New Insights into Structural Disorder in Human Respiratory Syncytial Virus Phosphoprotein and Implications for Binding of Protein Partners

被引:0
|
作者
Pereira, Nelson [1 ]
Cardone, Christophe [1 ]
Lassoued, Safa [1 ]
Galloux, Marie [2 ]
Fix, Jenna [2 ]
Assrir, Nadine [1 ]
Lescop, Ewen [1 ]
Bontems, Francois [1 ]
Eleouet, Jean-Francois [2 ]
Sizun, Christina [1 ]
机构
[1] Univ Paris Saclay, CNRS, UPR2301, Inst Chim Subst Nat, F-91190 Gif Sur Yvette, France
[2] INRA, UR892, Unite Virol & Immunol Mol, F-78350 Jouy En Josas, France
关键词
PARAMAGNETIC RELAXATION ENHANCEMENT; MULTIPLE SEQUENCE ALIGNMENTS; P-PROTEIN; N-PROTEIN; FUNCTIONAL-CHARACTERIZATION; POLYMERASE COMPLEX; INFECTED CELLS; M2-1; PROTEIN; RNA; IDENTIFICATION;
D O I
10.1074/jbc.M116.765958
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Phosphoprotein is the main cofactor of the viral RNA polymerase of Mononegavirales. It is involved in multiple interactions that are essential for the polymerase function. Most prominently it positions the polymerase complex onto the nucleocapsid, but also acts as a chaperone for the nucleoprotein. Mononegavirales phosphoproteins lack sequence conservation, but contain all large disordered regions. We show here that Nand Cterminal intrinsically disordered regions account for 80% of the phosphoprotein of the respiratory syncytial virus. But these regions display marked dynamic heterogeneity. Whereas almost stable helices are formed C terminally to the oligomerization domain, extremely transient helices are present in the N terminal region. They all mediate internal long range contacts in this non globular protein. Transient secondary elements together with fully disordered regions also provide protein binding sites recognized by the respiratory syncytial virus nucleoprotein and compatible with weak interactions required for the processivity of the polymerase.
引用
收藏
页码:2120 / 2131
页数:12
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