The Spodoptera exigua ABCC2 Acts as a Cry1A Receptor Independently of its Nucleotide Binding Domain II

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RESEARCH PRODUCT

The Spodoptera exigua ABCC2 Acts as a Cry1A Receptor Independently of its Nucleotide Binding Domain II

Salvador Herrero María Martínez-solís Patricia Hernández-martínez Juan Ferré Daniel Pinos

subject

0106 biological sciences Cell Survival Health Toxicology and Mutagenesis lcsh:Medicine Receptors Cell Surface ATP-binding cassette transporter Spodoptera Spodoptera Toxicology medicine.disease_cause Bt resistance 01 natural sciences Article Cell Line Hemolysin Proteins 03 medical and health sciences Bacterial Proteins mode of action GTP-Binding Proteins ATP hydrolysis medicine Animals Receptor 030304 developmental biology 0303 health sciences Mutation Bacillus thuringiensis Toxins biology Chemistry fungi lcsh:R heterologous expression Transporter biology.organism_classification Multidrug Resistance-Associated Protein 2 Cell biology Endotoxins 010602 entomology Cyclic nucleotide-binding domain Sf21 cells truncated transporter Insect Proteins Heterologous expression Multidrug Resistance-Associated Proteins

description

ABC proteins are primary-active transporters that require the binding and hydrolysis of ATP to transport substrates across the membrane. Since the first report of an ABCC2 transporter as receptor of Cry1A toxins, the number of ABC transporters known to be involved in the mode of action of Cry toxins has increased. In Spodoptera exigua, a mutation in the SeABCC2 gene is described as genetically linked to resistance to the Bt-product XentariTM. This mutation affects an intracellular domain involved in ATP binding, but not the extracellular loops. We analyzed whether this mutation affects the role of the SeABCC2 as a functional receptor to Cry1A toxins. The results show that Sf21 cells expressing the truncated form of the transporter were susceptible to Cry1A toxins. Moreover, specific Cry1Ac binding was observed in those cells expressing the truncated SeABCC2. Additionally, no differences in the irreversible Cry1Ac binding component (associated with the toxin insertion into the membrane) were observed when tested in Sf21 cells expressing either the full-length or the truncated form of the SeABCC2 transporter. Therefore, our results point out that the partial lack of the nucleotide binding domain II in the truncated transporter does not affect its functionality as a Cry1A receptor.

year	journal	country	edition	language
2019-03-22	Toxins

10.3390/toxins11030172 https://www.mdpi.com/2072-6651/11/3/172