Recombinant hirustasin: Production in yeast, crystallization, and interaction with serine proteases

Marco, Stefania Di; Fendrich, Gabriele; Knecht, René; Strauss, André; Pohlig, Gabriele; Heim, Jutta; Priestle, John P.; Sommerhoff, Christian P.; Grütter, Markus G.

doi:10.1002/pro.5560060112

Cited by 7 publications

(6 citation statements)

References 33 publications

(33 reference statements)

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“…This sequence is consistent with the intracellular processing of residues 1-64 of the ␣-factor leader peptide, resulting from the cleavage of the bond between Leu64 and Phe65. Interestingly, the N-terminal sequence found in the secreted precursor was the same as the one reported for a secreted ␣-factor-hirustatin fusion containing a wild-type ␣-factor leader sequence (29). Although the N-terminal extension does not affect the activity of hirustatin (29), its presence appears to abolish the inhibitory activity of the secreted ␣-factor-hirudin fusion protein.…”

Section: Expression Of An Inactive Hirudin Fusion and Its Activation supporting

confidence: 58%

Factor X Fusion Proteins: Improved Production and Use in the Release in Vitro of Biologically Active Hirudin from an Inactive α-Factor–Hirudin Fusion Protein

Guarna

Côté

Kwan

et al. 2000

Protein Expression and Purification

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Section: Expression Of An Inactive Hirudin Fusion and Its Activation supporting

confidence: 58%

Factor X Fusion Proteins: Improved Production and Use in the Release in Vitro of Biologically Active Hirudin from an Inactive α-Factor–Hirudin Fusion Protein

Guarna

Côté

Kwan

et al. 2000

Protein Expression and Purification

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“…Primary structural and X-ray crystallographic studies of antistasin and hirustasin have suggested that antistasin-type inhibitors have a similar disulfide bond pattern or tertiary structure (4,32,33). However, guamerin has a unique inhibition property toward elastase that is distinct from other antistasin-type inhibitors.…”

Section: Discussionmentioning

confidence: 99%

Production and Characterization of Recombinant Guamerin, an Elastase-Specific Inhibitor, in the Methylotrophic Yeast Pichia pastoris

Kim¹,

Lim²,

Lee³

et al. 2000

Protein Expression and Purification

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“…The importance of the reactive-site loop was partially demonstrated by the inhibitory activity of a disulRecently, X-ray crystallography of the hirustasin · tissue kallikrein complex [18,19] and the antistasin · factor Xa complex fide-bridge formation consisting of 19-residue peptides that contained the reactive-site sequence of guamerin [22]. Piguamerin [20,21] revealed the molecular interactions of the inhibitors with target proteases.…”

mentioning

confidence: 99%

Amino acid sequence of piguamerin, an antistasin‐type protease inhibitor from the blood sucking leech Hirudo nipponia

Kim

Kang

1998

European Journal of Biochemistry

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A serine-protease inhibitor of plasma kallikrein was screened and purified from a native Korean leech species, Hirudo nipponia. The peptide, named piguamerin, potently inhibited plasma and tissue kallikreins, and trypsin. Sequence analyses by automated Edman degradation revealed 48 amino acid residues and a molecular mass for the peptide of 5090 Da. Piguamerin is similar to antistasin-type inhibitors with the same spacing of ten cysteine residues, but shows differences from hirustasin, antistasin and ghilanten at the residues surrounding Arg27, which is a common P1 reactive residue for these inhibitors. The purified inhibitor modulated plasma clotting in tests of activated partial thromboplastin time at nanomolar concentrations. The serine-protease inhibitor of this leech may be involved in leech hematophagia.Keywords : leech ; plasma kallikrein; antistasin-type inhibitor.It has been demonstrated that hematophagous animals, such demonstrated no inhibition of factor Xa or thrombin. Unlike antistasin and ghilanten, hirustasin and the guamerins revealed as leeches, vampire bats, sucking lice and ticks, contain a variety of protease inhibitors that direct the coagulation mechanism [1]. no inhibitory activity against serine-protease functions related to coagulation. In the present paper, we report a kallikrein and trypAmong these animals, the leech is the most extensively studied for anticoagulant properties and for medical applications. Vari-sin inhibitor, piguamerin, which is derived from the blood-sucking leech H. nipponia. ous anticoagulants were purified from blood-sucking leeches: hirudin NH-Np, azocasein, and activated-partial-thromboplastin-time covered with the same cysteine spacing but half the molecular (APTT) kit (Cat.# A1801/A1926) were purchased from Sigma size of antistasin or ghilanten. Even though the primary strucChemical Co. Acetonitrile (HPLC grade) was purchased from tures of these inhibitors showed close similarity, each inhibitor Merck Chemical Co. Chromozym-TH was purchased from had a different protease target. Guamerin [9] and guamerin II Boehringer Mannheim. Chromatography columns, such as [10], isolated from blood-sucking Hirudo nipponia and nonAquapore RP-300 C 8 , Vydac 208TP54 C 8 and Macrpsphere 60 blood-sucking Whitmania edentula extracts, respectively, 7U Gel-Permeation, were purchased from Pierce, Vydac and Allshowed highly potent and specific inhibitory activities against tech, respectively. Adult leeches were collected from local ponds neutrophil and pancreatic elastases. Hirustasin, isolated from and cultivated in laboratory tanks until used [12]. Hirudo medicinalis, inhibits serine proteases such as trypsin, Purification. Crude extract was prepared by the aqueous chymotrypsin, cathepsin G and tissue kallikrein, but does not acetone/trichloroacetic acid method, as described previously [9, inhibit plasma kallikrein or elastase [11]. Furthermore, hirustasin 10]. The sample was passed through a DEAE-sepharose CL-6B column (50 ml), equilibrated with 10 mM Tris/HCl pH 8.0, and trifluro...

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Recombinant hirustasin: Production in yeast, crystallization, and interaction with serine proteases

Cited by 7 publications

References 33 publications

Factor X Fusion Proteins: Improved Production and Use in the Release in Vitro of Biologically Active Hirudin from an Inactive α-Factor–Hirudin Fusion Protein

Factor X Fusion Proteins: Improved Production and Use in the Release in Vitro of Biologically Active Hirudin from an Inactive α-Factor–Hirudin Fusion Protein

Production and Characterization of Recombinant Guamerin, an Elastase-Specific Inhibitor, in the Methylotrophic Yeast Pichia pastoris

Amino acid sequence of piguamerin, an antistasin‐type protease inhibitor from the blood sucking leech Hirudo nipponia

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