18 research outputs found
HSP90 Chaperoning in Addition to Phosphoprotein Required for Folding but Not for Supporting Enzymatic Activities of Measles and Nipah Virus L Polymerases
No full textMechanisms of partner recognition by intrinsically disordered proteins
No full text10th European-Biophysical-Societies-Association (EBSA) European Biophysics Congress, Dresden, GERMANY, JUL 18-22, 2015International audienceno abstrac
Mechanisms of partner recognition by intrinsically disordered proteins
No full text10th European-Biophysical-Societies-Association (EBSA) European Biophysics Congress, Dresden, GERMANY, JUL 18-22, 2015International audienceno abstrac
Etude de la structure de la mandibule à l'aide des méthodes modernes utilisées en engineering
No full textExploration of nucleoprotein α-MoRE and XD interactions of Nipah and Hendra viruses
No full textInternational audienceHenipavirus, including Hendra virus (HeV) and Nipah virus (NiV), is a newly discovered human pathogen genus. The nucleoprotein of Henipavirus contains an α-helical molecular recognition element (α-MoRE) that folds upon binding to the X domain (XD) of the phosphoprotein (P). In order to explore the conformational dynamics of free α-MoREs and the underlying binding-folding mechanism with XD, atomic force field-based and hybrid structure-based MD simulations were carried out. In our empirical force field-based simulations, characteristic structures and helicities of α-MoREs reveal the co-existence of partially structured and disordered conformations, as in the case of the well characterized cognate measles virus (MeV) α-MoRE. In spite of their overall similarity, the two α-MoREs display subtle helicity differences in their C-terminal region, but much different from that of MeV. For the α-MoRE/XD complexes, the results of our hybrid structure-based simulations provide the coupled binding-folding landscapes, and unveil a wide conformational selection mechanism at early binding stages, followed by a final induce-fit mechanism selection process. However, the HeV and NiV complexes have a lower binding barrier compared to that of MeV. Moreover, the HeV α-MoRE/XD complex shows much less coupling effects between binding and folding compared to that from both NiV and MeV. Our analysis revealed that contrary to NiV and MeV, the N- and C-terminal regions of the HeV α-MoRE maintains a low helicity also in the bound form
Demonstration of a Folding after Binding Mechanism in the Recognition between the Measles Virus N TAIL
No full textAtomic Resolution Description of the Interaction between the Nucleoprotein and Phosphoprotein of Hendra Virus
No full textRIG-I Self-Oligomerization Is Either Dispensable or Very Transient for Signal Transduction
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