Literature DB >> 27488102

Molecular cloning and in silico characterization of knottin peptide, U2-SCRTX-Lit2, from brown spider (Loxosceles intermedia) venom glands.

Gabriel Otto Meissner1, Pedro Túlio de Resende Lara2, Luis Paulo Barbour Scott2, Antônio Sérgio Kimus Braz2, Daniele Chaves-Moreira1, Fernando Hitomi Matsubara1, Eduardo Mendonça Soares1, Dilza Trevisan-Silva1, Luiza Helena Gremski1,3, Silvio Sanches Veiga1, Olga Meiri Chaim4.   

Abstract

Inhibitor cystine knots (ICKs) are a family of structural peptides with a large number of cysteine residues that form intramolecular disulfide bonds, resulting in a knot. These peptides are involved in a variety of biological functions including predation and defense, and are found in various species, such as spiders, scorpions, sea anemones, and plants. The Loxosceles intermedia venom gland transcriptome identified five groups of ICK peptides that represent more than 50 % of toxin-coding transcripts. Here, we describe the molecular cloning of U2-Sicaritoxin-Lit2 (U2-SCRTX-Lit2), bioinformatic characterization, structure prediction, and molecular dynamic analysis. The sequence of U2-SCRTX-Lit2 obtained from the transcriptome is similar to that of μ-Hexatoxin-Mg2, a peptide that inhibits the insect Nav channel. Bioinformatic analysis of sequences classified as ICK family members also showed a conservation of cysteine residues among ICKs from different spiders, with the three dimensional molecular model of U2-SCRTX-Lit2 similar in structure to the hexatoxin from μ-hexatoxin-Mg2a. Molecular docking experiments showed the interaction of U2-SCRTX-Lit2 to its predictable target-the Spodoptera litura voltage-gated sodium channel (SlNaVSC). After 200 ns of molecular dynamic simulation, the final structure of the complex showed stability in agreement with the experimental data. The above analysis corroborates the existence of a peptide toxin with insecticidal activity from a novel ICK family in L. intermedia venom and demonstrates that this peptide targets Nav channels.

Entities:  

Keywords:  Brown Spider; ICK; Insecticide toxin; Molecular modeling; Peptide structure; Venom

Mesh:

Substances:

Year:  2016        PMID: 27488102     DOI: 10.1007/s00894-016-3067-0

Source DB:  PubMed          Journal:  J Mol Model        ISSN: 0948-5023            Impact factor:   1.810


  72 in total

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Review 3.  CHARMM: the biomolecular simulation program.

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Journal:  J Comput Chem       Date:  2009-07-30       Impact factor: 3.376

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10.  KNOTTIN: the knottin or inhibitor cystine knot scaffold in 2007.

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Review 1.  Highlights in the knowledge of brown spider toxins.

Authors:  Daniele Chaves-Moreira; Andrea Senff-Ribeiro; Ana Carolina Martins Wille; Luiza Helena Gremski; Olga Meiri Chaim; Silvio Sanches Veiga
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2.  Loxosceles gaucho Spider Venom: An Untapped Source of Antimicrobial Agents.

Authors:  Paula J Segura-Ramírez; Pedro I Silva Júnior
Journal:  Toxins (Basel)       Date:  2018-12-06       Impact factor: 4.546

3.  Molecular, Biological and Structural Features of VL CDR-1 Rb44 Peptide, Which Targets the Microtubule Network in Melanoma Cells.

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Review 4.  Prospective Use of Brown Spider Venom Toxins as Therapeutic and Biotechnological Inputs.

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Journal:  Front Mol Biosci       Date:  2021-06-17
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