P3N-PIPO Interacts with P3 via the Shared N-Terminal Domain To Recruit Viral Replication Vesicles for Cell-to-Cell Movement

Chai, Mengzhu; Wu, Xiaoyun; Liu, Jiahui; Fang, Yue; Luan, Yameng; Cui, Xiaoyan; Zhou, Xueping; Wang, Aiming; Cheng, Xiaofei

doi:10.1128/jvi.01898-19

Cited by 51 publications

(48 citation statements)

References 56 publications

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“…At 1 dpi, co-expression of P3[UK1]-GFP together with 6K2[UK1]-ChFP revealed the joint perinuclear presence of both proteins and chloroplasts (Figure 8a-d (Figure 8i-p, Videos S15 and S16). 6K2 forms chloroplast-interacting ER-derived vesicles (Wei et al, 2010(Wei et al, , 2013Grangeon et al, 2012;Cui et al, 2017), and UK 1 P3 is present in these membranous structures, as described for TEV and TuMV by other authors (Cui et al, 2010(Cui et al, , 2017Chai et al, 2020), but the behaviour of JPN 1 P3 in relation to its 6K2 partner has not been previously described.…”

Section: Transiently Expressed Fluorescent Tumv P3 Co-expressed Witmentioning

confidence: 83%

“…P3 may or may not play a role in the formation of the VRC, but it would be its carrier, although at different rates depending on viral strains. Very recently a model for the role of TuMV P3 protein in the viral cell-to-cell movement has been proposed (Chai et al, 2020).…”

Section: Discussionmentioning

confidence: 99%

“…It was also proposed to interact with itself (Choi et al, 2000) and with no other viral protein (Kang et al, 2004). Very recently, the interaction of P3 with the fusion protein P3N-PIPO has been shown for TuMV (Chai et al, 2020).…”

Section: Introductionmentioning

confidence: 99%

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Association between flower stalk elongation, anArabidopsisdevelopmental trait, and the subcellular location and movement dynamics of the nonstructural protein P3 ofTurnip mosaic virus

López‐González

Navarro

Pacios

et al. 2020

Molecular Plant Pathology

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Virus infections affect plant developmental traits but this aspect of the interaction has not been extensively studied so far. Two strains of Turnip mosaic virus differentially affect Arabidopsis development, especially flower stalk elongation, which allowed phenotypical, cellular, and molecular characterization of the viral determinant, the P3 protein. Transiently expressed wild‐type green fluorescent protein‐tagged P3 proteins of both strains and selected mutants of them revealed important differences in their behaviour as endoplasmic reticulum (ER)‐associated peripheral proteins flowing along the reticulum, forming punctate accumulations. Three‐dimensional (3D) model structures of all expressed P3 proteins were computationally constructed through I‐TASSER protein structure predictions, which were used to compute protein surfaces and map electrostatic potentials to characterize the effect of amino acid changes on features related to protein interactions and to phenotypical and subcellular results. The amino acid at position 279 was the main determinant affecting stalk development. It also determined the speed of ER‐flow of the expressed proteins and their final location. A marked change in the protein surface electrostatic potential correlated with changes in subcellular location. One single amino acid in the P3 viral protein determines all the analysed differential characteristics between strains differentially affecting flower stalk development. A model proposing a role of the protein in the intracellular movement of the viral replication complex, in association with the viral 6K2 protein, is proposed. The type of association between both viral proteins could differ between the strains.

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Section: Transiently Expressed Fluorescent Tumv P3 Co-expressed Witmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

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Association between flower stalk elongation, anArabidopsisdevelopmental trait, and the subcellular location and movement dynamics of the nonstructural protein P3 ofTurnip mosaic virus

López‐González

Navarro

Pacios

et al. 2020

Molecular Plant Pathology

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“…During infection, RNA viruses re-organize cell membranes into ‘viral factories’ that are intracellular virus-specific compartments serving as sites of virus replication. These virus replication compartments (VRCs) contain viral RNA as well as virus and host proteins involved in genomic RNA replication [66] – [72] . In potyviruses, almost all virus polypeptides forming VRCs are involved in intercellular RNA genome movement as well.…”

