DOCSLIB.ORG

Human Papillomavirus and Related Diseases – from Bench to Bedside

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
Human Papillomavirus and Related Diseases – from Bench to Bedside HUMAN PAPILLOMAVIRUS AND RELATED DISEASES – FROM BENCH TO BEDSIDE A CLINICAL PERSPECTIVE Edited by Davy Vanden Broeck Human Papillomavirus and Related Diseases – From Bench to Bedside – A Clinical Perspective Edited by Davy Vanden Broeck Published by InTech Janeza Trdine 9, 51000 Rijeka, Croatia Copyright © 2011 InTech All chapters are Open Access distributed under the Creative Commons Attribution 3.0 license, which allows users to download, copy and build upon published articles even for commercial purposes, as long as the author and publisher are properly credited, which ensures maximum dissemination and a wider impact of our publications. After this work has been published by InTech, authors have the right to republish it, in whole or part, in any publication of which they are the author, and to make other personal use of the work. Any republication, referencing or personal use of the work must explicitly identify the original source. As for readers, this license allows users to download, copy and build upon published chapters even for commercial purposes, as long as the author and publisher are properly credited, which ensures maximum dissemination and a wider impact of our publications. Notice Statements and opinions expressed in the chapters are these of the individual contributors and not necessarily those of the editors or publisher. No responsibility is accepted for the accuracy of information contained in the published chapters. The publisher assumes no responsibility for any damage or injury to persons or property arising out of the use of any materials, instructions, methods or ideas contained in the book. Publishing Process Manager Ivona Lovric Technical Editor Teodora Smiljanic Cover Designer InTech Design Team First published January, 2012 Printed in Croatia A free online edition of this book is available at www.intechopen.com Additional hard copies can be obtained from [email protected] Human Papillomavirus and Related Diseases – From Bench to Bedside – A Clinical Perspective, Edited by Davy Vanden Broeck p. cm. ISBN 978-953-307-860-1 free online editions of InTech Books and Journals can be found at www.intechopen.com Contents Preface IX Part 1 Clinical Aspects of Human Papillomavirus Related Diseases 1 Chapter 1 Human Papillomavirus: Biology and Pathogenesis 3 José Veríssimo Fernandes and Thales Allyrio Araújo de Medeiros Fernandes Chapter 2 Immunohistochemistry in the Diagnosis of Squamous Intraepithelial Lesions of the Uterine Cervix 41 Evanthia A. Kostopoulou and George Koukoulis Chapter 3 Screening Methods in Prevention of Cervical Cancer 65 Robert Koiss Chapter 4 Clinical Manifestations of Genital HPV Infection 83 Edison Natal Fedrizzi Part 2 Human Papillomavirus Vaccines 99 Chapter 5 Development of New Human Papillomavirus Vaccines 101 Carmen Rodríguez-Cerdeira, Silvia Díez-Moreno, E. Sánchez and Alfonso Alba Chapter 6 Current Insight into Anti-HPV Immune Responses and Lessons for Prophylactic and Therapeutic Vaccines 125 Isabelle Bourgault-Villada and Simon Jacobelli Chapter 7 Plant Production of Vaccine Against HPV: A New Perspectives 147 Markéta Šmídková, Marcela Holá, Jitka Brouzdová and Karel J. Angelis Chapter 8 Development of Vaccines and Gene Therapy Against HPV Infection and Cervical Cancer 177 Zoraya De Guglielmo Cróquer and Armando Rodríguez Bermúdez VI Contents Part 3 Human Papillomavirus in Non-Uterine Disease 195 Chapter 9 Epidemiology of HPV in Head and Neck Cancer 197 Márcio Campos Oliveira, Maria da Conceição Andrade and Fabrício dos Santos Menezes Chapter 10 Implications of Human Papillomavirus Infections in the Biology of Head and Neck Cancers 221 Descamps Géraldine, Duray Anaëlle, Delvenne Philippe and Saussez Sven Chapter 11 The Role of Human Papillomavirus in Head and Neck Cancers 279 Lucinei Roberto Oliveira, Andrielle de Castilho Fernandes, Alícia Greyce Turatti Pessolato, Régia Caroline Peixoto Lira, João Paulo Oliveira-Costa, Luciana Souza Chavasco, Fabiana Alves Miranda, Ivan de Oliveira Pereira, Edson Garcia Soares and Alfredo Ribeiro-Silva Chapter 12 Human Papillomavirus in Donor Semen in Belgium 305 K.W.M. D’Hauwers, W.A.A. Tjalma, U. Punjabi and C.E. Depuydt Chapter 13 The Impact of Human Papillomavirus on Cancer Risk in Penile Cancer 319 Angela Adamski da Silva Reis and Aparecido Divino da Cruz Preface Cervical cancer is the second most prevalent cancer among women worldwide, mainly affecting young women. Infection with Human Papilloma Virus (HPV) has been identified as the causal agent for this condition. The natural history of cervical cancer is characterized by slow disease progression, generally taking over 10 years, from the initial infection with HPV, to the diagnosis of cancer. In essence, cervical cancer is a preventable disease, and treatable