Literature DB >> 12642398

A potent tryptase inhibitor nafamostat mesilate dramatically suppressed pulmonary dysfunction induced in rats by a radiographic contrast medium.

Toshiaki Sendo1, Yoshinori Itoh, Takeshi Goromaru, Tomoko Sumimura, Mami Saito, Keisei Aki, Takahisa Yano, Ryozo Oishi.   

Abstract

(1) Intravenous injection of ioxaglate (4 g iodine kg(-1)), an iodinated radiographic contrast medium, caused a marked protein extravasation, pulmonary oedema and a decrease in the arterial partial oxygen pressure in rats. (2) All of these reactions to ioxaglate were reversed by the pretreatment with gabexate mesilate (10 and 50 mg kg(-1), 5 min prior to injection) or nafamostat mesilate (3 and 10 mg kg(-1)), in which the inhibition was complete after injection of nafamostat mesilate (10 mg kg(-1)). (3) Both gabexate mesilate and nafamostat mesilate inhibited the activity of purified human lung tryptase, although the latter compound was far more potent than the former. (4) Ioxaglate enhanced the nafamostat-sensitive protease activity in the extracellular fluid of rat peritoneal mast cell suspensions. (5) Tryptase enhanced the permeability of protein through the monolayer of cultured human pulmonary arterial endothelial cells. Ioxaglate, when applied in combination with rat peritoneal mast cells, also produced the endothelial barrier dysfunction. These effects of tryptase and ioxaglate were reversed by nafamostat mesilate. (6) Consistent with these findings, immunofluorescence morphological analysis revealed that tryptase or ioxaglate in combination with mast cells increased actin stress fibre formation while decreasing VE-cadherin immunoreactivity. Both of these actions of tryptase and ioxaglate were reversed by nafamostat mesilate. (7) These findings suggest that tryptase liberated from mast cells plays a crucial role in the ioxaglate-induced pulmonary dysfunction. In this respect, nafamostat mesilate may become a useful agent for the cure or prevention of severe adverse reactions to radiographic contrast media.

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Year:  2003        PMID: 12642398      PMCID: PMC1573732          DOI: 10.1038/sj.bjp.0705121

Source DB:  PubMed          Journal:  Br J Pharmacol        ISSN: 0007-1188            Impact factor:   8.739


  43 in total

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Journal:  Invest Radiol       Date:  2002-01       Impact factor: 6.016

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Authors:  N Vergnolle; M D Hollenberg; K A Sharkey; J L Wallace
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4.  Presence and bronchomotor activity of protease-activated receptor-2 in guinea pig airways.

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5.  Contrast media as histamine liberators. II. Histamine release into venous plasma during intravenous urography in man.

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Journal:  Invest Radiol       Date:  1970 Nov-Dec       Impact factor: 6.016

6.  Histamine release and complement changes following injection of contrast media in humans.

Authors:  F C Cogen; M E Norman; E Dunsky; J Hirshfeld; B Zweiman
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7.  The kinetic and structural characterization of the reaction of nafamostat with bovine pancreatic trypsin.

Authors:  M K Ramjee; I M Henderson; S B McLoughlin; A Padova
Journal:  Thromb Res       Date:  2000-06-15       Impact factor: 3.944

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Authors:  S R Coughlin
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9.  Nitric oxide protects against contrast media-increased pulmonary vascular permeability in rats.

Authors:  T Sendo; Y Kataoka; Y Takeda; W Furuta; R Oishi
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10.  Selective inhibition of human mast cell tryptase by gabexate mesylate, an antiproteinase drug.

Authors:  F Erba; L Fiorucci; S Pascarella; E Menegatti; P Ascenzi; F Ascoli
Journal:  Biochem Pharmacol       Date:  2001-02-01       Impact factor: 5.858

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Journal:  Eur J Pharmacol       Date:  2015-05-07       Impact factor: 4.432

4.  THE AUTOCRINE ROLE OF TRYPTASE IN PRESSURE OVERLOAD-INDUCED MAST CELL ACTIVATION, CHYMASE RELEASE AND CARDIAC FIBROSIS.

Authors:  Jianping Li; Shaiban Jubair; Scott P Levick; Joseph S Janicki
Journal:  IJC Metab Endocr       Date:  2015-11-24

Review 5.  Targeted treatment of pruritus: a look into the future.

Authors:  H L Tey; G Yosipovitch
Journal:  Br J Dermatol       Date:  2011-05-30       Impact factor: 9.302

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7.  Carbazochrome sodium sulfonate (AC-17) reverses endothelial barrier dysfunction through inhibition of phosphatidylinositol hydrolysis in cultured porcine endothelial cells.

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  7 in total

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