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10.1110/ps.051411805

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C2279309!2279309!16046624
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suck abstract from ncbi


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pmid16046624      Protein+Sci 2005 ; 14 (8): 1975-92
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  • The intrinsically disordered C-terminal domain of the measles virus nucleoprotein interacts with the C-terminal domain of the phosphoprotein via two distinct sites and remains predominantly unfolded #MMPMID16046624
  • Bourhis JM; Receveur-Bréchot V; Oglesbee M; Zhang X; Buccellato M; Darbon H; Canard B; Finet S; Longhi S
  • Protein Sci 2005[Aug]; 14 (8): 1975-92 PMID16046624show ga
  • Measles virus is a negative-sense, single-stranded RNA virus within theMononegavirales order,which includes several human pathogens, including rabies, Ebola, Nipah, and Hendra viruses. Themeasles virus nucleoprotein consists of a structured N-terminal domain, and of an intrinsically disordered C-terminal domain, NTAIL (aa 401?525), which undergoes induced folding in the presence of the C-terminal domain (XD, aa 459?507) of the viral phosphoprotein. With in NTAIL, an ?-helical molecular recognition element (?-MoRE, aa 488?499) involved in binding to P and in induced folding was identified and then observed in the crystal structure of XD. Using small-angle X-ray scattering, we have derived a low-resolution structural model of the complex between XD and NTAIL, which shows that most of NTAIL remains disordered in the complex despite P-induced folding within the ?-MoRE. The model consists of an extended shape accommodating the multiple conformations adopted by the disordered N-terminal region of NTAIL, and of a bulky globular region, corresponding to XD and to the C terminus of NTAIL (aa 486?525). Using surface plasmon resonance, circular dichroism, fluorescence spectroscopy, and heteronuclear magnetic resonance, we show that NTAIL has an additional site (aa 517?525) involved in binding to XD but not in the unstructured-to-structured transition. This work provides evidence that intrinsically disordered domains can establish complex interactions with their partners, and can contact them through multiple sites that do not all necessarily gain regular secondary structure.
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