if diagnosed in early stage. Historically, the introduction of the Pap smear has markedly reduced the number of new cases in countries with an effective prevention program. The burden of disease is highest in developing countries, with peak incidence in Eastern Africa. Recently, prophylactic vaccines became available, equally contributing to a better disease prevention. Unfortunately, the global burden of disease is still very high. In the first section of this book, clinical aspects of HPV related disease are highlighted. Innovative clinical diagnostic tools are discussed and Dr Fedrizzi has provided a highly illustrative contribution on the clinical manifestation of HPV related disease. The introduction of the HPV prophylactic vaccine has been an important recent development in the fight against cervical cancer. The second section focuses on HPV vaccine related issues. Immune responses of the current vaccine are presented by Dr Bourgault-Villada, and options for the next generation vaccines, or more efficient production strategies, are discussed. Although HPV is most prominently known from its role in cervical carcinogenesis, the virus is also involved in other conditions. In the third section, HPV in non-uterine disease is discussed. Epidemiology and role of HPV in head-and-neck tumors are addressed. HPV also affects men, and this section covers the impact of HPV on penile cancers and its prevalence in semen. This book will be a useful tool for both researchers and clinicians dealing with cervical cancer, and it will provide them with the latest information in this field. Dr Davy Vanden Broeck, MSc, PhD Team Leader HPV/Cervical Cancer Research International Centre for Reproductive Health Ghent University Belgium X Preface Acknowledgements The editor of this book would like to express sincere thanks to all authors for their high quality contributions. The editor expresses the gratefulness to Ms. Bojana Zelenika and Ms. Ivona Lovric, process managers, for their continued cooperation. Part 1 Clinical Aspects of Human Papillomavirus Related Diseases 1 Human Papillomavirus: Biology and Pathogenesis José Veríssimo Fernandes1 and Thales Allyrio Araújo de Medeiros Fernandes2 1Federal University of Rio Grande do Norte 2University of Rio Grande do Norte State Brazil 1. Introduction The human papillomavirus (HPV) is one of the most common causes of sexually transmitted disease in both men and women around the world, especially in developing countries, where the prevalence of asymptomatic infection varies from 2 to 44%, depending on the population and studied region (Sanjosé et al., 2007). Most HPV infection is transient and some studies show that the majority of sexually active individuals are exposed to and acquire infection from this virus at some phase in their lives (Baseman and Koutsky, 2005; Trottier and Franco, 2006). HPV infection is more prevalent in young adults, at the beginning of their sexual activity, with a subsequent decline in the prevalence rate with increasing age, likely as a result of development of an immune response against the virus and reduction of sexual activity (Castle et al., 2005; Fernandes et al., 2009; Chan et al., 2010). HPV can infect basal epithelial cells of the skin or inner-lining tissues and are categorized as cutaneous types or mucosal types. Cutaneous types are epidermotropic and infect the keratinized surface of the skin, targeting the skin of the hands and feet. Mucosal types infect the lining of the mouth, throat, respiratory, or anogenital tract epithelium (Burd, 2003). Some HPVs are associated with warts while others have been well established as the main risk factor of invasive cervical cancers and their associated pre-cancerous lesions (Clifford et al., 2005; Zekri et al., 2006; Muñoz et al., 2006). However, only few HPV-infected individuals progress to invasive cervical cancer (Burd, 2003). Most infected individuals eliminate the virus without developing recognized clinical manifestation. (Bosch et al., 2008). Today, more than 150 different HPV types have been cataloged and about 40 can infect the epithelial lining of the anogenital tract and other mucosal areas of the human body. Based on their association with cervical cancer and precursor lesions, HPVs can also be classified as high-risk (HR-HPV) and low-risk (LR-HPV) oncogenic types. LR-HPV types, such as HPV 6 and 11, can cause common genital warts or benign hyperproliferative lesions with very limited tendency to malignant progression, while infection with HR-HPV types, highlighting HPV 16 and 18, is associated with the occurrence of pre-malignant and malignant cervical lesions (Muñoz et al., 2003; Bosch et al., 2002; Bosch et al., 2008). HR-HPV types are also associated with many penile, vulvar, anal, and head and neck
Load more

Recommended publications
  • Changes to Virus Taxonomy 2004
