Literature DB >> 8325506

Role of protein conformation in the processing of dengue virus type 2 nonstructural polyprotein precursor.

L Zhang1, R Padmanabhan.   

Abstract

The dengue virus type-2 (DEN-2) genome is a positive-strand RNA encoding a single polyprotein precursor, C-prM(M)-E-NS1-NS2A-NS2B-NS3-NS4A-NS4B- NS5, consisting of 3391 amino acids (aa). The N-terminal region of the polyprotein precursor, C-prM(M)-E, encodes the structural proteins and is processed cotranslationally by the host signal peptidase. The nonstructural region NS1-->NS5 is processed by the viral protease(s), as well as by the signal peptidase. A two-component viral protease consisting of NS2B and the serine protease domain of NS3 has been shown to be required for cleavages having the consensus sequence of dibasic aa (K-R, R-R, R-K, or Q-R). In this study, the region encoding all the nonstructural proteins, NS1-->NS5, was expressed using a recombinant vaccinia virus system. Cleavages at the consensus viral protease recognition sites, 2B-3 at the N terminus and 3-4A at the C terminus, are prerequisites to the release of mature NS3 protease. Although the 2B-3 site was cleaved readily in a variety of polyprotein precursors containing the intact NS2B and the NS3 protease domain, the 3-4A site was most efficiently cleaved, similar to that found in DEN-2-infected cells, only in the polyprotein precursor encoding the entire nonstructural region. Removal of NS1 at the N terminus or of NS5 coding sequences at the C terminus affected the cleavage at the 3-4A site to produce the processing intermediate, NS3-NS4A. These results indicate that the conformation of the nonstructural polyprotein precursor, NS1-->NS5, plays a major role in the efficient cleavage at the 3-4A site.

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Year:  1993        PMID: 8325506     DOI: 10.1016/0378-1119(93)90269-9

Source DB:  PubMed          Journal:  Gene        ISSN: 0378-1119            Impact factor:   3.688


  9 in total

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Review 2.  Elucidating the role of T cells in protection against and pathogenesis of dengue virus infections.

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4.  The serine protease and RNA-stimulated nucleoside triphosphatase and RNA helicase functional domains of dengue virus type 2 NS3 converge within a region of 20 amino acids.

Authors:  H Li; S Clum; S You; K E Ebner; R Padmanabhan
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5.  Dengue Protease Substrate Recognition: Binding of the Prime Side.

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7.  NS4A regulates the ATPase activity of the NS3 helicase: a novel cofactor role of the non-structural protein NS4A from West Nile virus.

Authors:  Sergey A Shiryaev; Andrei V Chernov; Alexander E Aleshin; Tatiana N Shiryaeva; Alex Y Strongin
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Review 8.  Structure and functionality in flavivirus NS-proteins: perspectives for drug design.

Authors:  Michela Bollati; Karin Alvarez; René Assenberg; Cécile Baronti; Bruno Canard; Shelley Cook; Bruno Coutard; Etienne Decroly; Xavier de Lamballerie; Ernest A Gould; Gilda Grard; Jonathan M Grimes; Rolf Hilgenfeld; Anna M Jansson; Hélène Malet; Erika J Mancini; Eloise Mastrangelo; Andrea Mattevi; Mario Milani; Grégory Moureau; Johan Neyts; Raymond J Owens; Jingshan Ren; Barbara Selisko; Silvia Speroni; Holger Steuber; David I Stuart; Torsten Unge; Martino Bolognesi
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9.  Targeting intramolecular proteinase NS2B/3 cleavages for trans-dominant inhibition of dengue virus.

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  9 in total

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