Your search keyword '"Satellite Viruses metabolism"' showing total 56 results

1. Ethylene response transcription factor 5 (ERF5) enhances defense against tobacco curly shoot virus and associated betasatellite (TbCSV/TbCSB) in Nicotiana benthamiana.

Author

Zhao M, Zhang L, Ghanem H, Wu G, Li M, and Qing L

Subjects

Gene Expression Regulation, Plant, Phylogeny, Satellite Viruses genetics, Satellite Viruses metabolism, DNA, Satellite genetics, DNA, Satellite metabolism, Nicotiana virology, Nicotiana genetics, Nicotiana metabolism, Begomovirus genetics, Plant Diseases virology, Plant Diseases genetics, Plant Proteins genetics, Plant Proteins metabolism, Transcription Factors metabolism, Transcription Factors genetics

Abstract

Begomovirus/betasatellite disease complex significantly threatens global crop production. Identifying potential plant antiviral genes is crucial for disease control. Nicotiana benthamiana is susceptible to viruses and contains 266 ethylene response transcription factors (ERFs). This study identified 29 NbERFs that were differentially upregulated in tobacco curly shoot virus and its associated betasatellite (TbCSV/TbCSB) infection, with ERF5 being the most common. Nine NbERF5s cluster phylogenetically and Niben101Scf00163g22002 (NbERF5) responds significantly to exogenous ACC treatment. Further analysis confirms the nuclear localization and transcriptional activation activity of NbERF5. Protein interaction assays demonstrate that NbERF5 has no self-interaction and does not interact with the βC1 protein of TbCSB. Silencing NbERF5 enhances TbCSV/TbCSB infection, and overexpression of NbERF5 inhibits TbCSV/TbCSB infection. Importantly, NbERF5 positively regulates the expression of the pathogenesis-related (PR) genes, NbPR1a and NbNPR1. Our findings suggest that NbERF5 enhances TbCSV/TbCSB resistance by activating the PR genes, indicating that NbERF5 is a potential antiviral gene., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Inc.)

Published

2025

2. Locally Directed Recombinant Adeno- Associated Virus-Mediated IGF-1 Gene Therapy Enhances Osteochondral Repair and Counteracts Early Osteoarthritis In Vivo.

Author

Peifer C, Oláh T, Venkatesan JK, Goebel L, Orth P, Schmitt G, Zurakowski D, Menger MD, Laschke MW, Cucchiarini M, and Madry H

Subjects

Animals, Dependovirus genetics, Genetic Therapy, Satellite Viruses genetics, Satellite Viruses metabolism, Sheep genetics, X-Ray Microtomography, Cartilage, Articular drug effects, Cartilage, Articular pathology, Insulin-Like Growth Factor I genetics, Insulin-Like Growth Factor I therapeutic use, Osteoarthritis genetics, Osteoarthritis therapy, Osteoarthritis metabolism

Abstract

Background: Restoration of osteochondral defects is critical, because osteoarthritis (OA) can arise., Hypothesis: Overexpression of insulin-like growth factor 1 (IGF-1) via recombinant adeno-associated viral (rAAV) vectors (rAAV-IGF-1) would improve osteochondral repair and reduce parameters of early perifocal OA in sheep after 6 months in vivo., Study Design: Controlled laboratory study., Methods: Osteochondral defects were created in the femoral trochlea of adult sheep and treated with rAAV-IGF-1 or rAAV- lacZ (control) (24 defects in 6 knees per group). After 6 months in vivo, osteochondral repair and perifocal OA were assessed by well-established macroscopic, histological, and immunohistochemical scoring systems as well as biochemical and micro-computed tomography evaluations., Results: Application of rAAV-IGF-1 led to prolonged (6 months) IGF-1 overexpression without adverse effects, maintaining a significantly superior overall cartilage repair, together with significantly improved defect filling, extracellular matrix staining, cellular morphology, and surface architecture compared with rAAV- lacZ . Expression of type II collagen significantly increased and that of type I collagen significantly decreased. Subchondral bone repair and tidemark formation were significantly improved, and subchondral bone plate thickness and subarticular spongiosa mineral density returned to normal. The OA parameters of perifocal structure, cell cloning, and matrix staining were significantly better preserved upon rAAV-IGF-1 compared with rAAV- lacZ . Novel mechanistic associations between parameters of osteochondral repair and OA were identified., Conclusion: Local rAAV-mediated IGF-1 overexpression enhanced osteochondral repair and ameliorated parameters of perifocal early OA., Clinical Relevance: IGF-1 gene therapy may be beneficial in repair of focal osteochondral defects and prevention of perifocal OA., Competing Interests: One or more of the authors has declared the following potential conflict of interest or source of funding: This work was funded by Deutsche Arthrose-Hilfe e.V. P229-A15-Madry-EP1-madr7-allgemein-pr-I-226k-2010-14 (M.C., H.M.). AOSSM checks author disclosures against the Open Payments Database (OPD). AOSSM has not conducted an independent investigation on the OPD and disclaims any liability or responsibility relating thereto.

Published

2024

3. Functional Characterization of Replication-Associated Proteins Encoded by Alphasatellites Identified in Yunnan Province, China.

Author

Zhao L, Che X, Wang Z, Zhou X, and Xie Y

Subjects

Amino Acid Sequence, Begomovirus chemistry, Begomovirus genetics, China, Plants, Genetically Modified genetics, Plants, Genetically Modified virology, Satellite Viruses chemistry, Satellite Viruses genetics, Sequence Alignment, Nicotiana genetics, Nicotiana virology, Viral Proteins chemistry, Viral Proteins genetics, Begomovirus metabolism, Plant Diseases virology, Satellite Viruses metabolism, Viral Proteins metabolism

Abstract

Alphasatellites, which encode only a replication-associated protein (alpha-Rep), are frequently found to be non-essential satellite components associated with begomovirus/betasatellite complexes, and their presence can modulate disease symptoms and/or viral DNA accumulation during infection. Our previous study has shown that there are three types of alphasatellites associated with begomovirus/betasatellite complexes in Yunnan province in China and they encode three corresponding types of alpha-Rep proteins. However, the biological functions of alpha-Reps remain poorly understood. In this study, we investigated the biological functions of alpha-Reps in post-transcriptional gene silencing (PTGS) and transcriptional gene silencing (TGS) using 16c and 16-TGS transgenic Nicotiana benthamiana plants. Results showed that all the three types of alpha-Rep proteins were capable of suppressing the PTGS and reversing the TGS. Among them, the alpha-Rep of Y10DNA1 has the strongest PTGS and TGS suppressor activities. We also found that the alpha-Rep proteins were able to increase the accumulation of their helper virus during coinfection. These results suggest that the alpha-Reps may have a role in overcoming host defense, which provides a possible explanation for the selective advantage provided by the association of alphasatellites with begomovirus/betasatellite complexes.

Published

2022

4. Structure of the Capsid Size-Determining Scaffold of "Satellite" Bacteriophage P4.

Author

Kizziah JL, Rodenburg CM, and Dokland T

Subjects

Bacteriophages genetics, Bacteriophages metabolism, Capsid metabolism, Capsid Proteins genetics, Capsid Proteins metabolism, Helper Viruses chemistry, Helper Viruses genetics, Helper Viruses metabolism, Mutation, Protein Conformation, Satellite Viruses chemistry, Satellite Viruses genetics, Satellite Viruses metabolism, Bacteriophages chemistry, Capsid chemistry, Capsid Proteins chemistry

Abstract

P4 is a mobile genetic element (MGE) that can exist as a plasmid or integrated into its Escherichia coli host genome, but becomes packaged into phage particles by a helper bacteriophage, such as P2. P4 is the original example of what we have termed "molecular piracy", the process by which one MGE usurps the life cycle of another for its own propagation. The P2 helper provides most of the structural gene products for assembly of the P4 virion. However, when P4 is mobilized by P2, the resulting capsids are smaller than those normally formed by P2 alone. The P4-encoded protein responsible for this size change is called Sid, which forms an external scaffolding cage around the P4 procapsids. We have determined the high-resolution structure of P4 procapsids, allowing us to build an atomic model for Sid as well as the gpN capsid protein. Sixty copies of Sid form an intertwined dodecahedral cage around the T = 4 procapsid, making contact with only one out of the four symmetrically non-equivalent copies of gpN. Our structure provides a basis for understanding the sir mutants in gpN that prevent small capsid formation, as well as the nms "super-sid" mutations that counteract the effect of the sir mutations, and suggests a model for capsid size redirection by Sid.

