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The N- and C-terminal fragments of ubiquitin are important for the antimicrobial activities.

作者信息

Kieffer Anne-Estelle, Goumon Yannick, Ruh Olivier, Chasserot-Golaz Sylvette, Nullans Gérard, Gasnier Claire, Aunis Dominique, Metz-Boutigue Marie-Héléne

机构信息

INSERM Unité 575, IFR 37, Physiopathologie du Système Nerveux, Strasbourg, France.

出版信息

FASEB J. 2003 Apr;17(6):776-8. doi: 10.1096/fj.02-0699fje. Epub 2003 Feb 19.

DOI:10.1096/fj.02-0699fje
PMID:12594174
Abstract

Secretory granules of chromaffin cells contain catecholamines and several antimicrobial peptides derived from chromogranins and proenkephalin-A. These peptides are secreted in the extracellular medium following exocytosis. Here, we show that ubiquitin is stored in secretory chromaffin granules and released into the circulation upon stimulation of chromaffin cells. We also show that the C-terminal fragment (residues 65-76) of ubiquitin displays, at the micromolar range, a lytic antifungal activity. Using confocal laser scan microscopy and rhodamine-labeled synthetic peptides, we could demonstrate that the C-terminal peptide (residues 65-76) is able to cross the cell wall and the plasma membrane of fungi and to accumulate in fungi, whereas the N-terminal peptide (residues 1-34) is stopped at the fungal wall level. Furthermore, these two peptides act synergistically to kill filamentous fungi. Because of the interaction of the C-terminal sequence of ubiquitin with calmodulin, the synthetic peptide (residues 65-76) was tested in vitro against calmodulin-dependent calcineurin, an enzyme crucial for fungal growth. This peptide was found to inhibit the phosphatase activity of calcineurin. Our data show a new property of ubiquitin C-terminal-derived peptide (65-76) that could be used with N-terminal peptide (1-34) as a new potent antifungal agent.

摘要

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