Helical peptides with disordered regions for measles viruses provide new generalized insights into fusion inhibitors

Kazushige Hirata; Aoi Takahara; Satoshi Suzuki; Shumei Murakami; Kumi Kawaji; Akie Nishiyama; Mina Sasano; Mariko Shoji-Ueno; Emiko Usui; Kazutaka Murayama; Hironori Hayashi; Shinya Oishi; Eiichi N. Kodama

doi:10.1016/j.isci.2024.108961

Helical peptides with disordered regions for measles viruses provide new generalized insights into fusion inhibitors

Kazushige Hirata, Aoi Takahara, Satoshi Suzuki, Shumei Murakami, Kumi Kawaji, Akie Nishiyama, Mina Sasano, Mariko Shoji-Ueno, Emiko Usui, Kazutaka Murayama, Hironori Hayashi, Shinya Oishi, Eiichi N. Kodama

Research output: Contribution to journal › Article › peer-review

1 Citation (Scopus)

Abstract

Despite effective vaccines, measles virus (MeV) outbreaks occur sporadically. Therefore, developing anti-MeV agents remains important for suppressing MeV infections. We previously designed peptide-based MeV fusion inhibitors, M1 and M2, that target MeV class I fusion protein (F protein). Here, we developed a novel fusion inhibitor, MEK35, that exerts potent activity against M1/M2-resistant MeV variants. Comparing MEK35 to M1 derivatives revealed that combining disordered and helical elements was essential for overcoming M1/M2 resistance. Moreover, we propose a three-step antiviral process for peptide-based fusion inhibitors: (i) disordered peptides interact with F protein; (ii) the peptides adopt a partial helical conformation and bind to F protein through hydrophobic interactions; and (iii) subsequent interactions involving the disordered region of the peptides afford a peptide-F protein with a high-affinity peptide-F protein interaction. An M1-resistant substitution blocks the second step. These results should aid the development of novel viral fusion inhibitors targeting class I F protein.

Original language	English
Article number	108961
Journal	iScience
Volume	27
Issue number	2
DOIs	https://doi.org/10.1016/j.isci.2024.108961
Publication status	Published - 2024 Feb 16

Keywords

Molecular biology
Virology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.isci.2024.108961

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Hirata, K., Takahara, A., Suzuki, S., Murakami, S., Kawaji, K., Nishiyama, A., Sasano, M., Shoji-Ueno, M., Usui, E., Murayama, K., Hayashi, H., Oishi, S., & Kodama, E. N. (2024). Helical peptides with disordered regions for measles viruses provide new generalized insights into fusion inhibitors. iScience, 27(2), Article 108961. https://doi.org/10.1016/j.isci.2024.108961

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abstract = "Despite effective vaccines, measles virus (MeV) outbreaks occur sporadically. Therefore, developing anti-MeV agents remains important for suppressing MeV infections. We previously designed peptide-based MeV fusion inhibitors, M1 and M2, that target MeV class I fusion protein (F protein). Here, we developed a novel fusion inhibitor, MEK35, that exerts potent activity against M1/M2-resistant MeV variants. Comparing MEK35 to M1 derivatives revealed that combining disordered and helical elements was essential for overcoming M1/M2 resistance. Moreover, we propose a three-step antiviral process for peptide-based fusion inhibitors: (i) disordered peptides interact with F protein; (ii) the peptides adopt a partial helical conformation and bind to F protein through hydrophobic interactions; and (iii) subsequent interactions involving the disordered region of the peptides afford a peptide-F protein with a high-affinity peptide-F protein interaction. An M1-resistant substitution blocks the second step. These results should aid the development of novel viral fusion inhibitors targeting class I F protein.",

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author = "Kazushige Hirata and Aoi Takahara and Satoshi Suzuki and Shumei Murakami and Kumi Kawaji and Akie Nishiyama and Mina Sasano and Mariko Shoji-Ueno and Emiko Usui and Kazutaka Murayama and Hironori Hayashi and Shinya Oishi and Kodama, \{Eiichi N.\}",

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doi = "10.1016/j.isci.2024.108961",

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AU - Hirata, Kazushige

AU - Takahara, Aoi

AU - Suzuki, Satoshi

AU - Murakami, Shumei

AU - Kawaji, Kumi

AU - Nishiyama, Akie

AU - Sasano, Mina

AU - Shoji-Ueno, Mariko

AU - Usui, Emiko

AU - Murayama, Kazutaka

AU - Hayashi, Hironori

AU - Oishi, Shinya

AU - Kodama, Eiichi N.

PY - 2024/2/16

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N2 - Despite effective vaccines, measles virus (MeV) outbreaks occur sporadically. Therefore, developing anti-MeV agents remains important for suppressing MeV infections. We previously designed peptide-based MeV fusion inhibitors, M1 and M2, that target MeV class I fusion protein (F protein). Here, we developed a novel fusion inhibitor, MEK35, that exerts potent activity against M1/M2-resistant MeV variants. Comparing MEK35 to M1 derivatives revealed that combining disordered and helical elements was essential for overcoming M1/M2 resistance. Moreover, we propose a three-step antiviral process for peptide-based fusion inhibitors: (i) disordered peptides interact with F protein; (ii) the peptides adopt a partial helical conformation and bind to F protein through hydrophobic interactions; and (iii) subsequent interactions involving the disordered region of the peptides afford a peptide-F protein with a high-affinity peptide-F protein interaction. An M1-resistant substitution blocks the second step. These results should aid the development of novel viral fusion inhibitors targeting class I F protein.

AB - Despite effective vaccines, measles virus (MeV) outbreaks occur sporadically. Therefore, developing anti-MeV agents remains important for suppressing MeV infections. We previously designed peptide-based MeV fusion inhibitors, M1 and M2, that target MeV class I fusion protein (F protein). Here, we developed a novel fusion inhibitor, MEK35, that exerts potent activity against M1/M2-resistant MeV variants. Comparing MEK35 to M1 derivatives revealed that combining disordered and helical elements was essential for overcoming M1/M2 resistance. Moreover, we propose a three-step antiviral process for peptide-based fusion inhibitors: (i) disordered peptides interact with F protein; (ii) the peptides adopt a partial helical conformation and bind to F protein through hydrophobic interactions; and (iii) subsequent interactions involving the disordered region of the peptides afford a peptide-F protein with a high-affinity peptide-F protein interaction. An M1-resistant substitution blocks the second step. These results should aid the development of novel viral fusion inhibitors targeting class I F protein.

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KW - Virology

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Helical peptides with disordered regions for measles viruses provide new generalized insights into fusion inhibitors

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Keywords

UN SDGs

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