Published

2020

5. Innate immune recognition and modulation in hepatitis D virus infection.

Author

Jung S, Altstetter SM, and Protzer U

Subjects

Carcinoma, Hepatocellular immunology, Carcinoma, Hepatocellular pathology, Carcinoma, Hepatocellular virology, Coinfection complications, Coinfection pathology, Coinfection virology, Hepatitis B virus genetics, Hepatitis B virus metabolism, Hepatitis B, Chronic complications, Hepatitis B, Chronic pathology, Hepatitis B, Chronic virology, Hepatitis D, Chronic complications, Hepatitis D, Chronic pathology, Hepatitis D, Chronic virology, Hepatitis Delta Virus genetics, Hepatitis Delta Virus metabolism, Hepatitis delta Antigens immunology, Hepatitis delta Antigens metabolism, Humans, Immunity, Innate, Interferon-Induced Helicase, IFIH1 metabolism, Liver immunology, Liver pathology, Liver virology, Liver Cirrhosis immunology, Liver Cirrhosis pathology, Liver Cirrhosis virology, Liver Neoplasms immunology, Liver Neoplasms pathology, Liver Neoplasms virology, Organic Anion Transporters, Sodium-Dependent metabolism, RNA, Viral immunology, RNA, Viral metabolism, Receptors, Pattern Recognition immunology, Receptors, Pattern Recognition metabolism, Satellite Viruses genetics, Satellite Viruses immunology, Satellite Viruses metabolism, Symporters metabolism, Virus Replication immunology, Coinfection immunology, Hepatitis B virus immunology, Hepatitis B, Chronic immunology, Hepatitis D, Chronic immunology, Hepatitis Delta Virus immunology, Immune Evasion

Abstract

Hepatitis D virus (HDV) is a global health threat with more than 15 million humans affected. Current treatment options are largely unsatisfactory leaving chronically infected humans at high risk to develop liver cirrhosis and hepatocellular carcinoma. HDV is the only human satellite virus known. It encodes only two proteins, and requires Hepatitis B virus (HBV) envelope protein expression for productive virion release and spread of the infection. How HDV could evolve and why HBV was selected as a helper virus remains unknown. Since the discovery of Na + -taurocholate co-transporting polypeptide as the essential uptake receptor for HBV and HDV, we are beginning to understand the interactions of HDV and the immune system. While HBV is mostly regarded a stealth virus, that escapes innate immune recognition, HBV-HDV coinfection is characterized by a strong innate immune response. Cytoplasmic RNA sensor melanoma differentiation antigen 5 has been reported to recognize HDV RNA replication and activate innate immunity. Innate immunity, however, seems not to impair HDV replication while it inhibits HBV. In this review, we describe what is known up-to-date about the interplay between HBV as a helper and HDV's immune evasion strategy and identify where additional research is required., Competing Interests: Conflict-of-interest statement: The authors declare no conflict of interests concerning the content of this article., (©The Author(s) 2020. Published by Baishideng Publishing Group Inc. All rights reserved.)

Published

2020

6. A neo-virus lifestyle exhibited by a (+)ssRNA virus hosted in an unrelated dsRNA virus: Taxonomic and evolutionary considerations.

Author

Hisano S, Zhang R, Faruk MI, Kondo H, and Suzuki N

Subjects

Amino Acid Sequence, Capsid Proteins genetics, Capsid Proteins metabolism, Evolution, Molecular, Fungal Viruses classification, Fungal Viruses isolation & purification, Fungal Viruses metabolism, Gene Transfer, Horizontal, Microbial Interactions, RNA Viruses classification, RNA Viruses isolation & purification, RNA Viruses metabolism, RNA, Double-Stranded genetics, RNA, Double-Stranded metabolism, RNA, Viral metabolism, RNA-Dependent RNA Polymerase genetics, RNA-Dependent RNA Polymerase metabolism, Satellite Viruses classification, Satellite Viruses isolation & purification, Satellite Viruses metabolism, Sequence Alignment, Sequence Homology, Amino Acid, Virus Replication, Fungal Viruses genetics, Fungi virology, Phylogeny, RNA Viruses genetics, RNA, Viral genetics, Satellite Viruses genetics

Abstract

Recent studies illustrate that fungi as virus hosts provides a unique platform for hunting viruses and exploring virus/virus and virus/host interactions. Such studies have revealed a number of as-yet-unreported viruses and virus/virus interactions. Among them is a unique intimate relationship between a (+)ssRNA virus, yado-kari virus (YkV1) and an unrelated dsRNA virus, yado-nushi virus (YnV1). YkV1 dsRNA, a replicated form of YkV1, and RNA-dependent RNA polymerase, are trans-encapsidated by the capsid protein of YnV1. While YnV1 can complete its replication cycle, YkV1 relies on YnV1 for its viability. We previously proposed a model in which YkV1 diverts YnV1 capsids as the replication sites. YkV1 is neither satellite virus nor satellite RNA, because YkV1 appears to encode functional RdRp and enhances YnV1 accumulation. This represents a unique mutualistic virus/virus interplay and similar relations in other virus/host fungus systems are detectable. We propose to establish the family Yadokariviridae that accommodates YkV1 and recently discovered viruses phylogenetically related to YkV1. This article overviews what is known and unknown about the YkV1/YnV1 interactions. Also discussed are the YnV1 Phytoreo_S7 and YkV1 2A-like domains that may have been captured via horizontal transfer during the course of evolution and are conserved across extant diverse RNA viruses. Lastly, evolutionary scenarios are envisioned for YkV1 and YnV1., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

7. An Insight into Cotton Leaf Curl Multan Betasatellite, the Most Important Component of Cotton Leaf Curl Disease Complex.

Author

Zubair M, Zaidi SS, Shakir S, Amin I, and Mansoor S

Subjects

Autophagy, DNA, Satellite, DNA, Viral genetics, India, Pakistan, Phylogeny, Plant Diseases virology, Satellite Viruses metabolism, Sequence Analysis, DNA, Ubiquitination, Viral Proteins genetics, Viral Proteins metabolism, Begomovirus genetics, Genome, Viral, Gossypium virology, Host-Pathogen Interactions, Satellite Viruses genetics

Abstract

Cotton leaf curl disease (CLCuD) is one of the most economically important diseases and is a constraint to cotton production in major producers, Pakistan and India. CLCuD is caused by monopartite plant viruses belonging to the family Geminiviridae (genus Begomovirus ), in association with an essential, disease-specific satellite, Cotton leaf curl Multan betasatellite (CLCuMuB) belonging to a newly-established family Tolecusatellitidae (genus Betasatellite ). CLCuMuB has a small genome (ca. 1350 nt) with a satellite conserved region, an adenine-rich region and a single gene that encodes for a multifunctional βC1 protein. CLCuMuB βC1 protein has a major role in pathogenicity and symptom determination, and alters several host cellular functions like autophagy, ubiquitination, and suppression of gene silencing, to assist CLCuD infectivity. Efficient trans -replication ability of CLCuMuB with several monopartite and bipartite begomoviruses, is also associated with the rapid evolution and spread of CLCuMuB. In this article we comprehensively reviewed the role of CLCuMuB in CLCuD, focusing on the βC1 functions and its interactions with host proteins., Competing Interests: The authors declare no conflict of interest.

Published

2017

8. AAVP displaying octreotide for ligand-directed therapeutic transgene delivery in neuroendocrine tumors of the pancreas.

Author

Smith TL, Yuan Z, Cardó-Vila M, Sanchez Claros C, Adem A, Cui MH, Branch CA, Gelovani JG, Libutti SK, Sidman RL, Pasqualini R, and Arap W

Subjects

Animals, Female, Ligands, Male, Mice, Mice, Transgenic, Bacteriophages genetics, Dependovirus genetics, Dependovirus metabolism, Genetic Vectors, Neuroendocrine Tumors therapy, Octreotide administration & dosage, Pancreatic Neoplasms therapy, Satellite Viruses metabolism

Abstract

Patients with inoperable or unresectable pancreatic neuroendocrine tumors (NETs) have limited treatment options. These rare human tumors often express somatostatin receptors (SSTRs) and thus are clinically responsive to certain relatively stable somatostatin analogs, such as octreotide. Unfortunately, however, this tumor response is generally short-lived. Here we designed a hybrid adeno-associated virus and phage (AAVP) vector displaying biologically active octreotide on the viral surface for ligand-directed delivery, cell internalization, and transduction of an apoptosis-promoting tumor necrosis factor (TNF) transgene specifically to NETs. These functional attributes of AAVP-TNF particles displaying the octreotide peptide motif (termed Oct-AAVP-TNF) were confirmed in vitro, in SSTR type 2-expressing NET cells, and in vivo using cohorts of pancreatic NET-bearing Men1 tumor-suppressor gene KO mice, a transgenic model of functioning (i.e., insulin-secreting) tumors that genetically and clinically recapitulates the human disease. Finally, preclinical imaging and therapeutic experiments with pancreatic NET-bearing mice demonstrated that Oct-AAVP-TNF lowered tumor metabolism and insulin secretion, reduced tumor size, and improved mouse survival. Taken together, these proof-of-concept results establish Oct-AAVP-TNF as a strong therapeutic candidate for patients with NETs of the pancreas. More broadly, the demonstration that a known, short, biologically active motif can direct tumor targeting and receptor-mediated internalization of AAVP particles may streamline the potential utility of myriad other short peptide motifs and provide a blueprint for therapeutic applications in a variety of cancers and perhaps many nonmalignant diseases as well.

