Literature DB >> 20015090

Isolation and pharmacological characterization of AdTx1, a natural peptide displaying specific insurmountable antagonism of the alpha1A-adrenoceptor.

L Quinton1, E Girard, A Maiga, M Rekik, P Lluel, G Masuyer, M Larregola, C Marquer, J Ciolek, T Magnin, R Wagner, J Molgó, R Thai, C Fruchart-Gaillard, G Mourier, J Chamot-Rooke, A Ménez, S Palea, D Servent, N Gilles.   

Abstract

BACKGROUND AND
PURPOSE: Venoms are a rich source of ligands for ion channels, but very little is known about their capacity to modulate G-protein coupled receptor (GPCR) activity. We developed a strategy to identify novel toxins targeting GPCRs. EXPERIMENTAL APPROACH: We studied the interactions of mamba venom fractions with alpha(1)-adrenoceptors in binding experiments with (3)H-prazosin. The active peptide (AdTx1) was sequenced by Edman degradation and mass spectrometry fragmentation. Its synthetic homologue was pharmacologically characterized by binding experiments using cloned receptors and by functional experiments on rabbit isolated prostatic smooth muscle. KEY
RESULTS: AdTx1, a 65 amino-acid peptide stabilized by four disulphide bridges, belongs to the three-finger-fold peptide family. It has subnanomolar affinity (K(i)= 0.35 nM) and high specificity for the human alpha(1A)-adrenoceptor subtype. We showed high selectivity and affinity (K(d)= 0.6 nM) of radio-labelled AdTx1 in direct binding experiments and revealed a slow association constant (k(on)= 6 x 10(6).M(-1).min(-1)) with an unusually stable alpha(1A)-adrenoceptor/AdTx1 complex (t(1/2diss)= 3.6 h). AdTx1 displayed potent insurmountable antagonism of phenylephrine's actions in vitro (rabbit isolated prostatic muscle) at concentrations of 10 to 100 nM. CONCLUSIONS AND IMPLICATIONS: AdTx1 is the most specific and selective peptide inhibitor for the alpha(1A)-adrenoceptor identified to date. It displays insurmountable antagonism, acting as a potent relaxant of smooth muscle. Its peptidic nature can be exploited to develop new tools, as a radio-labelled-AdTx1 or a fluoro-labelled-AdTx1. Identification of AdTx1 thus offers new perspectives for developing new drugs for treating benign prostatic hyperplasia.

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Year:  2009        PMID: 20015090      PMCID: PMC2825353          DOI: 10.1111/j.1476-5381.2009.00532.x

Source DB:  PubMed          Journal:  Br J Pharmacol        ISSN: 0007-1188            Impact factor:   8.739


  49 in total

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4.  Pharmacological evidence that different alpha 1 adrenoceptor subtypes mediate contraction in rabbit prostate and hypogastric artery.

Authors:  S Delaflotte; M Auguet; P E Chabrier
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5.  Three distinct binding sites for [3H]-prazosin in the rat cerebral cortex.

Authors:  M Oshita; S Kigoshi; I Muramatsu
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6.  Identification of alpha 1-adrenoceptor subtypes in the rabbit prostate.

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4.  Adrenoceptor activity of muscarinic toxins identified from mamba venoms.

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7.  Effects of ρ-Da1a a peptidic α(1) (A) -adrenoceptor antagonist in human isolated prostatic adenoma and anaesthetized rats.

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8.  Crystallization of recombinant green mamba ρ-Da1a toxin during a lyophilization procedure and its structure determination.

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Review 9.  Nature-Derived Peptides: A Growing Niche for GPCR Ligand Discovery.

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10.  Identification and structural characterization of a new three-finger toxin hemachatoxin from Hemachatus haemachatus venom.

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