MOLECULAR-CLONING AND CHARACTERIZATION OF NESP55, A NOVEL CHROMOGRANIN-LIKE PRECURSOR OF A PEPTIDE WITH 5-HT1B RECEPTOR ANTAGONIST ACTIVITY

Authors
ISCHIA R LOVISETTISCAMIHORN P HOGUEANGELETTI R WOLKERSDORFER M WINKLER H FISCHERCOLBRIE R
Citation
R. Ischia et al., MOLECULAR-CLONING AND CHARACTERIZATION OF NESP55, A NOVEL CHROMOGRANIN-LIKE PRECURSOR OF A PEPTIDE WITH 5-HT1B RECEPTOR ANTAGONIST ACTIVITY, The Journal of biological chemistry, 272(17), 1997, pp. 11657-11662
Citations number
30
Categorie Soggetti
Biology
Journal title
The Journal of biological chemistryACNP
ISSN journal
00219258
Volume
272
Issue
17
Year of publication
1997
Pages
11657 - 11662
Database
ISI
SICI code
0021-9258(1997)272:17<11657:MACONA>2.0.ZU;2-V
Abstract
The chromogranins comprise a class of acidic proteins that are secrete d from large dense core vesicles and expressed in neuronal and endocri ne tissues, We describe here the molecular characterization of NESP55 (neuroendocrine secretory protein of M-r 55,000), a novel member of th e chromogranins, Several NESP55 cDNA clones were isolated from bovine chromaffin cell libraries, The cDNA sequence of NESP55 totals 1499 nuc leotides, All of the clones that were isolated contained in their 3'-u ntranslated'mRNA a sequence that was homologous to exon 2 of the G-pro tein G(s) alpha. The open reading frame encodes for an acidic and hydr ophilic protein of 241 amino acids with a predicted molecular mass of 27,494 Da, An antiserum directed against the C terminus of NESP55 labe led a band of M-r 55,000 with an acidic pI ranging from 4.4 to 5.2 in one- and two dimensional immunoblots of secretory proteins from chroma ffin granules, NESP55 is localized within the cell to the large dense secretory vesicles and is expressed, apart from the adrenal medulla, i n the anterior and posterior pituitary and various regions of the brai n, For the physiological function, one interesting factor has emerged, NESP55 is proteolytically processed within the chromaffin granule to smaller peptides that might be physiologically active, One tetrapeptid e, Leu-Ser-Ala-Leu (LSAL), present in the NESP55 sequence and flanked by arginine residues suitable for cleavage by prohormone convertases, has been identified recently as an endogenous antagonist of the seroto nergic 5-HT1B receptor subtype, Alterations in the serotonergic system are thought to play an important role in mental disorders, especially depression, and might be related to abnormal ethanol consumption, It is tempting to speculate that increased expression of NESP55 or its pr oteolytically derived peptide LSAL might contribute to the pathophysio logy of the serotonergic transmission.