins

Cited by 19 publications

References 29 publications

Inhibitory effects of cytoskeleton disrupting drugs and GDP-locked Rab mutants on bradykinin B2 receptor cycling

Inhibitory effects of cytoskeleton disrupting drugs and GDP-locked Rab mutants on bradykinin B2 receptor cycling

Ex Vivo Smooth Muscle Pharmacological Effects of a Novel Bradykinin-Related Peptide, and Its Analogue, from Chinese Large Odorous Frog, Odorrana livida Skin Secretions

Vasopeptidase-activated latent ligands of the histamine receptor-1

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