Published

2016

9. Begomovirus-Associated Satellite DNA Diversity Captured Through Vector-Enabled Metagenomic (VEM) Surveys Using Whiteflies (Aleyrodidae).

Author

Rosario K, Marr C, Varsani A, Kraberger S, Stainton D, Moriones E, Polston JE, and Breitbart M

Subjects

Animals, Begomovirus metabolism, DNA, Satellite metabolism, DNA, Viral metabolism, Genetic Variation, Hemiptera classification, Metagenomics, Molecular Sequence Data, Phylogeny, Plant Diseases virology, Satellite Viruses metabolism, Begomovirus genetics, DNA, Satellite genetics, DNA, Viral genetics, Hemiptera virology, Insect Vectors virology, Satellite Viruses genetics

Abstract

Monopartite begomoviruses (Geminiviridae), which are whitefly-transmitted single-stranded DNA viruses known for causing devastating crop diseases, are often associated with satellite DNAs. Since begomovirus acquisition or exchange of satellite DNAs may lead to adaptation to new plant hosts and emergence of new disease complexes, it is important to investigate the diversity and distribution of these molecules. This study reports begomovirus-associated satellite DNAs identified during a vector-enabled metagenomic (VEM) survey of begomoviruses using whiteflies collected in various locations (California (USA), Guatemala, Israel, Puerto Rico, and Spain). Protein-encoding satellite DNAs, including alphasatellites and betasatellites, were identified in Israel, Puerto Rico, and Guatemala. Novel alphasatellites were detected in samples from Guatemala and Puerto Rico, resulting in the description of a phylogenetic clade (DNA-3-type alphasatellites) dominated by New World sequences. In addition, a diversity of small (~640-750 nucleotides) satellite DNAs similar to satellites associated with begomoviruses infecting Ipomoea spp. were detected in Puerto Rico and Spain. A third class of satellite molecules, named gammasatellites, is proposed to encompass the increasing number of reported small (<1 kilobase), non-coding begomovirus-associated satellite DNAs. This VEM-based survey indicates that, although recently recovered begomovirus genomes are variations of known genetic themes, satellite DNAs hold unexplored genetic diversity.

Published

2016

10. Three gene products of a begomovirus-betasatellite complex restore expression of a transcriptionally silenced green fluorescent protein transgene in Nicotiana benthamiana.

Author

Saeed M, Krczal G, and Wassenegger M

Subjects

Begomovirus genetics, Green Fluorescent Proteins metabolism, Plant Diseases genetics, Plant Diseases virology, Plants, Genetically Modified metabolism, Plants, Genetically Modified virology, Potexvirus genetics, Potexvirus metabolism, Satellite Viruses genetics, Nicotiana metabolism, Nicotiana virology, Trans-Activators genetics, Transcriptional Activation, Viral Proteins genetics, Begomovirus metabolism, Gene Silencing, Green Fluorescent Proteins genetics, Plants, Genetically Modified genetics, Satellite Viruses metabolism, Nicotiana genetics, Trans-Activators metabolism, Viral Proteins metabolism

Abstract

Single-stranded DNA geminiviruses replicate via double-stranded DNA intermediates forming mini-chromosomes that are targets for transcriptional gene silencing (TGS) in plants. The ability of the cotton leaf curl Kokhran virus (CLCuKoV)-cotton leaf curl Multan betasatellite (CLCuMuB) proteins, replication-associated protein (Rep), transcriptional activator protein (TrAP), C4, V2 and βC1, to suppress TGS was investigated by using the Nicotiana benthamiana line 16-TGS (16-TGS) harbouring a transcriptionally silenced green fluorescent protein (GFP) transgene. Inoculation of 16-TGS plants with a recombinant potato virus X vector carrying Rep, TrAP or βC1 resulted in re-expression of GFP. Northern blot analysis confirmed that the observed GFP fluorescence was associated with GFP mRNA accumulation. These results indicated that Rep, TrAP and βC1 proteins of CLCuKoV-CLCuMuB can re-activate the expression of a transcriptionally silenced GFP transgene in N. benthamiana. Although Rep, TrAP, or βC1 proteins have, for other begomoviruses or begomoviruses-betasatellites, been previously shown to have TGS suppressor activity, this is the first report demonstrating that a single begomovirus-betasatellite complex encodes three suppressors of TGS.

Published

2015

11. Virus-induced gene silencing using a modified betasatellite: a potential candidate for functional genomics of crops.

Author

Kumar J, Gunapati S, Kumar J, Kumari A, Kumar A, Tuli R, and Singh SP

Subjects

Begomovirus genetics, Crops, Agricultural genetics, Crops, Agricultural virology, Genetic Vectors metabolism, Gossypium virology, Solanum lycopersicum virology, Plant Diseases virology, Satellite Viruses metabolism, Nicotiana virology, Gene Silencing, Genetic Vectors genetics, Gossypium genetics, Solanum lycopersicum genetics, Plant Diseases genetics, Satellite Viruses genetics, Nicotiana genetics

Abstract

Betasatellites are geminivirus-associated single-stranded DNA molecules that play an important role in symptom modulation. A VIGS vector was developed by modifying cotton leaf curl Multan betasatellite (CLCuMB). CLCuMB DNA was modified by replacing the βC1 gene with a multiple cloning site. The silencing ability of the modified CLCuMB was investigated by cloning a fragment of a host gene (Su) or a reporter transgene (uidA) into the modified CLCuMB and co-agroinoculation with cotton leaf curl Multan virus, cotton leaf curl Kokhran virus, and ageratum enation virus, separately. The inoculated Nicotiana tabacum, N. benthamiana, Solanum lycopersicum, Arabidopsis thaliana and Gossypium hirsutum plants showed efficient silencing of the cognate genes.

Published

2014

12. Effects of the virus satellite gene βC1 on host plant defense signaling and volatile emission.

Author

Salvaudon L, De Moraes CM, Yang JY, Chua NH, and Mescher MC

Subjects

Acyclic Monoterpenes, Animals, Arabidopsis metabolism, Arabidopsis virology, Gene Expression Regulation, Plant, Herbivory, Solanum lycopersicum genetics, Solanum lycopersicum metabolism, Solanum lycopersicum virology, Monoterpenes metabolism, Plant Diseases genetics, Plant Diseases virology, Plants, Genetically Modified, Satellite Viruses genetics, Satellite Viruses metabolism, Signal Transduction, Nicotiana metabolism, Nicotiana virology, Arabidopsis genetics, Cyclopentanes metabolism, Disease Resistance genetics, Genes, Viral, Hemiptera, Oils, Volatile metabolism, Oxylipins metabolism, Nicotiana genetics

Abstract

Tomato Yellow Leaf Curl China virus spreads together with its invasive vector, the silverleaf whitefly B biotype, which exhibits higher growth rates on infected plants. Previous studies indicate that the virus satellite gene βC1 accounts for the visible symptoms of infection and inhibits the constitutive expression of jasmonic acid (JA)--a phytohormone involved in plant defense against whiteflies--and of some JA-regulated genes. Here we present new details of the effects of on plant signaling and defense, obtained with (non-host) transgenic Arabidopsis thaliana and Nicotiana benthamiana plants. We found that JA induction in response to wounding was reduced in plants expressing βC1. This result implies that βC1 acts on conserved plant regulation mechanisms and might impair the entire JA defense pathway. Furthermore, transformed N. benthamiana plants exhibited elevated emissions of the volatile compound linalool, suggesting that βC1 also influences plant-derived olfactory cues available to vector and non-vector insects.

Published

2013

13. Silencing suppressor activity of a begomovirus DNA β encoded protein and its effect on heterologous helper virus replication.

Author

Eini O, Dogra SC, Dry IB, and Randles JW

Subjects

Begomovirus genetics, DNA, Viral genetics, Helper Viruses genetics, Plant Diseases virology, Satellite Viruses genetics, Nicotiana genetics, Nicotiana virology, Viral Proteins genetics, Begomovirus metabolism, DNA, Viral metabolism, Helper Viruses physiology, Plant Diseases genetics, RNA Interference, Satellite Viruses metabolism, Viral Proteins metabolism, Virus Replication

Abstract

DNA β satellites are circular single-stranded molecules associated with some monopartite begomoviruses in the family Geminiviridae. They co-infect with their helper viruses to induce severe disease in economically important crops. The βC1 protein encoded by DNA β is a pathogenicity determinant and has been reported to suppress post-transcriptional gene silencing (PTGS). The βC1 proteins from various DNA β molecules show low levels of amino acid sequence conservation. We show here that the βC1 from DNA β associated with Cotton leaf curl Multan virus (CLCuMV) is a suppressor of systemic PTGS. When this DNA β satellite co-inoculated with a heterologous helper virus, Tomato leaf curl virus (ToLCV), reduced the level of ToLCV siRNA and this was associated with a higher level of virus accumulation in infected tobacco plants. This may be a mechanism by which βC1 protects a heterologous virus from host gene silencing., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

14. Tomato SlSnRK1 protein interacts with and phosphorylates βC1, a pathogenesis protein encoded by a geminivirus β-satellite.

