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The effectiveness of difenacoum against Norway Rats (Rattus norvegicus) on farms in a tyrosine139cysteine focus of anticoagulant resistance in Westphalia, Germany

Zugehörigkeit
Vertebrate Pests Unit, School of Biological Sciences, The University of Reading, Reading, UK
Buckle, Alan;
Zugehörigkeit
Bayer CropScience AG – Environmental Science,Monheim, Germany
Endepols, Stefan;
Zugehörigkeit
Spillenweg 3,Warendorf, Germany
Klemann, Nicole;
GND
122411307
Zugehörigkeit
Julius Kühn-Institute (JKI), Institute for Plant Protection in Horticulture and Forests, Germany
Jacob, Jens

BACKGROUND: Anticoagulant resistance in Norway rats at foci in Belgium, Denmark, France, Germany, the Netherlands and the United Kingdom is genetically characterised by the same single nucleotide polymorphism (SNP) and consequent amino acid exchange from tyrosine to cysteine at location 139 of the vkorc1 gene (i.e. tyrosine139cysteine or Y139C). The purpose of this study was to assess the degree of resistance among rats at two infested farm sites in the Y139C focus in Westphalia, Germany, using blood clotting response (BCR) tests, and to determine the practical efficacy of applications of a commercial 50 ppm difenacoum bait (Neokil) against them. RESULTS: BCR tests showed that the difenacoum resistance factor (RF) among the Y139C rats was about 2.5. DNA analysis for the Y139C mutation revealed that it was present among rats at the two sites with a prevalence of 75 and 93%. Applications of difenacoum bait at the two sites achieved 86.8 and 59.9% control. The different outcomes did not appear to be due to differences either in the degree and prevalence of resistance or in the quantities of poisoned bait consumed. CONCLUSION: The study showed that, although the RF for difenacoum among rats carrying the Y139C SNP was apparently low, an acceptable level of control of resistant Norway rat infestations was not achieved using difenacoum. Continued use of anticoagulants against rats that are resistant to them will exacerbate resistance problems in terms of both increased severity and prevalence. These conclusions are likely to apply elsewhere in Europe where the Y139C SNP occurs.

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