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Targeting the Respiratory Syncytial Virus N0-P Complex with Constrained ?-Helical Peptides in Cells and Mice.


ABSTRACT: Respiratory syncytial virus (RSV) is the main cause of severe respiratory infection in young children worldwide, and no therapies have been approved for the treatment of RSV infection. Data from recent clinical trials of fusion or L polymerase inhibitors for the treatment of RSV-infected patients revealed the emergence of escape mutants, highlighting the need for the discovery of inhibitors with novel mechanisms of action. Here we describe stapled peptides derived from the N terminus of the phosphoprotein (P) that act as replication inhibitors. We demonstrate that these peptides inhibit RSV replication in vitro and in vivo by preventing the formation of the N0-P complex. The present strategy provides a novel means of targeting RSV replication with constrained macrocyclic peptides or small molecules and is broadly applicable to other viruses of the Mononegavirales order.

SUBMITTER: Galloux M 

PROVIDER: S-EPMC7508628 | biostudies-literature | 2020 Sep

REPOSITORIES: biostudies-literature

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Targeting the Respiratory Syncytial Virus N<sup>0</sup>-P Complex with Constrained α-Helical Peptides in Cells and Mice.

Galloux Marie M   Gsponer Nadège N   Gaillard Vanessa V   Fenner Brice B   Larcher Thibaut T   Vilotte Marthe M   Rivière Julie J   Richard Charles-Adrien CA   Eléouët Jean-François JF   Le Goffic Ronan R   Mettier Joelle J   Nyanguile Origène O  

Antimicrobial agents and chemotherapy 20200921 10


Respiratory syncytial virus (RSV) is the main cause of severe respiratory infection in young children worldwide, and no therapies have been approved for the treatment of RSV infection. Data from recent clinical trials of fusion or L polymerase inhibitors for the treatment of RSV-infected patients revealed the emergence of escape mutants, highlighting the need for the discovery of inhibitors with novel mechanisms of action. Here we describe stapled peptides derived from the N terminus of the phos  ...[more]

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