Author

Shen Q, Liu Z, Song F, Xie Q, Hanley-Bowdoin L, and Zhou X

Subjects

DNA, Viral metabolism, Geminiviridae metabolism, Gene Expression Regulation, Plant, Solanum lycopersicum genetics, Mutation genetics, Phosphorylation, Phosphoserine metabolism, Phosphothreonine metabolism, Plant Diseases virology, Plant Proteins chemistry, Plant Proteins genetics, Plant Proteins metabolism, Protein Binding, Protein Interaction Domains and Motifs, Satellite Viruses metabolism, Subcellular Fractions metabolism, Viral Proteins chemistry, Geminiviridae pathogenicity, Solanum lycopersicum enzymology, Solanum lycopersicum virology, Satellite Viruses pathogenicity, Viral Proteins metabolism

Abstract

The βC1 protein of tomato yellow leaf curl China β-satellite functions as a pathogenicity determinant. To better understand the molecular basis of βC1 in pathogenicity, a yeast two-hybrid screen of a tomato (Solanum lycopersicum) cDNA library was carried out using βC1 as bait. βC1 interacted with a tomato SUCROSE-NONFERMENTING1-related kinase designated as SlSnRK1. Their interaction was confirmed using a bimolecular fluorescence complementation assay in Nicotiana benthamiana cells. Plants overexpressing SnRK1 were delayed for symptom appearance and contained lower levels of viral and satellite DNA, while plants silenced for SnRK1 expression developed symptoms earlier and accumulated higher levels of viral DNA. In vitro kinase assays showed that βC1 is phosphorylated by SlSnRK1 mainly on serine at position 33 and threonine at position 78. Plants infected with βC1 mutants containing phosphorylation-mimic aspartate residues in place of serine-33 and/or threonine-78 displayed delayed and attenuated symptoms and accumulated lower levels of viral DNA, while plants infected with phosphorylation-negative alanine mutants contained higher levels of viral DNA. These results suggested that the SlSnRK1 protein attenuates geminivirus infection by interacting with and phosphorylating the βC1 protein.

Published

2011

15. Suppression of methylation-mediated transcriptional gene silencing by βC1-SAHH protein interaction during geminivirus-betasatellite infection.

Author

Yang X, Xie Y, Raja P, Li S, Wolf JN, Shen Q, Bisaro DM, and Zhou X

Subjects

Adenosylhomocysteinase metabolism, Begomovirus metabolism, Begomovirus pathogenicity, Gene Expression Regulation, Enzymologic, Host-Pathogen Interactions, Plant Diseases genetics, Plant Diseases virology, Satellite Viruses metabolism, Satellite Viruses pathogenicity, Transcription, Genetic, Two-Hybrid System Techniques, Viral Proteins metabolism, Adenosylhomocysteinase genetics, Begomovirus genetics, DNA Methylation, Gene Expression Regulation, Viral, Gene Silencing, Satellite Viruses genetics

Abstract

DNA methylation is a fundamental epigenetic modification that regulates gene expression and represses endogenous transposons and invading DNA viruses. As a counter-defense, the geminiviruses encode proteins that inhibit methylation and transcriptional gene silencing (TGS). Some geminiviruses have acquired a betasatellite called DNA β. This study presents evidence that suppression of methylation-mediated TGS by the sole betasatellite-encoded protein, βC1, is crucial to the association of Tomato yellow leaf curl China virus (TYLCCNV) with its betasatellite (TYLCCNB). We show that TYLCCNB complements Beet curly top virus (BCTV) L2⁻ mutants deficient for methylation inhibition and TGS suppression, and that cytosine methylation levels in BCTV and TYLCCNV genomes, as well as the host genome, are substantially reduced by TYLCCNB or βC1 expression. We also demonstrate that while TYLCCNB or βC1 expression can reverse TGS, TYLCCNV by itself is ineffective. Thus its AC2/AL2 protein, known to have suppression activity in other geminiviruses, is likely a natural mutant in this respect. A yeast two-hybrid screen of candidate proteins, followed by bimolecular fluorescence complementation analysis, revealed that βC1 interacts with S-adenosyl homocysteine hydrolase (SAHH), a methyl cycle enzyme required for TGS. We further demonstrate that βC1 protein inhibits SAHH activity in vitro. That βC1 and other geminivirus proteins target the methyl cycle suggests that limiting its product, S-adenosyl methionine, may be a common viral strategy for methylation interference. We propose that inhibition of methylation and TGS by βC1 stabilizes geminivirus/betasatellite complexes.

Published

2011

16. Suppressors of RNA silencing encoded by the components of the cotton leaf curl begomovirus-betasatellite complex.

Author

Amin I, Hussain K, Akbergenov R, Yadav JS, Qazi J, Mansoor S, Hohn T, Fauquet CM, and Briddon RW

Subjects

Agrobacterium tumefaciens, Begomovirus genetics, Gene Expression Regulation, Viral physiology, Genes, Suppressor physiology, Green Fluorescent Proteins genetics, Host-Pathogen Interactions, Protein Binding, RNA, Viral metabolism, Satellite Viruses genetics, Nicotiana genetics, Transgenes physiology, Viral Proteins genetics, Viral Proteins metabolism, Begomovirus metabolism, Plant Leaves virology, RNA Interference, Satellite Viruses metabolism, Nicotiana virology

Abstract

Begomoviruses (family Geminiviridae) are single-stranded DNA viruses transmitted by the whitefly Bemisia tabaci. Many economically important diseases in crops are caused by begomoviruses, particularly in tropical and subtropical environments. These include the betasatellite-associated begomoviruses causing cotton leaf curl disease (CLCuD) that causes significant losses to a mainstay of the economy of Pakistan, cotton. RNA interference (RNAi) or gene silencing is a natural defense response of plants against invading viruses. In counter-defense, viruses encode suppressors of gene silencing that allow them to effectively invade plants. Here, we have analyzed the ability of the begomovirus Cotton leaf curl Multan virus (CLCuMV) and its associated betasatellite, Cotton leaf curl Multan β-satellite (CLCuMB) which, together, cause CLCuD, and the nonessential alphasatellite (Cotton leaf curl Multan alphasatellite [CLCuMA]) for their ability to suppress gene silencing in Nicotiana benthamiana. The results showed that CLCuMV by itself was unable to efficiently block silencing. However, in the presence of the betasatellite, gene silencing was entirely suppressed. Silencing was not affected in any way when infections included CLCuMA, although the alphasatellite was, for the first time, shown to be a target of RNA silencing, inducing the production in planta of specific small interfering RNAs, the effectors of silencing. Subsequently, using a quantitative real-time polymerase chain reaction assay and Northern blot analysis, the ability of all proteins encoded by CLCuMV and CLCuMB were assessed for their ability to suppress RNAi and the relative strengths of their suppression activity were compared. The analysis showed that the V2, C2, C4, and βC1 proteins exhibited suppressor activity, with the V2 showing the strongest activity. In addition, V2, C4, and βC1 were examined for their ability to bind RNA and shown to have distinct specificities. Although each of these proteins has, for other begomoviruses or betasatellites, been previously shown to have suppressor activity, this is the first time all proteins encoded by a geminiviruses (or begomovirus-betasatellite complex) have been examined and also the first for which four separate suppressors have been identified.

Published

2011

17. C68 from the Sulfolobus islandicus plasmid-virus pSSVx is a novel member of the AbrB-like transcription factor family.

Author

Contursi P, D'Ambrosio K, Pirone L, Pedone E, Aucelli T, She Q, De Simone G, and Bartolucci S

Subjects

Amino Acid Sequence, Crystallography, X-Ray, DNA Footprinting, DNA, Intergenic metabolism, DNA-Binding Proteins chemistry, DNA-Binding Proteins genetics, DNA-Binding Proteins isolation & purification, DNA-Binding Proteins metabolism, Dimerization, Fuselloviridae genetics, Molecular Sequence Data, Operator Regions, Genetic, Plasmids genetics, Promoter Regions, Genetic, Protein Conformation, Recombinant Proteins chemistry, Recombinant Proteins isolation & purification, Recombinant Proteins metabolism, Satellite Viruses genetics, Satellite Viruses metabolism, Selenomethionine metabolism, Sequence Alignment, Sequence Homology, Amino Acid, Sulfolobus metabolism, Transcription Factors genetics, Transcription Factors isolation & purification, Viral Proteins genetics, Viral Proteins isolation & purification, Fuselloviridae metabolism, Plasmids metabolism, Sulfolobus virology, Transcription Factors chemistry, Transcription Factors metabolism, Viral Proteins chemistry, Viral Proteins metabolism

Abstract

The genetic element pSSVx from Sulfolobus islandicus, strain REY15/4, is a hybrid between a plasmid and a fusellovirus. This plasmid-virus hybrid infects several species of the hyperthermophilic acidophilic crenarchaeon Sulfolobus. The open reading frame orfc68 of pSSVx encodes a 7.7 kDa protein that does not show significant sequence homology with any protein with known three-dimensional structure. EMSA (electrophoretic mobility-shift assay) experiments, DNA footprinting and CD analyses indicate that recombinant C68, purified from Escherichia coli, binds to two different operator sites that are located upstream of its own promoter. The three-dimensional structure, solved by a single-wavelength anomalous diffraction experiment on a selenomethionine derivative, shows that the protein assumes a swapped-hairpin fold, which is a distinctive fold associated with a family of prokaryotic transcription factors, such as AbrB from Bacillus subtilis. Nevertheless, C68 constitutes a novel representative of this family because it shows several peculiar structural and functional features.

