H. Parry scite author profile

1Dimethylarginine dimethylaminohydrolase (DDAH), an enzyme that metabolizes the endogenous nitric oxide synthase inhibitors N0-monomethyl-L-arginine and NG,NG-dimethy-L-arginine to citrulline, was identified by Western blotting in rat and human tissue homogenates.2 S-2-amino-4(3-methylguanidino)butanoic acid (4124W) inhibited the metabolism of ["4C]-N0-monomethyl-L-arginine to ["4C]-citrulline by rat liver homogenates (IC50 416 + 66 giM; n = 9), human cultured endothelial cells (IC50 250 + 34 gLM; n = 9) and isolated purified dimethylarginine dimethylaminohydrolase. 3 Addition of 4124W to culture medium increased the accumulation of endogenously-generated N',N0-dimethy-L-arginine in the supernatant of human cultured endothelial cells from 3.1 + 0.3 to 5+0.7 ,M (n= 15; P<0.005). 4 4124W (1 uM-1 mM) had no direct effect on endothelial nitric oxide synthase activity but caused endothelium-dependent contraction of rat aortic rings (1 mM 4124W increased tone by 81.5 + 9.6% of that caused by phenylephrine 100 nM). This effect was reversed by L-arginine (100 giM). 4124W reversed endothelium-dependent relaxation of human saphenous vein (19.2 + 6.7% reversal of bradykinin-induced relaxation at 1 mM 4124W). 5 These data suggest that inhibition of dimethylarginine dimethylaminohydrolase increases the intracellular concentration of N',N0-dimethyl-L-arginine sufficiently to inhibit nitric oxide synthesis.Inhibiting the activity of DDAH may provide an alternative mechanism for inhibition of nitric oxide synthases and changes in the activity of DDAH could contribute to pathophysiological alterations in NO generation.

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Identification of a fibrinolytic enzyme in Schistosoma mansoni eggs and modulated blood fibrinogen metabolism in S. mansoni-infected mice

Doenhoff

Stanley

Pryce

et al. 2003

Parasitology

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Aqueous extracts of Schistosoma mansoni eggs have been shown to have fibrinolytic activity inhibitable by a serine protease inhibitor. Fibrinolytic activity was not present in extracts of either adult worms or cercariae. A 27 kDa enzyme that was proteolytically active on fibrinogen in zymography and that degraded fibrinogen in a pattern similar to that of plasmin, is presumed to be responsible for the schistosome egg fibrinolytic activity. Anti-human fibrinogen antisera were shown to have antibodies that cross-reacted with mouse fibrinogen in Western immunoblots. Electroblotted sera from S. mansoni-infected and control uninfected mice displayed different antigenic profiles when probed with the cross-reactive anti-human fibrinogen antibodies, suggesting an alteration in mouse host fibrinogen metabolism as a result of the parasitic infection. We discuss the possibility that modulation of fibrinogen metabolism is a factor in a recently discovered anti-atherogenic effect exerted by schistosomes.

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Immune-dependent thrombocytopaenia in mice infected with Schistosoma mansoni

Stanley

Ngaiza²,

Atieno

et al. 2003

Parasitology

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As has been shown previously, immunologically intact mice with patent Schistosoma mansoni infections had a significantly lower mean platelet number than intact uninfected mice (P<0.0001). However, platelet numbers in T-cell deprived mice with patent infections were not significantly different from those in uninfected T-cell deprived mice. Also, platelet counts in both the infected and uninfected T-cell deprived groups were not significantly different from those in intact uninfected mice. The S. mansoni-induced thrombocytopaenia in mice is thus seemingly immune dependent. Immunologically intact mice with chronic 12-week-old S. mansoni infections had IgG antibodies that were reactive in an ELISA-type assay with whole fixed platelets of both mouse and human origin. In Western immunoblots the IgG antibodies from chronically-infected mice reacted in particular against mouse and human platelet antigens of 90, 37 and 30 kDa. Antisera raised from 2 rabbits, immunized respectively with mouse and human platelet antigens, cross-reacted with antigens of the larval, adult worm and egg stages of S. mansoni. These results support the hypothesis that an anti-platelet antibody response may be the cause of the thrombocytopaenia observed in mice with patent schistosome infections.

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Inhibition of dimethylarginine dimethylaminohydrolase

MacAllister

Whitley²,

Parry

et al. 1995

Journal of Hypertension

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H. Parry

Regulation of nitric oxide synthesis by dimethylarginine dimethylaminohydrolase

Identification of a fibrinolytic enzyme in Schistosoma mansoni eggs and modulated blood fibrinogen metabolism in S. mansoni-infected mice

Immune-dependent thrombocytopaenia in mice infected with Schistosoma mansoni

Inhibition of dimethylarginine dimethylaminohydrolase

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