Extracellular Vesicles Deliver Host and Virus RNA and Regulate Innate Immune Response

Kouwaki, Takahisa; Okamoto, Masaaki; Tsukamoto, Hirotake; Fukushima, Yoshio; Oshiumi, Hiroyuki

doi:10.3390/ijms18030666

Cited by 93 publications

(78 citation statements)

References 84 publications

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“…In this scenario, PD might serve as an access point (‘hot spot’) for the secretory pathway to circumvent the physical limitations of the cell wall consisting of a narrow cellulose fibre meshwork (Somerville et al ., ). PD pores stretching across the cell wall would be a route enabling cells to exchange secretory vesicles/exosomes analogous to the mammalian extracellular vesicle/exosome signalling system delivering RNA to distant cells (Kouwaki et al ., ; Maas et al ., ). Given the overlap between the proteomes of plant exosome and PD, one could postulate that intercellularly delivered RNAs are transported via the ER‐related membranes spanning the PD pores or as independent vesicles/exosomes via the PD channel.…”

Section: Mode Of Rna Transportmentioning

confidence: 98%

Long distance RNA movement

Kehr¹,

2018

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Contents Summary29I.Introduction29II.Phloem as a conduit for macromolecules30III.Classes of phloem transported RNAs and their function32IV.Mode of RNA transport35V.Conclusions37Acknowledgements37References37 Summary In higher plants, small noncoding RNAs and large messenger RNA (mRNA) molecules are transported between cells and over long distances via the phloem. These large macromolecules are thought to get access to the sugar‐conducting phloem vessels via specialized plasmodesmata (PD). Analyses of the phloem exudate suggest that all classes of RNA molecules, including silencing‐induced RNAs (siRNAs), micro RNAs (miRNAs), transfer RNAs (tRNAs), ribosomal RNA (rRNAs) and mRNAs, are transported via the vasculature to distant tissues. Although the functions of mobile siRNAs and miRNAs as signalling molecules are well established, we lack a profound understanding of mobile mRNA function(s) in recipient cells and tissues, and how they are selected for transport. A surprisingly high number of up to thousands of mRNAs were described in diverse plant species such as cucumber, pumpkin, Arabidopsis and grapevine to move long distances over graft junctions to distinct body parts. In this review, we present an overview of the classes of mobile RNAs, the potential mechanisms facilitating RNA long‐distance transport, and the roles of mobile RNAs in regulating transcription and translation. Furthermore, we address potential function(s) of mobile protein‐encoding mRNAs with respect to their characteristics and evolutionary constraints.

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Section: Mode Of Rna Transportmentioning

confidence: 98%

Long distance RNA movement

Kehr¹,

2018

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“…During virus infection in animals, dendritic cells and macrophages internalize virus particles and/or extracellular vesicles containing viral RNA. The RNAs are then released into endosomes, where they are recognized by Toll-like receptors to induce immune responses (Baglio et al, 2016;Brencicova and Diebold, 2013;Dreux et al, 2012;Kouwaki et al, 2016Kouwaki et al, , 2017Kouwaki et al, , 2016Kouwaki et al, , 2017Okamoto et al, 2014). In analogy to the mammalian system, it is known that bacterial PAMP receptor-complexes in plants re-localize from the plasma membrane to endosomes (Avila et al, 2015;Beck et al, 2012;Frescatada-Rosa et al, 2015;Russinova et al, 2004) and that plant receptor proteins can signal from endosomes during immunity and development (Geldner et al, 2007;Irani et al, 2012;Mbengue et al, 2016;Sharfman et al, 2011).…”

Section: Endomembrane-associated Intracellular Perception Of Dsrnamentioning

confidence: 99%

Perception of double‐stranded RNA in plant antiviral immunity

Niehl

Heinlein

2019

Molecular Plant Pathology

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Summary RNA silencing and antiviral pattern‐triggered immunity (PTI) both rely on recognition of double‐stranded (ds)RNAs as defence‐inducing signals. While dsRNA recognition by dicer‐like proteins during antiviral RNA silencing is thoroughly investigated, the molecular mechanisms involved in dsRNA perception leading to antiviral PTI are just about to be untangled. Parallels to antimicrobial PTI thereby only partially facilitate our view on antiviral PTI. PTI against microbial pathogens involves plasma membrane bound receptors; however, dsRNAs produced during virus infection occur intracellularly. Hence, how dsRNA may be perceived during this immune response is still an open question. In this short review, we describe recent discoveries in PTI signalling upon sensing of microbial patterns and endogenous ‘danger’ molecules with emphasis on immune signalling‐associated subcellular trafficking processes in plants. Based on these studies, we develop different scenarios how dsRNAs could be sensed during antiviral PTI.