Published

2011

18. The capsid protein of satellite Panicum mosaic virus contributes to systemic invasion and interacts with its helper virus.

Author

Omarov RT, Qi D, and Scholthof KB

Subjects

Capsid Proteins chemistry, Capsid Proteins metabolism, Cell Membrane metabolism, Cell Membrane virology, Cell Wall metabolism, Cell Wall virology, Cytosol metabolism, Cytosol virology, Helper Viruses chemistry, Molecular Weight, Mosaic Viruses chemistry, Mosaic Viruses metabolism, Movement, Panicum virology, Plant Diseases virology, RNA, Viral biosynthesis, Satellite Viruses chemistry, Satellite Viruses metabolism, Subcellular Fractions metabolism, Virus Assembly, Capsid Proteins physiology, Helper Viruses physiology, Mosaic Viruses physiology, Satellite Viruses physiology

Abstract

Satellite panicum mosaic virus (SPMV) depends on its helper Panicum mosaic virus (PMV) for replication and spread in host plants. The SPMV RNA encodes a 17-kDa capsid protein (CP) that is essential for formation of its 16-nm virions. The results of this study indicate that in addition to the expression of the full-length SPMV CP from the 5'-proximal AUG start codon, SPMV RNA also expresses a 9.4-kDa C-terminal protein from the third in-frame start codon. Differences in solubility between the full-length protein and its C-terminal product were observed. Subcellular fractionation of infected plant tissues showed that SPMV CP accumulates in the cytosol, cell wall-, and membrane-enriched fractions. However, the 9.4-kDa protein exclusively cofractionated with cell wall- and membrane-enriched fractions. Earlier studies revealed that the 5'-untranslated region (5'-UTR) from nucleotides 63 to 104 was associated with systemic infection in a host-specific manner in millet plants. This study shows that nucleotide deletions and insertions in the 5'-UTR plus simultaneous truncation of the N-terminal part of the CP impaired SPMV spread in foxtail millet, but not in proso millet plants. In contrast, the expression of the full-length version of SPMV CP efficiently compensated the negative effect of the 5'-UTR deletions in foxtail millet. Finally, immunoprecipitation assays revealed the presence of a specific interaction between the capsid proteins of SPMV and its helper virus (PMV). Our findings show that the SPMV CP has several biological functions, including facilitating efficient satellite virus infection and movement in millet plants.

Published

2005

19. Satellite panicum mosaic virus capsid protein elicits symptoms on a nonhost plant and interferes with a suppressor of virus-induced gene silencing.

Author

Qiu W and Scholthof KB

Subjects

Capsid Proteins metabolism, Gene Expression Regulation, Plant, Gene Expression Regulation, Viral, Genes, Suppressor physiology, Genetic Vectors genetics, Green Fluorescent Proteins, Helper Viruses genetics, Helper Viruses metabolism, Luminescent Proteins genetics, Luminescent Proteins metabolism, Mosaic Viruses metabolism, Panicum genetics, Panicum virology, Plants, Genetically Modified, Potexvirus genetics, Potexvirus metabolism, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Satellite Viruses metabolism, Nicotiana metabolism, Capsid Proteins genetics, Gene Silencing physiology, Mosaic Viruses genetics, Satellite Viruses genetics, Nicotiana genetics

Abstract

The capsid protein (CP) of satellite panicum mosaic virus (SPMV) has been implicated as a pathogenicity factor, inducing severe chlorosis on millet plants co-infected with SPMV and its helper virus, Panicum mosaic virus (PMV). In this study, we tested the effects of SPMV CP on Nicotiana benthamiana, a plant that does not support PMV+SPMV infections. SPMV CP expressed from a Potato virus X (PVX) gene vector elicited necrotic lesions on N. benthamiana. Pathogenicity factors often have the additional feature of acting as suppressors of gene silencing; therefore, several assays were developed to test if SPMV CP could act in such a capacity. The results showed that SPMV CP failed to act as a suppressor of posttranscriptional gene silencing when such tests were performed with transgenic N. benthamiana plants silenced for green fluorescent protein (GFP) expression by agroinfiltration or plant virus vectors. However SPMV CP expressed from the PVX gene vector did interfere with suppressor activity associated with PVX p25. This included a rebounded level of GFP silencing along the vascular tissues, including the veins on upper noninoculated leaves. Therefore, the roles of the SPMV CP now include encapsidation of the SPMV RNA, activity as a pathogenicity factor in both host and nonhost plants, and the enigmatic feature of interfering with suppression of gene silencing.

Published

2004

20. RNA: protein interactions associated with satellites of panicum mosaic virus.

Author

Desvoyes B and Scholthof KB

Subjects

Capsid isolation & purification, Centrifugation, Density Gradient, Mosaic Viruses genetics, Satellite Viruses genetics, Capsid metabolism, Mosaic Viruses metabolism, Panicum virology, RNA, Viral metabolism, Satellite Viruses metabolism

Abstract

The interactions between satellite panicum mosaic virus (SPMV) capsid protein (CP) and its 824 nucleotide (nt) single stranded RNA were investigated by gel mobility shift assay and Northwestern blot assay. SPMV CP has specificity for its RNA at high affinity, but little affinity for non-viral RNA. The SPMV CP also bound a 350 nt satellite RNA (satRNA) that, like SPMV, is dependent on panicum mosaic virus for its replication. SPMV CP has the novel property of encapsidating SPMV RNA and satRNA. Competition gel mobility shift assays performed with a non-viral RNA and unlabeled SPMV RNA and satRNA revealed that these RNA:protein interactions were in part sequence specific.

Published

2000

21. In vitro- and in vivo-generated defective RNAs of satellite panicum mosaic virus define cis-acting RNA elements required for replication and movement.

Author

Qiu W and Scholthof KB

Subjects

3' Untranslated Regions physiology, 5' Untranslated Regions physiology, Base Sequence, Capsid analysis, Capsid deficiency, Capsid genetics, DNA, Complementary genetics, Gene Deletion, Molecular Sequence Data, Mutagenesis, Site-Directed, Nucleic Acid Hybridization, Open Reading Frames, Panicum virology, RNA, Messenger genetics, RNA, Satellite chemistry, Satellite Viruses metabolism, Sequence Alignment, Genome, Viral, Mosaic Viruses genetics, RNA, Satellite genetics, Satellite Viruses genetics, Virus Replication

Abstract

Satellite panicum mosaic virus (SPMV) depends on its helper virus, panicum mosaic virus (PMV), to provide trans-acting proteins for replication and movement. The 824-nucleotide (nt) genome of SPMV possesses an open reading frame encoding a 17.5-kDa capsid protein (CP), which is shown to be dispensable for SPMV replication. To localize cis-acting RNA elements required for replication and movement, a comprehensive set of SPMV cDNA deletion mutants was generated. The results showed that the 263-nt 3' untranslated region (UTR) plus 73 nt upstream of the CP stop codon and the first 16 nt in the 5' UTR are required for SPMV RNA amplification and/or systemic spread. A region from nt 17 to 67 within the 5' UTR may have an accessory role in RNA accumulation, and a fragment bracketing nt 68 to 104 appears to be involved in the systemic movement of SPMV RNA in a host-dependent manner. Unexpectedly, defective RNAs (D-RNAs) accumulated de novo in millet plants coinfected with PMV and either of two SPMV mutants: SPMV-91, which is incapable of expressing the 17.5-kDa CP, and SPMV-GUG, which expresses low levels of the 17.5-kDa CP. The D-RNA derived from SPMV-91 was isolated from infected plants and used as a template to generate a cDNA clone. RNA transcripts derived from this 399-nt cDNA replicated and moved in millet plants coinoculated with PMV. The characterization of this D-RNA provided a biological confirmation that the critical RNA domains identified by the reverse genetic strategy are essential for SPMV replication and movement. The results additionally suggest that a potential "trigger" for spontaneous D-RNA accumulation may be associated with the absence or reduced accumulation of the 17.5-kDa SPMV CP. This represents the first report of a D-RNA associated with a satellite virus.

