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Literature summary extracted from
- A sterol C-14 reductase encoded by FgERG24B is responsible for the intrinsic resistance of Fusarium graminearum to amine fungicides (2011), Microbiology, 157, 1665-1675.
Inhibitors
| EC Number | Inhibitors | Comment | Organism | Structure |
|---|---|---|---|---|
| 1.3.1.70 | fenpropidin | - |
Fusarium graminearum |  |
| 1.3.1.70 | spiroxamine | - |
Fusarium graminearum | |
| 1.3.1.70 | tridemorph | - |
Fusarium graminearum | |
Organism
| EC Number | Organism | UniProt | Comment | Textmining |
|---|---|---|---|---|
| 1.3.1.70 | Fusarium graminearum | - |
- |
- |
Synonyms
| EC Number | Synonyms | Comment | Organism |
|---|---|---|---|
| 1.3.1.70 | FgERG24A | - |
Fusarium graminearum |
| 1.3.1.70 | FgERG24B | - |
Fusarium graminearum |
| 1.3.1.70 | sterol C-14 reductase | - |
Fusarium graminearum |
General Information
| EC Number | General Information | Comment | Organism |
|---|---|---|---|
| 1.3.1.70 | malfunction | FgERG24A and FgERG24B are deleted in Fusarium graminearum. Compared to the wild-type strain HN9-1, FgERG24A and FgERG24B deletion mutants do not show recognizable phenotypic changes in mycelial growth on potato dextrose agar or in virulence on wheat heads. FgERG24B deletion mutants exhibit significantly increased sensitivity to amine fungicides, including tridemorph, fenpropidin and spiroxamine. FgERG24A deletion mutants do not show changed sensitivity to any amine tested. The resistance of the FgERG24B deletion mutant to amines is restored by genetic complementation of the mutant with wild-type FgERG24B | Fusarium graminearum |
| 1.3.1.70 | physiological function | FgERG24B controls the intrinsic resistance of Fusarium graminearum to amines | Fusarium graminearum |
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