Stimulation of Nipah Fusion: Small Intradomain Changes Trigger Extensive Interdomain Rearrangements

Nipah is an emerging paramyxovirus that is of serious concern to human health. It invades host cells using two of its membrane proteins—G and F. G binds to host ephrins and this stimulates G to activate F. Upon activation, F mediates virus-host membrane fusion. Here we focus on mechanisms that under...

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Published in:Biophysical journal 2016-10, Vol.111 (8), p.1621-1630
Main Authors: Dutta, Priyanka, Siddiqui, Ahnaf, Botlani, Mohsen, Varma, Sameer
Format: Article
Language:English
Subjects:
Binding sites
Biophysics
Computer simulation
Ephrins - metabolism
Membranes
Models, Molecular
Mutation
Nipah Virus - genetics
Nipah Virus - metabolism
Nipah Virus - physiology
Protein Binding
Protein Domains
Proteins
Viral Matrix Proteins - chemistry
Viral Matrix Proteins - genetics
Viral Matrix Proteins - metabolism
Virus Internalization
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creator Dutta, Priyanka
Siddiqui, Ahnaf
Botlani, Mohsen
Varma, Sameer
description Nipah is an emerging paramyxovirus that is of serious concern to human health. It invades host cells using two of its membrane proteins—G and F. G binds to host ephrins and this stimulates G to activate F. Upon activation, F mediates virus-host membrane fusion. Here we focus on mechanisms that underlie the stimulation of G by ephrins. Experiments show that G interacts with ephrin and F through separate sites located on two different domains, the receptor binding domain (RBD) and the F activation domain (FAD). No models explain this allosteric coupling. In fact, the analogous mechanisms in other paramyxoviruses also remain undetermined. The structural organization of G is such that allosteric coupling must involve at least one of the two interfaces—the RBD-FAD interface and/or the RBD-RBD interface. Here we examine using molecular dynamics the effect of ephrin binding on the RBD-RBD interface. We find that despite inducing small changes in individual RBDs, ephrin reorients the RBD-RBD interface extensively, and in a manner that will enhance solvent exposure of the FAD. While this finding supports a proposed model of G stimulation, we also find from additional simulations that ephrin induces a similar RBD-RBD reorientation in a stimulation-deficient G mutant, V209 VG → AAA. Together, our simulations suggest that while inter-RBD reorientation may be important, it is not, by itself, a sufficient condition for G stimulation. Additionally, we find that the mutation affects the conformational ensemble of RBD globally, including the RBD-FAD interface, suggesting the latter’s role in G stimulation. Because ephrin induces small changes in individual RBDs, a proper analysis of conformational ensembles required that they are compared directly—we employ a method we developed recently, which we now release at SimTK, and show that it also performs excellently for non-Gaussian distributions.
doi_str_mv 10.1016/j.bpj.2016.09.002
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subjects Binding sites
Biophysics
Computer simulation
Ephrins - metabolism
Membranes
Models, Molecular
Mutation
Nipah Virus - genetics
Nipah Virus - metabolism
Nipah Virus - physiology
Protein Binding
Protein Domains
Proteins
Viral Matrix Proteins - chemistry
Viral Matrix Proteins - genetics
Viral Matrix Proteins - metabolism
Virus Internalization
title Stimulation of Nipah Fusion: Small Intradomain Changes Trigger Extensive Interdomain Rearrangements
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