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Applied and Environmental Microbiology, April 1999, p. 1413-1419, Vol. 65, No. 4
0099-2240/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Integrative Model for Binding of Bacillus
thuringiensis Toxins in Susceptible and Resistant Larvae
of the Diamondback Moth (Plutella xylostella)
Victoria
Ballester,1
Francisco
Granero,1
Bruce E.
Tabashnik,2
Thomas
Malvar,3 and
Juan
Ferré1,*
Departament de Genètica, Universitat de
València, 46100 Burjassot, València,
Spain1; Department of Entomology,
University of Arizona, Tucson, Arizona
857212; and Monsanto Co., St. Louis,
Missouri 631983
Received 17 September 1998/Accepted 5 January 1999
Insecticidal crystal proteins from Bacillus
thuringiensis in sprays and transgenic crops are extremely useful
for environmentally sound pest management, but their long-term efficacy
is threatened by evolution of resistance by target pests. The
diamondback moth (Plutella xylostella) is the first insect
to evolve resistance to B. thuringiensis in open-field
populations. The only known mechanism of resistance to B. thuringiensis in the diamondback moth is reduced binding of toxin
to midgut binding sites. In the present work we analyzed
competitive binding of B. thuringiensis toxins Cry1Aa,
Cry1Ab, Cry1Ac, and Cry1F to brush border membrane vesicles from larval
midguts in a susceptible strain and in resistant strains from the
Philippines, Hawaii, and Pennsylvania. Based on the results, we propose
a model for binding of B. thuringiensis crystal
proteins in susceptible larvae with two binding sites for
Cry1Aa, one of which is shared with Cry1Ab, Cry1Ac, and Cry1F. Our
results show that the common binding site is altered in each of the
three resistant strains. In the strain from the Philippines, the
alteration reduced binding of Cry1Ab but did not affect binding of the
other crystal proteins. In the resistant strains from
Hawaii and Pennsylvania, the alteration affected binding of
Cry1Aa, Cry1Ab, Cry1Ac, and Cry1F. Previously
reported evidence that a single mutation can confer resistance to
Cry1Ab, Cry1Ac, and Cry1F corresponds to expectations based on the
binding model. However, the following two other observations do not:
the mutation in the Philippines strain affected binding of only Cry1Ab,
and one mutation was sufficient for resistance to Cry1Aa. The imperfect
correspondence between the model and observations suggests that reduced
binding is not the only mechanism of resistance in the diamondback moth
and that some, but not all, patterns of resistance and cross-resistance can be predicted correctly from the results of competitive binding analyses of susceptible strains.
*
Corresponding author. Mailing address: Departament de
Genètica, Universitat de València, 46100 Burjassot,
València, Spain. Phone: 34-96-386-4506. Fax: 34-96-398-3029. E-mail: juan.ferre{at}uv.es.
Applied and Environmental Microbiology, April 1999, p. 1413-1419, Vol. 65, No. 4
0099-2240/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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