Literature summary for 3.2.1.14 extracted from

Takeo, S.; Hisamori, D.; Matsuda, S.; Vinetz, J.; Sattabongkot, J.; Tsuboi, T.
Enzymatic characterization of the Plasmodium vivax chitinase, a potential malaria transmission-blocking target (2009), Parasitol. Int., 58, 243-248.

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Cloned(Commentary)

Cloned (Comment)	Organism
expression with wheat germ cell-free system	Plasmodium vivax

Inhibitors

Inhibitors	Comment	Organism	Structure
allosamidin	-	Plasmodium vivax

Localization

Localization	Comment	Organism	GeneOntology No.	Textmining
cytoplasm	anterior cytoplasm of ookinete	Plasmodium vivax	5737	-

Organism

Organism	UniProt	Comment	Textmining
Plasmodium vivax	Q76EB5	-	-

Source Tissue

Source Tissue	Comment	Organism	Textmining
ookinete	-	Plasmodium vivax	-

Substrates and Products (Substrate)

Substrates	Comment Substrates	Organism	Products	Comment (Products)	Rev.	Reac.
4-methylumbelliferyl N,N',N''-beta-D-triacetylchitotrioside + H2O	substrate is prefered over shorter GlcNAc-substrates	Plasmodium vivax	4-methylumbelliferol + N,N',N''-beta-D-triacetylchitotriose	-	?

Temperature Optimum [°C]

Temperature Optimum [°C]	Temperature Optimum Maximum [°C]	Comment	Organism
25	-	-	Plasmodium vivax

pH Optimum

pH Optimum Minimum	pH Optimum Maximum	Comment	Organism
7	8	-	Plasmodium vivax

IC50 Value

IC50 Value	IC50 Value Maximum	Comment	Organism	Inhibitor	Structure
0.006	-	26°C	Plasmodium vivax	allosamidin

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Release 2023.1 (January 2023)