Section: Potyvirusesmentioning

confidence: 99%

“…In potyviruses, a small viral membrane protein 6K2 is involved in the local spatial re-arrangement of the ER membrane and the formation of vesicular VRC at the ER exit sites [59] , [65] , [73] – [76] . Several other viral proteins including CI (replicative SF2 RNA helicase), 6K1, 6K2, NIa, HC-Pro, P3, and P3N-PIPO have been shown to be functional protein elements of VRC in addition to NIb [65] , [72] , [77] , [78] . The VRC with incorporated viral CP may work as the motile vesicles moving along actin filaments and involved in virus replication, the genome intercellular movement and localization on chloroplasts [42] , [65] , [76] , [79] , [80] .…”

Section: Potyvirusesmentioning

confidence: 99%

Small hydrophobic viral proteins involved in intercellular movement of diverse plant virus genomes

Morozov

Solovyev

2020

AIMS Microbiology

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Most plant viruses code for movement proteins (MPs) targeting plasmodesmata to enable cell-to-cell and systemic spread in infected plants. Small membrane-embedded MPs have been first identified in two viral transport gene modules, triple gene block (TGB) coding for an RNA-binding helicase TGB1 and two small hydrophobic proteins TGB2 and TGB3 and double gene block (DGB) encoding two small polypeptides representing an RNA-binding protein and a membrane protein. These findings indicated that movement gene modules composed of two or more cistrons may encode the nucleic acid-binding protein and at least one membrane-bound movement protein. The same rule was revealed for small DNA-containing plant viruses, namely, viruses belonging to genus Mastrevirus (family Geminiviridae ) and the family Nanoviridae . In multi-component transport modules the nucleic acid-binding MP can be viral capsid protein(s), as in RNA-containing viruses of the families Closteroviridae and Potyviridae . However, membrane proteins are always found among MPs of these multicomponent viral transport systems. Moreover, it was found that small membrane MPs encoded by many viruses can be involved in coupling viral replication and cell-to-cell movement. Currently, the studies of evolutionary origin and functioning of small membrane MPs is regarded as an important pre-requisite for understanding of the evolution of the existing plant virus transport systems. This paper represents the first comprehensive review which describes the whole diversity of small membrane MPs and presents the current views on their role in plant virus movement.

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Innovative Arylimidazole‐Fused Phytovirucides via Carbene‐Catalyzed [3+4] Cycloaddition: Locking Viral Cell‐To‐Cell Movement by Out‐Competing Virus Capsid‐Host Interactions

Wei,

Zhao,

et al. 2024

Advanced Science

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The control of potato virus Y (PVY) induced crop failure is a challengeable issue in agricultural chemistry. Although many anti‐PVY agents are designed to focus on the functionally important coat protein (CP) of virus, how these drugs act on CP to inactivate viral pathogenicity, remains largely unknown. Herein, a PVY CP inhibitor ‐3j (S) is disclosed, which is accessed by developing unusually efficient (up to 99% yield) and chemo‐selective (> 99:1 er in most cases) carbene‐catalyzed [3+4] cycloaddition reactions. Compound ‐3j bears a unique arylimidazole‐fused diazepine skeleton and shows chirality‐preferred performance against PVY. In addition, ‐3j (S) as a mediator allows ARG191 (R191) of CP to be identified as a key amino acid site responsible for intercellular movement of virions. R191 is further demonstrated to be critical for the interaction between PVY CP and the plant functional protein NtCPIP, enabling virions to cross plasmodesmata. This key step can be significantly inhibited through bonding with the ‐3j (S) to further impair pathogenic behaviors involving systemic infection and particle assembly. The study reveals the in‐depth mechanism of action of antiviral agents targeting PVY CP, and contributes to new drug structures and synthetic strategies for PVY management.

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P3N-PIPO Interacts with P3 via the Shared N-Terminal Domain To Recruit Viral Replication Vesicles for Cell-to-Cell Movement

Cited by 51 publications

References 56 publications

Association between flower stalk elongation, anArabidopsisdevelopmental trait, and the subcellular location and movement dynamics of the nonstructural protein P3 ofTurnip mosaic virus

Association between flower stalk elongation, anArabidopsisdevelopmental trait, and the subcellular location and movement dynamics of the nonstructural protein P3 ofTurnip mosaic virus

Small hydrophobic viral proteins involved in intercellular movement of diverse plant virus genomes

Innovative Arylimidazole‐Fused Phytovirucides via Carbene‐Catalyzed [3+4] Cycloaddition: Locking Viral Cell‐To‐Cell Movement by Out‐Competing Virus Capsid‐Host Interactions

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