3D structure of acetolactate synthase explains why the Asp-376-Glu point mutation does not give the same resistance level to different imidazolinone herbicides

3D structure of acetolactate synthase explains why the Asp-376-Glu point mutation does not give the same resistance level to different imidazolinone herbicides

Resistance to ALS-inhibiting herbicides has dramatically increased worldwide due to the persisting evolution of target site mutations that reduce the affinity between the herbicide and the target. We evaluated the effect of the well-known ALS Asp-376-Glu target site mutation on different imidazolino...

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Veröffentlicht in:Pesticide biochemistry and physiology 2024-09, Vol.204, p.106070, Article 106070
Hauptverfasser: Porri, Aimone, Panozzo, Silvia, Tekeste Sisay, Mihiret, Scarabel, Laura, Lerchl, Jens, Milani, Andrea
Format: Artikel
Sprache:eng
Schlagworte:
acetolactate synthase
Acetolactate Synthase - chemistry
Acetolactate Synthase - genetics
Acetolactate Synthase - metabolism
ALS enzyme structure
Amaranthus - drug effects
Amaranthus - genetics
Amaranthus retroflexus
Asp-376-Glu
biotypes
dose response
evolution
greenhouses
Herbicide resistance
Herbicide Resistance - genetics
Herbicides - chemistry
Herbicides - pharmacology
imazamox
imazethapyr
Imidazoles - chemistry
Imidazoles - pharmacology
Imidazolinones
Johnsongrass
ligands
Molecular Docking Simulation
mutants
Niacin - analogs & derivatives
Nicotinic Acids - pharmacology
oxygen
Plant Proteins - chemistry
Plant Proteins - genetics
Plant Proteins - metabolism
Point Mutation
Redroot pigweed
site-directed mutagenesis
Sorghum - drug effects
Sorghum - genetics
Sorghum halepense
sulfur
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Zusammenfassung:Resistance to ALS-inhibiting herbicides has dramatically increased worldwide due to the persisting evolution of target site mutations that reduce the affinity between the herbicide and the target. We evaluated the effect of the well-known ALS Asp-376-Glu target site mutation on different imidazolinone herbicides, including imazamox and imazethapyr. Greenhouse dose response experiments indicate that the Amaranthus retroflexus biotype carrying Asp-376-Glu was fully controlled by applying the field recommended dose of imazamox, whereas it displayed high level of resistance to imazethapyr. Likewise, Sorghum halepense, carrying Asp-376-Glu showed resistance to field recommended doses of imazethapyr but not of imazamox. Biochemical inhibition and kinetic characterization of the Asp-376-Glu mutant enzyme heterologously expressed using different plant sequence backbones, indicate that the Asp-376-Glu shows high level of insensitivity to imazethapyr but not to imazamox, corroborating the greenhouse results. Docking simulations revealed that imazamox can still inhibit the Asp-376-Glu mutant enzyme through a chalcogen interaction between the oxygen of the ligand and the sulfur atom of the ALS Met200, while imazethapyr does not create such interaction. These results explain the different sensitivity of the Asp-376-Glu mutation towards imidazolinone herbicides, thus providing novel information that can be exploited for defining stewardship guidelines to manage fields infested by weeds harboring the Asp-376-Glu mutation. [Display omitted] •different imidazolinones caused similar response in ALS 376-mutants of A. retroflexus and S. halepense.•Higher resistance level to imazethapyr was observed with respect to imazamox.•In vitro ALS enzyme activity confirmed the in vivo dose-response results.•Docking and structure-activity relationships of isoforms revealed the causal features.
ISSN:0048-3575
1095-9939
1095-9939
DOI:10.1016/j.pestbp.2024.106070