2017
DOI: 10.1101/211284
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The amyloidogenicity of the influenza virus PB1-derived peptide sheds light on its antiviral activity

Abstract: The influenza virus polymerase complex is a promising target for new antiviral drug development. It is known that, within the influenza virus polymerase complex, the PB1 subunit region from the 1 st to the 25 th amino acid residues has to be is in an alpha-helical conformation for proper interaction with the PA subunit. We have previously shown that PB1(6-13) peptide at low concentrations is able to interact with the PB1 subunit N-terminal region in a peptide model which shows aggregate formation and antiviral… Show more

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Cited by 1 publication
(2 citation statements)
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“…The third mechanism is rarely reported. Zabrodskaya et al (2018) reported that the amyloid peptide PB1(6-13) (6-13 residues of basic polymerase 1) monomer, derived from the influenza A virus polymerase complex PB1, was found to interact with its matrix protein PB1 subunit N-terminal region, causing a conformation of PB1 shift toward beta structures, and making PB1 lost its ability to interact with the acidic polymerase subunit; as a result, the influenza virus' polymerase complex functionality was broken (Egorov et al 2013;Zabrodskaya et al 2018).…”
Section: Third Antimicrobial Mechanism: Conformation Change and Funct...mentioning
confidence: 99%
See 1 more Smart Citation
“…The third mechanism is rarely reported. Zabrodskaya et al (2018) reported that the amyloid peptide PB1(6-13) (6-13 residues of basic polymerase 1) monomer, derived from the influenza A virus polymerase complex PB1, was found to interact with its matrix protein PB1 subunit N-terminal region, causing a conformation of PB1 shift toward beta structures, and making PB1 lost its ability to interact with the acidic polymerase subunit; as a result, the influenza virus' polymerase complex functionality was broken (Egorov et al 2013;Zabrodskaya et al 2018).…”
Section: Third Antimicrobial Mechanism: Conformation Change and Funct...mentioning
confidence: 99%
“…In addition, Juhl et al (2020) found the antimicrobial activities of peptidyl-glycineleucine-carboxyamide (PGLa) decreased with fibril formation. Besides, Zabrodskaya et al (2018) found that after the amyloid peptide PB1(6-13) monomer formation into fibrils, it was no longer able to interact with PB1 N-terminal region, nor was it able to exert antiviral activity. Different antimicrobial effectiveness are reported even for the same amyloid proteins.…”
Section: Which State Is Effective: Monomers Oligomers or Fibrils?mentioning
confidence: 99%