| Literature DB >> 29777666 |
Joaquín Gomis-Cebolla1, Yuequin Wang2, Yudong Quan1, Kanglai He2, Tom Walsh3, Bill James3, Sharon Downes4, Wendy Kain5, Ping Wang5, Kathy Leonard6, Tom Morgan6, Brenda Oppert6, Juan Ferré7.
Abstract
Bacillus thuringiensis Vip3 proteins are synthesized and secreted during the vegetative growth phase. They are activated by gut proteases, recognize and bind to midgut receptors, form pores and lyse cells. We tested the susceptibility to Vip3Aa and Vip3Ca of Cry1A-, Cry2A-, Dipel- and Vip3-resistant insect colonies from different species to determine whether resistance to other insecticidal proteins confers cross-resistance to Vip3 proteins. As expected, the colonies resistant to Cry1A proteins, Dipel (Helicoverpa armigera, Trichoplusia ni, Ostrinia furnacalis and Plodia interpunctella) or Cry2Ab (H. armigera and T. ni) were not cross-resistant to Vip3 proteins. In contrast, H. armigera colonies resistant to Vip3Aa or Vip3Aa/Cry2Ab showed cross-resistance to the Vip3Ca protein. Moreover, the Vip3Ca protein was highly toxic to O. furnacalis (LC50 not significantly different from that of Cry1Ab), whereas the Vip3Aa protein only showed moderate growth inhibition at the highest concentration tested (100 µg/g of diet). These results extend the cross-resistance studies between Vip3 and Cry proteins, show for the first time cross-resistance between proteins within the Vip3 subfamily, and points to O. furnacalis as a target for the Vip3Ca protein.Entities:
Keywords: Crop protection; Insect pest control; Insect resistance management
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Year: 2018 PMID: 29777666 DOI: 10.1016/j.jip.2018.05.004
Source DB: PubMed Journal: J Invertebr Pathol ISSN: 0022-2011 Impact factor: 2.841