AI Article Synopsis

  • The study focuses on the Vip3Aa protein, which is effective against agricultural pests but faces resistance from lepidoptera species in the field.
  • Researchers constructed loop mutants by modifying specific loops in domain III of the protein and tested these mutants for toxicity and receptor binding.
  • They identified single mutants with significantly increased toxicity compared to the original Vip3Aa, demonstrating that modifying the loops can enhance the insecticidal properties of the protein.

Article Abstract

Vip3Aa, secreted by , is effective at controlling major agricultural pests such as However, to control Vip3Aa resistance evolved in the field by different lepidoptera species, an in-depth study of sequence--structure--activity relationships is necessary to design new Vip3Aa variants. In this study, the four specific loops (4-5 loop, 9-10 loop, 12-13 loop, and 14-15 loop) in domain III were selected and four loop mutants were constructed by replacing all residues in each specific loop with alanine. We obtained soluble proteins for three of the loop mutants, excluding the 9-10 loop. These loop mutants have been characterized by toxicity bioassays against , proteolytic processing, and receptor binding. These results indicate that the 4-5 loop and 14-15 loop are involved in receptor binding and Vip3Aa toxicity. Based on this, we constructed numerous mutants and obtained three single mutants (Vip3Aa-S366T, Vip3Aa-S366L, and Vip3Aa-R501A) that exhibited significantly increased toxicity of 2.61-fold, 3.39-fold, and 2.51-fold, respectively. Compared to Vip3Aa, the receptor affinity of Vip3Aa-S366T and Vip3Aa-S366L was significantly enhanced. Furthermore, we also analyzed and aligned the three-dimensional structures of the mutants and Vip3Aa. In summary, these results indicate that the loops in domain III have the potential to be targeted to enhance the insecticidal toxicity of the Vip3Aa protein.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10820090PMC
http://dx.doi.org/10.3390/toxins16010023DOI Listing

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