    Arch Virol (2005) 150: 189–198 DOI 10.1007/s00705-004-0429-1 Changes to virus taxonomy 2004 M. A. Mayo (ICTV Secretary) Scottish Crop Research Institute, Invergowrie, Dundee, U.K. Received July 30, 2004; accepted September 25, 2004 Published online November 10, 2004 c Springer-Verlag 2004 This note presents a compilation of recent changes to virus taxonomy decided by voting by the ICTV membership following recommendations from the ICTV Executive Committee. The changes are presented in the Table as decisions promoted by the Subcommittees of the EC and are grouped according to the major hosts of the viruses involved. These new taxa will be presented in more detail in the 8th ICTV Report scheduled to be published near the end of 2004 (Fauquet et al., 2004). Fauquet, C.M., Mayo, M.A., Maniloff, J., Desselberger, U., and Ball, L.A. (eds) (2004). Virus Taxonomy, VIIIth Report of the ICTV. Elsevier/Academic Press, London, pp. 1258. Recent changes to virus taxonomy Viruses of vertebrates Family Arenaviridae • Designate Cupixi virus as a species in the genus Arenavirus • Designate Bear Canyon virus as a species in the genus Arenavirus • Designate Allpahuayo virus as a species in the genus Arenavirus Family Birnaviridae • Assign Blotched snakehead virus as an unassigned species in family Birnaviridae Family Circoviridae • Create a new genus (Anellovirus) with Torque teno virus as type species Family Coronaviridae • Recognize a new species Severe acute respiratory syndrome coronavirus in the genus Coro- navirus, family Coronaviridae, order Nidovirales
    [Show full text]
  • Comparative Analysis, Distribution, and Characterization of Microsatellites in Orf Virus Genome
    www.nature.com/scientificreports OPEN Comparative analysis, distribution, and characterization of microsatellites in Orf virus genome Basanta Pravas Sahu1, Prativa Majee 1, Ravi Raj Singh1, Anjan Sahoo2 & Debasis Nayak 1* Genome-wide in-silico identifcation of microsatellites or simple sequence repeats (SSRs) in the Orf virus (ORFV), the causative agent of contagious ecthyma has been carried out to investigate the type, distribution and its potential role in the genome evolution. We have investigated eleven ORFV strains, which resulted in the presence of 1,036–1,181 microsatellites per strain. The further screening revealed the presence of 83–107 compound SSRs (cSSRs) per genome. Our analysis indicates the dinucleotide (76.9%) repeats to be the most abundant, followed by trinucleotide (17.7%), mononucleotide (4.9%), tetranucleotide (0.4%) and hexanucleotide (0.2%) repeats. The Relative Abundance (RA) and Relative Density (RD) of these SSRs varied between 7.6–8.4 and 53.0–59.5 bp/ kb, respectively. While in the case of cSSRs, the RA and RD ranged from 0.6–0.8 and 12.1–17.0 bp/kb, respectively. Regression analysis of all parameters like the incident of SSRs, RA, and RD signifcantly correlated with the GC content. But in a case of genome size, except incident SSRs, all other parameters were non-signifcantly correlated. Nearly all cSSRs were composed of two microsatellites, which showed no biasedness to a particular motif. Motif duplication pattern, such as, (C)-x-(C), (TG)- x-(TG), (AT)-x-(AT), (TC)- x-(TC) and self-complementary motifs, such as (GC)-x-(CG), (TC)-x-(AG), (GT)-x-(CA) and (TC)-x-(AG) were observed in the cSSRs.
    [Show full text]
  • The P1N-PISPO Trans-Frame Gene of Sweet Potato Feathery Mottle
    crossmark The P1N-PISPO trans-Frame Gene of Sweet Potato Feathery Mottle Potyvirus Is Produced during Virus Infection and Functions as an RNA Silencing Suppressor Downloaded from Ares Mingot,a Adrián Valli,b Bernardo Rodamilans,c David San León,c David C. Baulcombe,b Juan Antonio García,c Juan José López-Moyaa Center for Research in Agricultural Genomics, CSIC-IRTA-UAB-UB, Cerdanyola del Vallès, Barcelona, Spaina; Department of Plant Sciences, University of Cambridge, Cambridge, United Kingdomb; Centro Nacional de Biotecnología CNB, CSIC, Madrid, Spainc ABSTRACT The positive-sense RNA genome of Sweet potato feathery mottle virus (SPFMV) (genus Potyvirus, family Potyviridae) contains a /large open reading frame (ORF) of 3,494 codons translatable as a polyprotein and two embedded shorter ORFs in the ؊1 frame: http://jvi.asm.org PISPO, of 230 codons, and PIPO, of 66 codons, located in the P1 and P3 regions, respectively. PISPO is specific to some sweet potato-infecting potyviruses, while PIPO is present in all potyvirids. In SPFMV these two extra ORFs are preceded by conserved G2A6 motifs. We have shown recently that a polymerase slippage mechanism at these sites could produce transcripts bringing these ORFs in frame with the upstream polyprotein, thus leading to P1N-PISPO and P3N-PIPO products (B. Rodamilans, A. Valli, A. Mingot, D. San Leon, D. B. Baulcombe, J. J. Lopez-Moya, and J.A. Garcia, J Virol 89:6965–6967, 2015, doi:10.1128/JVI.00 337-15). Here, we demonstrate by liquid chromatography coupled to mass spectrometry that both P1 and P1N-PISPO are produced during viral infection and coexist in SPFMV-infected Ipomoea batatas plants.
