Serveur d'exploration sur les relations entre la France et l'Australie

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Cardiac synthesis, processing, and coronary release of enkephalin-related peptides

Identifieur interne : 00C342 ( Main/Exploration ); précédent : 00C341; suivant : 00C343

Cardiac synthesis, processing, and coronary release of enkephalin-related peptides

Auteurs : Antoine Younes [France] ; Salvatore Pepe [Australie] ; Barbara A. Barron [États-Unis] ; Harold A. Spurgeon [États-Unis] ; Edward G. Lakatta [États-Unis] ; James L. Caffrey [États-Unis]

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RBID : Pascal:01-0003244

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English descriptors

Abstract

Although preproenkephalin mRNA is abundant in the heart, the myocardial synthesis and processing of proenkephalin is largely undefined. Isolated working rat hearts were perfused to determine the rate of myocardial proenkephalin synthesis, its processing into enkephalin-containing peptides, their subsequent release into the coronary arteries, and the influence of prior sympathectomy. Enkephalin-containing peptides were separated by gel filtration and quantified with antisera for specific COOH-terminal sequences. Proenkephalin, peptide B, and [Met5]enkephalin-Arg6-Phe7 (MEAP) comprised 95% of the extracted myocardial enkephalins (35 pmol/g). Newly synthesized enkephalins, estimated during a 1-h perfusion with [14C]phenylalanine (4 pmol.h-1.g wet wt-1), were rapidly cleared from the heart during a second isotope-free hour. Despite a steady release of enkephalins into the coronary effluent (4 pmol.h-1.g wet wt-1), enkephalin replacement apparently exceeded its release, and tissue enkephalins actually accumulated during hour 2. In contrast to the tissue, methionine-enkephalin accounted for more than half of the released enkephalin. Chemical sympathectomy produced an increase in total enkephalin content similar to that observed after 2-h control perfusion. This observation suggested that the normal turnover of myocardial enkephalin may depend in part on continued sympathetic influences.


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Le document en format XML

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<title xml:lang="en" level="a">Cardiac synthesis, processing, and coronary release of enkephalin-related peptides</title>
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<keywords scheme="KwdEn" xml:lang="en">
<term>Animal</term>
<term>Biosynthesis</term>
<term>Coronary artery</term>
<term>Heart</term>
<term>Metabolism</term>
<term>Opioid peptide</term>
<term>Proenkephalin</term>
<term>Rat</term>
<term>Release</term>
<term>Sympathectomy</term>
<term>Sympathetic nervous system</term>
<term>Turnover</term>
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<term>Biosynthèse</term>
<term>Métabolisme</term>
<term>Proenképhaline</term>
<term>Coeur</term>
<term>Libération</term>
<term>Artère coronaire</term>
<term>Peptide opioïde</term>
<term>Turnover</term>
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<div type="abstract" xml:lang="en">Although preproenkephalin mRNA is abundant in the heart, the myocardial synthesis and processing of proenkephalin is largely undefined. Isolated working rat hearts were perfused to determine the rate of myocardial proenkephalin synthesis, its processing into enkephalin-containing peptides, their subsequent release into the coronary arteries, and the influence of prior sympathectomy. Enkephalin-containing peptides were separated by gel filtration and quantified with antisera for specific COOH-terminal sequences. Proenkephalin, peptide B, and [Met
<sup>5</sup>
]enkephalin-Arg
<sup>6</sup>
-Phe
<sup>7</sup>
(MEAP) comprised 95% of the extracted myocardial enkephalins (35 pmol/g). Newly synthesized enkephalins, estimated during a 1-h perfusion with [
<sup>14</sup>
C]phenylalanine (4 pmol.h
<sup>-1</sup>
.g wet wt
<sup>-1</sup>
), were rapidly cleared from the heart during a second isotope-free hour. Despite a steady release of enkephalins into the coronary effluent (4 pmol.h
<sup>-1</sup>
.g wet wt
<sup>-1</sup>
), enkephalin replacement apparently exceeded its release, and tissue enkephalins actually accumulated during hour 2. In contrast to the tissue, methionine-enkephalin accounted for more than half of the released enkephalin. Chemical sympathectomy produced an increase in total enkephalin content similar to that observed after 2-h control perfusion. This observation suggested that the normal turnover of myocardial enkephalin may depend in part on continued sympathetic influences.</div>
</front>
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<name sortKey="Younes, Antoine" sort="Younes, Antoine" uniqKey="Younes A" first="Antoine" last="Younes">Antoine Younes</name>
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<name sortKey="Pepe, Salvatore" sort="Pepe, Salvatore" uniqKey="Pepe S" first="Salvatore" last="Pepe">Salvatore Pepe</name>
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<name sortKey="Lakatta, Edward G" sort="Lakatta, Edward G" uniqKey="Lakatta E" first="Edward G." last="Lakatta">Edward G. Lakatta</name>
<name sortKey="Spurgeon, Harold A" sort="Spurgeon, Harold A" uniqKey="Spurgeon H" first="Harold A." last="Spurgeon">Harold A. Spurgeon</name>
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