The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families
Brüning M, Lummer M, Bentele C, Smolenaars MMW, Rodenburg KW, Ragg H (2007)
Biochem. J. 401(1): 325-331.
Zeitschriftenaufsatz
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Autor*in
Brüning, Mareke;
Lummer, MartinaUniBi;
Bentele, Caterina;
Smolenaars, Marcel M. W.;
Rodenburg, Kees W;
Ragg, HermannUniBi
Einrichtung
Centrum für Biotechnologie > Institut für Biochemie und Biotechnik
Fakultät für Biologie > RNA Biologie und Molekulare Physiologie
Centrum für Biotechnologie > Institut für Genomforschung und Systembiologie
Technische Fakultät > AG Zelluläre Genetik
Centrum für Biotechnologie > Arbeitsgruppe H. Ragg
Fakultät für Biologie > RNA Biologie und Molekulare Physiologie
Centrum für Biotechnologie > Institut für Genomforschung und Systembiologie
Technische Fakultät > AG Zelluläre Genetik
Centrum für Biotechnologie > Arbeitsgruppe H. Ragg
Abstract / Bemerkung
By alternative use of four RSL (reactive site loop) coding exon cassettes, the serpin (serine protease inhibitor) gene Spn4 from Drosophila melanogaster was proposed to enable the synthesis of multiple protease inhibitor isoforms, one of which has been shown to be a potent inhibitor of human furin. Here, we have investigated the inhibitory spectrum of all Spn4 RSL variants. The analyses indicate that the Spn4 gene encodes inhibitors that may inhibit serine proteases of the subtilase family (S8), the chymotrypsin family (SI), and the papain-like cysteine protease family (CI), most of them at high rates. Thus a cohort of different protease inhibitors is generated simply by grafting enzyme-adapted RSL sequences on to a single serpin scaffold, even though the target proteases contain different types and/or a varying order of catalytic residues and are descendents of different phylogenetic lineages. Since all of the Spn4 RSL isoforms are produced as intracellular residents and additionally as variants destined for export or associated with the secretory pathway, the Spn4 gene represents a versatile defence tool kit that may provide multiple antiproteolytic functions.
Stichworte
endoplasmic reticulum (ER) retention;
signal;
serpin;
cysteine protease inhibitor;
serine protease inhibitor;
furin
Erscheinungsjahr
2007
Zeitschriftentitel
Biochem. J.
Band
401
Ausgabe
1
Seite(n)
325-331
ISSN
0264-6021
eISSN
1470-8728
Page URI
https://pub.uni-bielefeld.de/record/1953796
Zitieren
Brüning M, Lummer M, Bentele C, Smolenaars MMW, Rodenburg KW, Ragg H. The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families. Biochem. J. 2007;401(1):325-331.
Brüning, M., Lummer, M., Bentele, C., Smolenaars, M. M. W., Rodenburg, K. W., & Ragg, H. (2007). The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families. Biochem. J., 401(1), 325-331. https://doi.org/10.1042/BJ20060648
Brüning, Mareke, Lummer, Martina, Bentele, Caterina, Smolenaars, Marcel M. W., Rodenburg, Kees W, and Ragg, Hermann. 2007. “The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families”. Biochem. J. 401 (1): 325-331.
Brüning, M., Lummer, M., Bentele, C., Smolenaars, M. M. W., Rodenburg, K. W., and Ragg, H. (2007). The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families. Biochem. J. 401, 325-331.
Brüning, M., et al., 2007. The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families. Biochem. J., 401(1), p 325-331.
M. Brüning, et al., “The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families”, Biochem. J., vol. 401, 2007, pp. 325-331.
Brüning, M., Lummer, M., Bentele, C., Smolenaars, M.M.W., Rodenburg, K.W., Ragg, H.: The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families. Biochem. J. 401, 325-331 (2007).
Brüning, Mareke, Lummer, Martina, Bentele, Caterina, Smolenaars, Marcel M. W., Rodenburg, Kees W, and Ragg, Hermann. “The Spn4 gene from Drosophila melanogaster is a multipurpose defense tool directed against proteases from three different peptidase families”. Biochem. J. 401.1 (2007): 325-331.
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Aguilar R, Jedlicka AE, Mintz M, Mahairaki V, Scott AL, Dimopoulos G., Insect Biochem. Mol. Biol. 35(7), 2005
PMID: 15894188
Aguilar R, Jedlicka AE, Mintz M, Mahairaki V, Scott AL, Dimopoulos G., Insect Biochem. Mol. Biol. 35(7), 2005
PMID: 15894188
The novel bovine serpin endopin 2C demonstrates selective inhibition of the cysteine protease cathepsin L compared to the serine protease elastase, in cross-class inhibition.
Hwang SR, Stoka V, Turk V, Hook VY., Biochemistry 44(21), 2005
PMID: 15909990
Hwang SR, Stoka V, Turk V, Hook VY., Biochemistry 44(21), 2005
PMID: 15909990
Endosomal proteolysis of the Ebola virus glycoprotein is necessary for infection.
Chandran K, Sullivan NJ, Felbor U, Whelan SP, Cunningham JM., Science 308(5728), 2005
PMID: 15831716
Chandran K, Sullivan NJ, Felbor U, Whelan SP, Cunningham JM., Science 308(5728), 2005
PMID: 15831716
Drosophila host defense after oral infection by an entomopathogenic Pseudomonas species.
Vodovar N, Vinals M, Liehl P, Basset A, Degrouard J, Spellman P, Boccard F, Lemaitre B., Proc. Natl. Acad. Sci. U.S.A. 102(32), 2005
PMID: 16061818
Vodovar N, Vinals M, Liehl P, Basset A, Degrouard J, Spellman P, Boccard F, Lemaitre B., Proc. Natl. Acad. Sci. U.S.A. 102(32), 2005
PMID: 16061818
Cathepsin L in secretory vesicles functions as a prohormone-processing enzyme for production of the enkephalin peptide neurotransmitter.
Yasothornsrikul S, Greenbaum D, Medzihradszky KF, Toneff T, Bundey R, Miller R, Schilling B, Petermann I, Dehnert J, Logvinova A, Goldsmith P, Neveu JM, Lane WS, Gibson B, Reinheckel T, Peters C, Bogyo M, Hook V., Proc. Natl. Acad. Sci. U.S.A. 100(16), 2003
PMID: 12869695
Yasothornsrikul S, Greenbaum D, Medzihradszky KF, Toneff T, Bundey R, Miller R, Schilling B, Petermann I, Dehnert J, Logvinova A, Goldsmith P, Neveu JM, Lane WS, Gibson B, Reinheckel T, Peters C, Bogyo M, Hook V., Proc. Natl. Acad. Sci. U.S.A. 100(16), 2003
PMID: 12869695
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