Published

2000

22. Bacteriophage P2 and P4 morphogenesis: assembly precedes proteolytic processing of the capsid proteins.

Author

Marvik OJ, Jacobsen E, Dokland T, and Lindqvist BH

Subjects

Bacteriophage P2 growth & development, Bacteriophage P2 ultrastructure, Base Sequence, Capsid ultrastructure, Coliphages growth & development, Coliphages ultrastructure, DNA Primers, Hydrolysis, Microscopy, Electron, Molecular Sequence Data, Satellite Viruses growth & development, Satellite Viruses ultrastructure, Bacteriophage P2 metabolism, Capsid metabolism, Coliphages metabolism, Protein Processing, Post-Translational, Satellite Viruses metabolism

Abstract

Several of the structural proteins of phage P2 and its satellite P4 undergo proteolytic processing during development of mature phage particles. Here, we report that uncleaved shell protein, gpN, is present in immature capsids of both P2 and P4, showing that assembly precedes processing. This excludes the possibility that processing of gpN is involved in capsid size determination. We also find that N*, the fully processed version of gpN, produced from a plasmid, can assemble into both P2- and P4-sized particles, implying that the amino-terminal end of gpN is not required for assembly initiation nor for the formation of a T = 4 shell. As may be expected for a scaffolding protein, we find that gpO coexists with gpN in immature P2, as well as P4, capsids. This result supports the conclusion that gpO is required for both phages and strongly suggests that the O derivative, h7 (found in mature capsids), results from proteolytic cleavage after gpN/gpO coassembly.

Published

1994

23. Characterization of the capsid associating activity of bacteriophage P4's Psu protein.

Author

Isaksen ML, Dokland T, and Lindqvist BH

Subjects

Amino Acid Sequence, Capsid immunology, Capsid isolation & purification, Capsid ultrastructure, Coliphages ultrastructure, DNA, Viral, Microscopy, Immunoelectron, Molecular Sequence Data, Satellite Viruses ultrastructure, Capsid metabolism, Capsid Proteins, Coliphages metabolism, Satellite Viruses metabolism

Abstract

The Psu (Polarity suppression) protein of satellite bacteriophage P4 was first characterized as an anti-terminator of transcription termination in Escherichia coli. Psu is also a structural component of mature P4 capsids, where it is present as a decoration protein. Psu is located externally on the capsid surface, and it appears to protect the capsid from loss of DNA through the capsid shell. The ability of Psu to specifically bind to the P4 capsid appears not to be dependent on any P4 specific components such as the capsid protein cleavage products h1 and h2, or P4 DNA. We suggest that Psu binds to the P4 capsid as a result of the special structure of the hexamers in the P4 capsid.

Published

1993

24. Characterization of the five-fold Ca2+ binding site of satellite tobacco necrosis virus using Eu3+ luminescence spectroscopy: a marked size-selectivity among rare earth ions.

Author

Burroughs SE, Eisenman G, and Horrocks WD Jr

Subjects

Binding Sites, Cations, Divalent, Europium, Luminescent Measurements, Spectrum Analysis, Calcium metabolism, Plant Viruses metabolism, Satellite Viruses metabolism

Abstract

Satellite tobacco necrosis virus (STNV) is an icosahedral virus which contains three classes of Ca2+ binding site. One of these classes, a five-fold carbonyl site which is believed to exist in a Ca2+ channel, has been investigated using laser-induced Eu3+ luminescence spectroscopy. These twelve identical sites are rather rigid, as evidenced by the single narrow (full width at half-maximum is 6.5 cm-1) band observed at 579.58 nm in the 7F0----5D0 excitation spectrum of the Eu(3+)-STNV complex. Lifetimes of 270 microseconds in H2O and 1620 microseconds in D2O indicate that there are three water molecules bound to the Eu3+ at this site. Ligand field splitting of the 7F0----5D1 and 7F0----5D2 excitation spectra show that this site possesses fairly high symmetry (less than or equal to C5V). The Eu3+ complex of nitrilotriacetic acid was determined via titration to have a dissociation constant, Kd, of 20 +/- 2 nM; this value has been used in competition experiments to deduce that the virus site class binds Eu3+ with a Kd of 1.1 +/- 0.3 nM. This putative ion channel demonstrates remarkable size selectivity, with lanthanide affinities varying by more than one order of magnitude.

Published

1992

25. A transactivation mutant of satellite phage P4.

Author

Souza L, Calendar R, Six EW, and Lindqvist BH

Subjects

Coliphages metabolism, DNA Replication, DNA, Viral biosynthesis, Escherichia coli, Genetic Complementation Test, Helper Viruses growth & development, Helper Viruses metabolism, Lysogeny, Satellite Viruses metabolism, Temperature, Viral Proteins biosynthesis, Virus Replication, Coliphages growth & development, Genes, Mutation, Satellite Viruses growth & development

Published

1977

26. Genome localization of adeno-associated virus RNA.

Author

Carter BJ, Fife KH, de la Maza LM, and Berns KI

Subjects

DNA Restriction Enzymes metabolism, DNA, Viral metabolism, Nucleic Acid Hybridization, Genes, RNA, Viral biosynthesis, Satellite Viruses metabolism, Transcription, Genetic

Abstract

In previous work, linear duplex molecules of adeno-associated virus, type 2 (AAV2), DNA were cleaved with the restriction endonucleases R-EcoRI, R-HindII, and R-HindIII. The physical order of the specific fragments obtained was deduced and oriented with respect to the DNA strand polarity and the direction of transcription. Stable AAV RNA is transcribed only from 70% of the minus DNA strand. We report here RNA-DNA hybridization experiments using these restriction fragments to obtain a more accurate map of the portion of the AAV genome represented in stable RNA. The data obtained with several sets of restriction fragments annealed to either whole-cell RNA or poly(A)-containing RNA were internally consistent. The AAV RNA annealed with a continuous region of the AAV DNA, beginning at 0.18 map units (18%) from the left end of the molecule and ending at 0.88 map units. In addition, the restriction endonuclease BamHI was found to make one specific cleavage in AAV2 DNA at 0.22 map units, which is 0.04 map units (i.e., 160 nucleotides) to the right (""down stream'') of the point corresponding to the 5' end of the viral mRNA.

Published

1976

27. Tobacco ringspot virus codes for the coat protein of its satellite.

Author

Schneider IR and White RM

Subjects

Antigens, Viral analysis, Plant Viruses growth & development, Plant Viruses immunology, Protein Conformation, Satellite Viruses growth & development, Satellite Viruses immunology, Viral Proteins immunology, Virus Replication, Genetic Code, Plant Viruses metabolism, Satellite Viruses metabolism, Viral Proteins biosynthesis

Published

1976

28. Study of the fine structure of adeno-associated virus DNA with bacterial restriction endonucleases.

Author

Berns KI, Kort J, Fife KH, Grogan EW, and Spear I

Subjects

Base Sequence, Chromosomes analysis, DNA, Viral metabolism, Molecular Weight, Satellite Viruses metabolism, DNA Restriction Enzymes metabolism, DNA, Viral analysis, Endonucleases metabolism, Satellite Viruses analysis

Abstract

A physical map of the adeno-associated virus type 2 genome has been constructed on the basis of the five fragments produced by the restriction endonucleases HindII + III from Hemophilus influenzae. There are three endo R-HindII cleavage sites and one endo R-HindIII site. Evidence has been obtained to support the existence of two nucleotide sequence permutations in adeno-associated virus DNA, the start points of which have been estimated to be separated by 1% of the genome. The three cleavage fragments produced by endo R-Eco RI have been ordered and oriented with respect to the endo R-HindII + III cleavage map.

Published

1975

29. EcoRI endonuclease cleavage map of bacteriophage P4-DNA.

Author

Goldstein L, Thomas M, and Davis RW

Subjects

Base Sequence, Binding Sites, Coliphages metabolism, DNA Viruses, DNA, Viral metabolism, Electrophoresis, Agar Gel, Escherichia coli enzymology, Microscopy, Electron, Molecular Weight, Nucleic Acid Denaturation, Satellite Viruses metabolism, Coliphages analysis, DNA Restriction Enzymes metabolism, DNA, Viral analysis, Endonucleases metabolism, Satellite Viruses analysis

Published

1975

30. Characterization of adenovirus-associated virus-induced polypeptides in KB cells.

Author

Buller RM and Rose JA

Subjects

Adenoviruses, Human growth & development, Canavanine pharmacology, Cell Line, Humans, Molecular Weight, Parvoviridae growth & development, Phenylmethylsulfonyl Fluoride pharmacology, Satellite Viruses growth & development, Tosyllysine Chloromethyl Ketone pharmacology, Tosylphenylalanyl Chloromethyl Ketone pharmacology, Virus Replication, Parvoviridae metabolism, Peptide Biosynthesis, Satellite Viruses metabolism, Viral Proteins biosynthesis

Abstract

Electrophoretic analysis of KB cells coinfected with adenovirus-associated virus (AAV) type 2, a defective parvovirus, and adenovirus type 5 (as helper) have revealed the synthesis in vivo of at least five AAV-specific polypeptides. The three largest polypeptides, with molecular weights of 90,700, 71,600, and 60,000 comigrated in polyacrylamide gels with the three AAV structural polypeptides. The remaining two polypeptides had molecular weights of 24,900 and 15,800. The concentrations of the AAV-induced polypeptides relative to one another remained approximately constant during the infectious cycle, and the structural components were present in proportions similar to those found in purified virions. As determined by pulse-chase experiments, all polypeptides were generated at the level of protein synthesis and not by posttranslational proteolytic processing. Although inhibitors of proteolytic enzymes failed to influence the pattern of AAV-induced polypeptides, and amino acid analog, L-canavanine, blocked the appearances of both the major structural polypeptide (60,000 daltons) and the larger nonstructural polypeptide (24,900 daltons). Taken in conjunction with pulse-chase data, this result supports a model whereby the major virion polypeptide is produced by proteolytic cleavage of the nascent polypeptide chain.