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“…Li & Nagy, 2011;Nagy & Pogany, 2011;R. Y. Wang & Li, 2012) Host mRNA transcription shutoff CPSF4, PABPN1, POLR2 (Herbert & Nag, 2016) Splicing HNRNPA1, HNRNPA2B1, HNRNPA3, HNRNPH, HNRNPC, HNRNPM, U2AF1, U2AF2, SR proteins (Meyer, 2016;Stoltzfus & Madsen, 2006;Tazi et al, 2010) RNA editing/ reading of edited RNA ADAR, ADARB1, ADARB2, RBM15, ALKBH5, YTHDF1, YTHDF3 (Gonzales-van Horn & Sarnow, 2017;Samuel, 2011) Nucleus-cytoplasm shuttling PTBP1, PCBP2, SSB, CSDE1, HNRNPC, HNRNPA1, HNRNPK, HNRNPM, DHX9, SYNCRIP, TIA1, TIAL1, G3BP1 (Lloyd, 2015) vRNA export from nucleus NXF1, ALYREF, RAN, SR proteins, DDX1, DDX3X, DDX5, HNRNPA2B1, SFPQ, MATR3 (Kuss, Mata, Zhang, & Fontoura, 2013;Stake, Bann, Kaddis, & Parent, 2013) vRNA trafficking and packaging HNRNPA2B1, EEF1A1, STAU1 (Cochrane, McNally, & Mouland, 2006;Kaddis Maldonado & Parent, 2016;Stake et al, 2013) Extracellular trafficking HNRNPA2B1, AGO2, SYNCRIP, YBX1 (Kouwaki, Okamoto, Tsukamoto, Fukushima, & Oshiumi, 2017) vRNA stability ELAVL1, PCBP2, HNRNPD, YBX1, ILF3 (Dickson & Wilusz, 2011;Moon & Wilusz, 2013) 5 0 !3 0 RNA degradation XRN1, PATL1, XRN2 (Molleston & Cherry, 2017;Moon, Barnhart, & Wilusz, 2012;Narayanan & Makino, 2013;Oshiumi, Mifsud, et al, 2016;Rigby & Rehwinkel, 2015) 3 0 !5 0 RNA degradation DDX17, ZC3HAV1, UPF1, UPF3, RRP6 (Molleston & Cherry, 2017;Moon, Barnhart, & Wilusz, 2012;Narayanan & Makino, 2013;Oshiumi, Mifsud, et al, 2016;Rigby & Rehwinkel, 2015) Translation PABPC1, EIF4E, EIF4G, EIF4A, EIF2, EIF3, ribosomal proteins, EIF5B, EEF1A1, EEF2, ETF1 (McCormick & Khaperskyy, 2017;Smith & Gray, 2010;Walsh & Mohr, 2011) RNP granules G3BP1, G3BP2, EIF2AK2, LSM14A, XR...…”

Section: Well-known Rbps Meet Virusesmentioning

confidence: 99%

Unconventional RNA‐binding proteins step into the virus–host battlefront

2018

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The crucial participation of cellular RNA-binding proteins (RBPs) in virtually all steps of virus infection has been known for decades. However, most of the studies characterizing this phenomenon have focused on well-established RBPs harboring classical RNA-binding domains (RBDs). Recent proteome-wide approaches have greatly expanded the census of RBPs, discovering hundreds of proteins that interact with RNA through unconventional RBDs. These domains include protein-protein interaction platforms, enzymatic cores, and intrinsically disordered regions. Here, we compared the experimentally determined census of RBPs to gene ontology terms and literature, finding that 472 proteins have previous links with viruses. We discuss what these proteins are and what their roles in infection might be. We also review some of the pioneering examples of unorthodox RBPs whose RNA-binding activity has been shown to be critical for virus infection. Finally, we highlight the potential of these proteins for host-based therapies against viruses. This article is categorized under: RNA Interactions with Proteins and Other Molecules > Protein-RNA Interactions: Functional Implications RNA in Disease and Development > RNA in Disease RNA Interactions with Proteins and Other Molecules > RNA-Protein Complexes.

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Extracellular Vesicles Deliver Host and Virus RNA and Regulate Innate Immune Response

Cited by 93 publications

References 84 publications

Long distance RNA movement

Long distance RNA movement

Perception of double‐stranded RNA in plant antiviral immunity

Unconventional RNA‐binding proteins step into the virus–host battlefront

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