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Chemical Society Reviews 38 (4), 1187 (2009)
The Journal of biological chemistry 278 (9), 6809-15 (28 Feb 2003)
Trypanosoma brucei, the causative agent of African sleeping sickness, has three nearly identical genes encoding cysteine homologues of classical selenocysteine-containing glutathione peroxidases. The proteins are expressed in the mammalian and insect stages of the parasite. One of the genes, which contains a mitochondrial as well as a glycosomal targeting signal has been overexpressed. The recombinant T. brucei peroxidase has a high preference for the trypanothione/tryparedoxin couple as electron donor for the reduction of different hydroperoxides but accepts also T. brucei thioredoxin. The apparent rate constants k(2)' for the regeneration of the reduced enzyme are 2 x 10(5) m(-1) s(-1) with tryparedoxin and 5 x 10(3) m(-1) s(-1) with thioredoxin. No saturation kinetics was observed and the rate-limiting step of the overall reaction is reduction of the hydroperoxide. With glutathione, the peroxidase has marginal activity and reduction of the enzymes becomes limiting with a k(2)' value of 3 m (-1) s(-1). The T. brucei peroxidase, in contrast to the related Trypanosoma cruzi enzyme, also accepts hydrogen peroxide as substrate. The catalytic efficiency of the peroxidase studied here is comparable with that of the peroxiredoxin-like tryparedoxin peroxidases, which shows that trypanosomes possess two distinct peroxidase systems both dependent on the unique dithiol trypanothione.
Nature 452 (7189), 846-50 (17 Apr 2008)
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Dennis G. Morrell Catalysis Of Organic Reactions 2003 Description This text offers authoritative contributions from nearly 200 leaders in the field and new rapidshare.com ebook audiobook megaupload mediafire free download zip rar txt pdf chm books library direct links
Science (New York, N.Y.) 243 (4897), 1485-8 (17 Mar 1989)
Structure (London, England : 1993) 11 (8), 1015-23 (Aug 2003)
Structure (London, England : 1993) 16 (2), 196-209 (Feb 2008)
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