Published

1978

31. Growth of adeno-associated satellitte virus under conditions of arginine deprivation.

Author

Mayor HD and Gorman C

Subjects

Adenoviruses, Simian growth & development, Adenoviruses, Simian metabolism, Adenoviruses, Simian ultrastructure, Animals, Cell Line, Cell Nucleus microbiology, Centrifugation, Density Gradient, Crystallography, Cytoplasm microbiology, Haplorhini, Helper Viruses growth & development, Helper Viruses metabolism, Helper Viruses ultrastructure, Hemagglutination Tests, Hemagglutinins, Viral analysis, Kidney, Microscopy, Electron, Satellite Viruses metabolism, Satellite Viruses ultrastructure, Virus Replication, Arginine metabolism, Satellite Viruses growth & development

Published

1975

32. DNA-minus temperature-sensitive mutants of adenovirus type 5 help adenovirus-associated virus replication.

Author

Straus SE, Ginsberg HS, and Rose JA

Subjects

Adenoviridae metabolism, Cell Line, DNA Replication, DNA, Viral biosynthesis, Mutation, RNA, Viral biosynthesis, Satellite Viruses metabolism, Temperature, Transcription, Genetic, Adenoviridae growth & development, Helper Viruses growth & development, Satellite Viruses growth & development, Virus Replication

Abstract

Efficient potentiation of adenovirus-associated viruses (AAV) replication occurs in coinfections with either of two DNA-minus temperature-sensitive mutants of adenovirus type 5 (Ad5), ts125 and ts149. The helper activity of these mutants does not result from leakiness. At the nonpermissive termperature (39.5 C) there was little or no detectable adenovirus DNA synthesis, and only a relatively low level of adenovirus transcription was observed. However, the synthesis of AAV DNA and RNA and the yield of infectious AAV were comparable in amounts to those found when wild-type Ad5 was the helper. Furthermore, an apparent lag in the initiation of AAV transcription after the onset of AAV DNA synthesis was seen in coinfections with both wild type or ts125. These findings strongly suggest that the adenovirus factor(s) required for AAV multiplication is produced early in the adenovirus DNA replication, this requirement does not include all factors directly needed for adenovirus DNA synthesis.

Published

1975

33. Distribution of RNA polymerase binding sites on the P4 chromosome.

Author

Lindqvist BH and Williams RC

Subjects

Binding Sites, Coliphages genetics, Genes, Viral, Satellite Viruses genetics, Transcription, Genetic, Coliphages metabolism, DNA, Viral metabolism, DNA-Directed RNA Polymerases metabolism, Escherichia coli enzymology, Satellite Viruses metabolism

Published

1979

34. Escherichia coli deoxyribonucleic acid synthesis mutants: their effect upon bacteriophage P2 and satellite bacteriophage P4 deoxyribonucleic acid synthesis.

Author

Bowden DW, Twersky RS, and Calendar R

Subjects

Coliphages growth & development, DNA Replication, DNA Viruses, Genes, Mitomycins pharmacology, Satellite Viruses growth & development, Temperature, Virus Replication, Coliphages metabolism, DNA, Bacterial biosynthesis, DNA, Viral biosynthesis, Escherichia coli metabolism, Mutation, Satellite Viruses metabolism

Abstract

Escherichia coli C strains containing different deoxyribonucleic acid (DNA) synthesis mutations have been tested for their support of the DNA synthesis of bacteriophage P2 and its satellite phage P4. Bacteriophage P2 requires functional dnaB, dnaE, and dnaG E. coli gene products for DNA synthesis, whereas it does not require the products of the dnaA, dnaC, or dnaH genes. In contrast, the satellite virus P4 requires functional dnaE and dnaH gene products for DNA synthesis and does not need the products of the dnaA, dnaB, dnaC, and dnaG genes. Thus the P2 and P4 genomes are replicated differently, even though they are packaged in heads made of the same protein.

Published

1975

35. In vitro packaging of satellite phage P4 DNA.

Author

Pruss G, Goldstein RN, and Calendar R

Subjects

Coliphages growth & development, Genotype, Molecular Weight, Satellite Viruses growth & development, Coliphages metabolism, DNA, Viral metabolism, Satellite Viruses metabolism, Viral Proteins biosynthesis

Abstract

Satellite phage P4 directs the capsid proteins of its helper phage, P2, to form a head which is only one-third the size of the normal P2 head. The P2 head contains a genome of molecular weight 22 x 10(6), while the small P4 head contains a genome with a molecular weight of only 7 x 10(6). We have used in vitro DNA packaging to test whether P2 and P4 phage head sizes are determined by DNA size. The small DNA of satellite phage P4 added to a P2-infected cell extract was packaged primarily into particles containing three copies of the P4 genome. This process occurred with approximately the same efficiency as P2 DNA packaging in the same cell extract. In contrast, the large DNA of P2 was packaged 300-fold less efficiently than the small DNA of P4 in an extract derived from P4-infected, P2-lysogenic cells. These results suggest that DNA size is not sufficient to determine head size. The results are compatible with DNA packaging via the filling of preformed empty capsids.

Published

1974

36. Concatemers of alternating plus and minus strands are intermediates in adenovirus-associated virus DNA synthesis.

Author

Straus SE, Sebring ED, and Rose JA

Subjects

DNA Replication, DNA, Viral isolation & purification, Models, Biological, DNA, Viral biosynthesis, Parvoviridae metabolism, Satellite Viruses metabolism

Abstract

Replicating DNA molecules of adenovirus-associated virus (AAV) were selectively extracted from KB cells coinfected at 39.5 detrees with a DNA minus, temperature-sensitive mutant of adenovirus 5 (ts125) as helper. Under these conditions AAV DNA replication proceeds normally, but there is little, if any, adenovirus DNA synthesis. An analysis of the replicating molecules in sucrose density gradients reveals that there are AAV DNA intermediates which consist of covalently linked plus and minus DNA strands. Under denaturing conditions, these concatemers are linear single strands whose lengths can reach at least four times the size of the AAV genome. The most abundant concatemeric species is a dimer which presumably exists in vivo as a unit length hairpin. Unit length linear duplexes appear to be immediate precursors of plus and minus progeny strands. These findings are compatible with a self-priming mechanism for the synthesis of AAV DNA.

Published

1976

37. Molecular similarities among the adenovirus-associated virus polypeptides and evidence for a precursor protein.

Author

Johnson FB, Thomson TA, Taylor PA, and Vlazny DA

Subjects

Adenoviridae, Antigens, Viral, Aspartic Acid analysis, Leucine analysis, Lysine analysis, Molecular Weight, Parvoviridae metabolism, Satellite Viruses metabolism, Viral Proteins biosynthesis, Viral Proteins immunology, Parvoviridae analysis, Protein Precursors analysis, Satellite Viruses analysis, Viral Proteins analysis

Published

1977

38. Multiple structures of adeno-associated virus DNA: analysis of terminally labeled molecules with endonuclease R-Hae III.

Author

Denhardt DT, Eisenberg S, Bartok K, and Carter BJ

Subjects

Base Sequence, DNA, Viral metabolism, Haemophilus enzymology, Molecular Weight, Nucleotides analysis, Satellite Viruses metabolism, DNA Restriction Enzymes metabolism, DNA, Viral analysis, Endonucleases metabolism, Satellite Viruses analysis

Abstract

The double-stranded form of adeno-associated virus (AAV) DNA has about 20 sites sensitive to endonuclease R.Hae III from Haemophilus aegypitus; the fragments produced fall into about 13 size classes, 8 of which contain single fragments. The location of the Hae III-produced AAV fragments relative to the three EcoR1 fragments was determined. Using revised figures for the molecular weights of the Hae III cleavage products of phiX174 replicative form DNA, we calculated that AAV DNA contains about 4,000 nucleotides. After Hae III digestiion of duplex DNA terminally labeled with 32P using polynucleotide kinase, the majority of fragments containing a 5' 32P label were about 40 nucleotides in length, and fragments of similar size were generated from each end, suggesting that the Hae site closest to the end is within the terminal repetition. Two more-slowly-migrating cleavage products also bore 5' 32P end label. These three terminally labeled species were also generated from single-stranded AAV DNA by digestion with Hae III, and evidence that one may have a nonlinear ("rabbit-ear") structure is presented. The predominant 5' terminal base was identified as thymine for both the plus and minus strands of AAV. Single-stranded AAV molecules could not be efficiently covalently circularized by incubation with polynucleotide ligase or ligase plus T4 DNA polymerase.

