Development of original metabolically stable apelin‐17 analogs with diuretic and cardiovascular effects

Gerbier, Romain; Alvear-Perez, Rodrigo; Margathe, Jean-François; Flahault, Adrien; Couvineau, Pierre; Gao, Ji; Mota, Nadia De; Dabiré, Hubert; Li, Bo; Ceraudo, Emilie; Hus-Citharel, Annette; Esteoulle, Lucie; Bisoo, Cynthia; Hibert, Marcel; Berdeaux, Alain; Iturrioz, Xavier; Bron, Dominique; Llorens-Cortes, Catherine

doi:10.1096/fj.201600784r

Cited by 50 publications

(73 citation statements)

References 47 publications

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“…However, K17F is 30 times more potent in inducing rat ApelinR internalization when compared to pE13F (33). Deletion of the C-terminal Phe of K17F (K16P) or its substitution by an alanine (K17A) strongly decreases the ability of the peptide to trigger ApelinR internalization without effect on its affinity for the ApelinR or its ability to activate Gαi-coupling (18, 20).…”

Section: Metabolism Of Apelin Peptides and Pharmacological Characterimentioning

confidence: 99%

“…In addition, Gerbier et al (33) showed that K17F and pE13F have a half-life in mouse plasma of 4.6 and 7.2 min, respectively, and Murza et al (42) showed that pE13F has a 14 min half-life in rat plasma. Regarding apelin-36, Japp et al (43) suggested from experiments conducted in healthy human subjects that the half-life of apelin 36 is lower than 5 min.…”

Section: Development Of Metabolically Stable Apelin Analogsmentioning

confidence: 99%

“…Numerous technologies, such as PEGylation (44, 45), palmytoylation (46) conjugation to albumin, N-terminal acetylation (33), C-terminal amidation (47), use of unnatural amino acids (15, 33, 42, 48), or main chain modifications (cyclization) (49–51) have now been set up to increase the in vivo plasma half-life of peptides (52). Table 1 summarizes the pharmacological characteristics of the main metabolically stable apelin analogs described in this section.…”

Section: Development Of Metabolically Stable Apelin Analogsmentioning

confidence: 99%

“…Given these findings, metabolically stable K17F analogs were recently developed (15, 33). For this purpose, each amino acid of the sequence of K17F, which includes that of pE13F, was replaced with its D-isomer or with an unnatural amino acid.…”

Section: Development Of Metabolically Stable Apelin Analogsmentioning

confidence: 99%

“…P92 and LIT01-196 displayed full agonist activity for cAMP production, ERK1/2 phosphorylation (nanomolar range), induction of ApelinR internalization (subnanomolar range), and β-arrestin recruitment (33). …”

Section: Development Of Metabolically Stable Apelin Analogsmentioning

confidence: 99%

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Role of the Vasopressin/Apelin Balance and Potential Use of Metabolically Stable Apelin Analogs in Water Metabolism Disorders

et al. 2017

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Apelin, a (neuro)vasoactive peptide, plays a prominent role in controlling body fluid homeostasis and cardiovascular functions. In animal models, experimental data demonstrate that intracerebroventricular injection of apelin into lactating rats inhibits the phasic electrical activity of arginine vasopressin (AVP) neurons, reduces plasma AVP levels, and increases aqueous diuresis. In the kidney, apelin increases diuresis by increasing the renal microcirculation and by counteracting the antidiuretic effect of AVP at the tubular level. Moreover, after water deprivation or salt loading, in humans and in rodents, AVP and apelin are conversely regulated to facilitate systemic AVP release and to avoid additional water loss from the kidney. Furthermore, apelin and vasopressin secretion are significantly altered in various water metabolism disorders including hyponatremia and polyuria-polydipsia syndrome. Since the in vivo half-life of apelin is in the minute range, metabolically stable apelin analogs were developed. The efficacy of these lead compounds for decreasing AVP release and increasing both renal blood flow and diuresis, make them promising candidates for the treatment of water retention and/or hyponatremic disorders.

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Section: Metabolism Of Apelin Peptides and Pharmacological Characterimentioning

confidence: 99%

Section: Development Of Metabolically Stable Apelin Analogsmentioning

confidence: 99%

Section: Development Of Metabolically Stable Apelin Analogsmentioning

confidence: 99%

Section: Development Of Metabolically Stable Apelin Analogsmentioning

confidence: 99%

Section: Development Of Metabolically Stable Apelin Analogsmentioning

confidence: 99%

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Role of the Vasopressin/Apelin Balance and Potential Use of Metabolically Stable Apelin Analogs in Water Metabolism Disorders

et al. 2017

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Self‐organization Properties of a GPCR‐Binding Peptide with a Fluorinated Tail Studied by Fluorine NMR Spectroscopy

Muizon¹,

Ramanoudjame

Esteoulle

et al. 2020

ChemBioChem

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Conjugation of the bioactive apelin‐17 peptide with a fluorocarbon chain results in self‐organization of the peptide into micelles. Fluorine NMR spectroscopy studies show that the fluoropeptide‘s micelles are monodisperse, while proton NMR indicates that the peptide moiety remains largely disordered despite micellization. A very fast exchange rate is measured between the free and micellar states of the peptide which enables the number of molecules present in the micelle to be estimated as 200, in agreement with values found by dynamic light scattering measurements.

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Apelinergic System Structure and Function

Shin

Kenward

Rainey

2017

Comprehensive Physiology

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Apelin and apela (ELABELA/ELA/Toddler) are two peptide ligands for a class A G-protein-coupled receptor named the apelin receptor (AR/APJ/APLNR). Ligand-AR interactions have been implicated in regulation of the adipoinsular axis, cardiovascular system, and central nervous system alongside pathological processes. Each ligand may be processed into a variety of bioactive isoforms endogenously, with apelin ranging from 13 to 55 amino acids and apela from 11 to 32, typically being cleaved C-terminal to dibasic proprotein convertase cleavage sites. The C-terminal region of the respective precursor protein is retained and is responsible for receptor binding and subsequent activation. Interestingly, both apelin and apela exhibit isoform-dependent variability in potency and efficacy under various physiological and pathological conditions, but most studies focus on a single isoform. Biophysical behavior and structural properties of apelin and apela isoforms show strong correlations with functional studies, with key motifs now well determined for apelin. Unlike its ligands, the AR has been relatively difficult to characterize by biophysical techniques, with most characterization to date being focused on effects of mutagenesis. This situation may improve following a recently reported AR crystal structure, but there are still barriers to overcome in terms of comprehensive biophysical study. In this review, we summarize the three components of the apelinergic system in terms of structure-function correlation, with a particular focus on isoform-dependent properties, underlining the potential for regulation of the system through multiple endogenous ligands and isoforms, isoform-dependent pharmacological properties, and biological membrane-mediated receptor interaction. © 2018 American Physiological Society. Compr Physiol 8:407-450, 2018.

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Development of original metabolically stable apelin‐17 analogs with diuretic and cardiovascular effects

Cited by 50 publications

References 47 publications

Role of the Vasopressin/Apelin Balance and Potential Use of Metabolically Stable Apelin Analogs in Water Metabolism Disorders

Role of the Vasopressin/Apelin Balance and Potential Use of Metabolically Stable Apelin Analogs in Water Metabolism Disorders

Self‐organization Properties of a GPCR‐Binding Peptide with a Fluorinated Tail Studied by Fluorine NMR Spectroscopy

Apelinergic System Structure and Function

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