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      Inactivation of the complement anaphylatoxin C5a by secreted products of parasitic nematodes

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          Abstract

          Given the importance of the complement anaphylatoxins in cellular recruitment during infection, the ability of secreted products from larval stages of Brugia malayi and Trichinella spiralis to influence C5a-mediated chemotaxis of human peripheral blood granulocytes in vitro was examined. Secreted products from B. malayi microfilariae almost completely abolished chemotaxis. This inhibition was blocked by phenylmethylsulphonyl fluoride, indicating the presence of a serine protease, which was subsequently shown to cleave C5a. In contrast, secreted products from T. spiralis infective larvae showed modest inhibition of C5a-mediated granulocyte chemotaxis, and this was blocked by potato carboxypeptidase inhibitor, an inhibitor of several metallocarboxypeptidases. Adult and larval stages of both parasites were demonstrated to secrete carboxypeptidases which cleaved hippuryl- l-lysine and hippuryl- l-arginine, and the T. spiralis enzyme was partially characterised. The data are discussed with reference to inflammation in parasitic nematode infection.

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          Tricine-SDS-PAGE.

          Tricine-SDS-PAGE is commonly used to separate proteins in the mass range 1-100 kDa. It is the preferred electrophoretic system for the resolution of proteins smaller than 30 kDa. The concentrations of acrylamide used in the gels are lower than in other electrophoretic systems. These lower concentrations facilitate electroblotting, which is particularly crucial for hydrophobic proteins. Tricine-SDS-PAGE is also used preferentially for doubled SDS-PAGE (dSDS-PAGE), a proteomic tool used to isolate extremely hydrophobic proteins for mass spectrometric identification, and it offers advantages for resolution of the second dimension after blue-native PAGE (BN-PAGE) and clear-native PAGE (CN-PAGE). Here I describe a protocol for Tricine-SDS-PAGE, which includes efficient methods for Coomassie blue or silver staining and electroblotting, thereby increasing the versatility of the approach. This protocol can be completed in 1-2 d.
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            Preparation of iodine-131 labelled human growth hormone of high specific activity.

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              The dark side of C5a in sepsis.

              C. Ward (2004)
              Sepsis is a major clinical problem for which therapeutic interventions have been largely unsuccessful, in spite of promising strategies that were successful in animals, especially rodents. There is new evidence that sepsis causes excessive activation of the complement system and that this induces paralysis of innate immune functions in phagocytic cells due to effects of the powerful complement-activation product, C5a. This review describes our present understanding of how and why sepsis is a life-threatening condition and how it might be more effectively treated.
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                Author and article information

                Journal
                Int J Parasitol
                Int. J. Parasitol
                International Journal for Parasitology
                Elsevier Science
                0020-7519
                1879-0135
                April 2010
                April 2010
                : 40
                : 5
                : 527-532
                Affiliations
                Division of Cell & Molecular Biology, Department of Life Sciences, Imperial College London, London SW7 2AZ, UK
                Author notes
                [* ]Corresponding author. Tel.: +44 20 7594 5214; fax: +44 20 7594 5207. m.selkirk@ 123456imperial.ac.uk
                Article
                PARA3050
                10.1016/j.ijpara.2009.10.006
                2852653
                19874826
                6873da6b-942f-49af-857a-8d7015927646
                © 2010 Elsevier Ltd.

                This document may be redistributed and reused, subject to certain conditions.

                History
                : 14 August 2009
                : 4 October 2009
                : 8 October 2009
                Categories
                Article

                Parasitology
                trichinella spiralis,brugia malayi,nematode,complement,anaphylatoxin,c5a,inflammation
                Parasitology
                trichinella spiralis, brugia malayi, nematode, complement, anaphylatoxin, c5a, inflammation

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