Published

1976

39. Survival of a satellite RNA in vivo and its dependence on cucumber mosaic virus for replication.

Author

Mossop DW and Francki RI

Subjects

Helper Viruses growth & development, Mosaic Viruses metabolism, Plants, Toxic, Satellite Viruses metabolism, Nicotiana microbiology, Mosaic Viruses growth & development, Plant Viruses growth & development, RNA, Viral biosynthesis, Virus Replication

Published

1978

40. Origin and termination of adeno-associated virus DNA replication.

Author

Hauswirth WW and Berns KI

Subjects

Base Sequence, Cell Line, DNA Restriction Enzymes metabolism, DNA, Viral analysis, Deoxyribonucleases metabolism, Exonucleases metabolism, Nucleotides analysis, Satellite Viruses analysis, DNA Replication, DNA, Viral biosynthesis, Satellite Viruses metabolism

Published

1977

41. Multiplication of adeno-associated virus type 1 in cells coinfected with a temperature-sensitive mutant of human adenovirus type 31.

Author

Handa H, Shimojo H, and Yamaguchi K

Subjects

Antigens, Viral, Cell Line, Cycloheximide pharmacology, DNA, Viral biosynthesis, Inclusion Bodies, Viral, Mutation, Satellite Viruses immunology, Satellite Viruses metabolism, Temperature, Adenoviruses, Human growth & development, Satellite Viruses growth & development

Published

1976

42. Complementation of adeno-associated satellite virus (AAV) by temperature-sensitive mutants of adenovirus type 31.

Author

Mayor HD, Carrier S, and Jordan L

Subjects

Adenoviruses, Human immunology, Adenoviruses, Human metabolism, Antigens, Viral analysis, Cell Line, DNA, Viral biosynthesis, Satellite Viruses immunology, Satellite Viruses metabolism, Temperature, Viral Proteins biosynthesis, Virus Replication, Adenoviruses, Human growth & development, Mutation, Satellite Viruses growth & development

Abstract

Temperature-sensitive (ts) matants of human adenovirus type 31 were able to complement adeno-associated satellite virus (AAV) antigen production in both HEK and KB cells at both permissive and non-permissive temperatures. However, mutant ts 94, an adenovirus 31 mutant which produces apparently normal amounts of structural protein and DNA but is defective in maturation, was significantly inhibited in its ability to potentiate AAV infectivity at the non-permissive temperature. Normal AAV DNA and adenovirus DNA were isolated from co-infections with AAV and mutant ts 94 at the non-permissive temperature. We suggest that an adenovirus-coded maturation function common to both adenovirus and AAV maturation is defective in the ts 94 system.

Published

1977

43. Mutual derepression in the P2-P4 bacteriophage system.

Author

Six EW and Lindqvist BH

Subjects

Coliphages growth & development, Coliphages metabolism, DNA Replication, DNA, Viral biosynthesis, Lysogeny, Mutation, Satellite Viruses growth & development, Satellite Viruses metabolism, Virus Replication, Coliphages genetics, Genes, Regulator, Genes, Viral, Satellite Viruses genetics

Published

1978

44. Helper-dependent bacteriophage P4: a model satellite virus and its implications for animal virology.

Author

Barrett K, Calendar R, Gibbs W, Goldstein RN, Lindqvist B, and Six E

Subjects

Adenoviridae, Avian Sarcoma Viruses, Bacteriolysis, DNA Replication, DNA Viruses growth & development, DNA Viruses metabolism, DNA, Viral biosynthesis, Friend murine leukemia virus, Gammaretrovirus, Genes, Lysogeny, Microscopy, Electron, Morphogenesis, Oncogenic Viruses, Coliphages growth & development, Coliphages metabolism, Helper Viruses, Satellite Viruses growth & development, Satellite Viruses metabolism

Published

1973

45. Separate helper functions provided by adenovirus for adenovirus-associated virus multiplication.

Author

Carter BJ, Koczot FJ, Garrison J, Rose JA, and Dolin R

Subjects

Adenoviridae drug effects, Carcinoma, Cell Line, DNA, Viral biosynthesis, Floxuridine pharmacology, Humans, Kinetics, Mouth Neoplasms, RNA, Viral biosynthesis, Satellite Viruses drug effects, Thymidine metabolism, Tritium, Uridine metabolism, Adenoviridae metabolism, Helper Viruses metabolism, Satellite Viruses metabolism, Virus Replication

Published

1973

46. Two new isolates of the satellite of tobacco ringspot virus.

Author

Schneider IR, White RM, and Gooding GV Jr

Subjects

Centrifugation, Density Gradient, North Carolina, Plant Diseases, Plant Viruses metabolism, Plants, Edible, Plants, Toxic, Satellite Viruses metabolism, Nicotiana, Viral Proteins biosynthesis, Plant Viruses isolation & purification, Satellite Viruses isolation & purification

Published

1972

47. The RNA of RNA-containing tumor viruses.

Author

Bader JP

Subjects

Animals, Avian Sarcoma Viruses metabolism, Cell-Free System, Chick Embryo, Cycloheximide pharmacology, Dactinomycin pharmacology, Electrophoresis, Polyacrylamide Gel, Leukemia Virus, Murine metabolism, Mice, Polysaccharides, RNA, Viral analysis, Satellite Viruses metabolism, Spleen microbiology, Tritium, Uridine metabolism, RNA Viruses metabolism, RNA, Viral biosynthesis

Published

1970

48. Studies of the enhancement of an adenovirus-associated virus by herpes simplex virus.

Author

Blacklow NR, Dolin R, and Hoggan MD

Subjects

Antigens metabolism, Arginine metabolism, Carbon Isotopes, Carcinoma, Cell Line, Culture Media, Cytarabine pharmacology, Satellite Viruses drug effects, Satellite Viruses growth & development, Satellite Viruses immunology, Satellite Viruses metabolism, Satellite Viruses pathogenicity, Adenoviridae growth & development

Published

1971

49. Translation of the initial codons of satellite tobacco necrosis virus ribonucleic acid in a cell-free system from wheat embryo.

Author

Seal SN and Marcus A

Subjects

Adenosine Triphosphate, Alanine, Carbon Radioisotopes, Cell-Free System, Centrifugation, Density Gradient, Chlortetracycline pharmacology, Chromatography, Paper, Dipeptides biosynthesis, Guanosine Triphosphate, Lysine, Magnesium, Methionine, Peptide Chain Initiation, Translational, Peptide Elongation Factors, Peptide Initiation Factors, Plant Cells, Ribosomes metabolism, Satellite Viruses drug effects, Transfer RNA Aminoacylation, Triticum, Plants metabolism, Protein Biosynthesis drug effects, RNA, Messenger metabolism, RNA, Transfer metabolism, RNA, Viral metabolism, Satellite Viruses metabolism

Published

1973

50. Adenovirus-associated virus multiplication. IX. Extent of transcription of the viral genome in vivo.

Author

Carter BJ, Khoury G, and Rose JA

Subjects

Adenoviridae metabolism, Carcinoma, Cell Line, Centrifugation, Density Gradient, Chromatography, DNA Replication, Filtration, Helper Viruses growth & development, Humans, Hydroxyapatites, Mouth Neoplasms, Nucleic Acid Hybridization, Nucleic Acid Renaturation, Phosphorus Isotopes, RNA, Viral, Satellite Viruses metabolism, Simplexvirus growth & development, Tritium, Adenoviridae growth & development, DNA, Viral, Satellite Viruses growth & development, Transcription, Genetic, Virus Replication

Abstract

Nucleic acid hybridization procedures were used to measure the extent of transcription of adenovirus-associated virus (AAV) deoxyribonucleic acid (DNA) in KB cells in the presence of either adenovirus or herpes simplex virus as the helper. Annealing of AAV ribonucleic acid to AAV DNA was monitored by a hybridization inhibition assay on nitrocellulose filters or by hydroxyapatite chromatography. These experiments confirmed the previous observation that, in the presence of either type of helper virus, only one strand of AAV DNA (the thymidine-rich or "minus" strand) is transcribed in vivo. However, it was found that only 70 to 80% of this strand appears to be transcribed in vivo. Furthermore, studies with minus strands employing hydroxyapatite chromatography and nuclease S(1), which specifically degrades single-stranded DNA, indicated that up to 20% of the minus strand is self-complementary. It seems likely that these self-complementary sequences account for the bulk of that portion of the minus strand (20 to 30%) which is not transcribed in vivo.

Published

1972