    [Show full text]
  • Virus World As an Evolutionary Network of Viruses and Capsidless Selfish Elements
    Virus World as an Evolutionary Network of Viruses and Capsidless Selfish Elements Koonin, E. V., & Dolja, V. V. (2014). Virus World as an Evolutionary Network of Viruses and Capsidless Selfish Elements. Microbiology and Molecular Biology Reviews, 78(2), 278-303. doi:10.1128/MMBR.00049-13 10.1128/MMBR.00049-13 American Society for Microbiology Version of Record http://cdss.library.oregonstate.edu/sa-termsofuse Virus World as an Evolutionary Network of Viruses and Capsidless Selfish Elements Eugene V. Koonin,a Valerian V. Doljab National Center for Biotechnology Information, National Library of Medicine, Bethesda, Maryland, USAa; Department of Botany and Plant Pathology and Center for Genome Research and Biocomputing, Oregon State University, Corvallis, Oregon, USAb Downloaded from SUMMARY ..................................................................................................................................................278 INTRODUCTION ............................................................................................................................................278 PREVALENCE OF REPLICATION SYSTEM COMPONENTS COMPARED TO CAPSID PROTEINS AMONG VIRUS HALLMARK GENES.......................279 CLASSIFICATION OF VIRUSES BY REPLICATION-EXPRESSION STRATEGY: TYPICAL VIRUSES AND CAPSIDLESS FORMS ................................279 EVOLUTIONARY RELATIONSHIPS BETWEEN VIRUSES AND CAPSIDLESS VIRUS-LIKE GENETIC ELEMENTS ..............................................280 Capsidless Derivatives of Positive-Strand RNA Viruses....................................................................................................280
    [Show full text]
  • Aphid Transmission of Potyvirus: the Largest Plant-Infecting RNA Virus Genus
    Supplementary Aphid Transmission of Potyvirus: The Largest Plant-Infecting RNA Virus Genus Kiran R. Gadhave 1,2,*,†, Saurabh Gautam 3,†, David A. Rasmussen 2 and Rajagopalbabu Srinivasan 3 1 Department of Plant Pathology and Microbiology, University of California, Riverside, CA 92521, USA 2 Department of Entomology and Plant Pathology, North Carolina State University, Raleigh, NC 27606, USA; [email protected] 3 Department of Entomology, University of Georgia, 1109 Experiment Street, Griffin, GA 30223, USA; [email protected] * Correspondence: [email protected]. † Authors contributed equally. Received: 13 May 2020; Accepted: 15 July 2020; Published: date Abstract: Potyviruses are the largest group of plant infecting RNA viruses that cause significant losses in a wide range of crops across the globe. The majority of viruses in the genus Potyvirus are transmitted by aphids in a non-persistent, non-circulative manner and have been extensively studied vis-à-vis their structure, taxonomy, evolution, diagnosis, transmission and molecular interactions with hosts. This comprehensive review exclusively discusses potyviruses and their transmission by aphid vectors, specifically in the light of several virus, aphid and plant factors, and how their interplay influences potyviral binding in aphids, aphid behavior and fitness, host plant biochemistry, virus epidemics, and transmission bottlenecks. We present the heatmap of the global distribution of potyvirus species, variation in the potyviral coat protein gene, and top aphid vectors of potyviruses. Lastly, we examine how the fundamental understanding of these multi-partite interactions through multi-omics approaches is already contributing to, and can have future implications for, devising effective and sustainable management strategies against aphid- transmitted potyviruses to global agriculture.
    [Show full text]
  • Molecular Analysis of Vanilla Mosaic Virus from the Cook Islands
    Molecular Analysis of Vanilla mosaic virus from the Cook Islands Christopher Puli’uvea A thesis submitted to Auckland University of Technology in partial fulfilment of the requirements for the degree of Master of Science (MSc) 2017 School of Science I Abstract Vanilla was first introduced to French Polynesia in 1848 and from 1899-1966 was a major export for French Polynesia who then produced an average of 158 tonnes of cured Vanilla tahitensis beans annually. In 1967, vanilla production declined rapidly to a low of 0.6 tonnes by 1981, which prompted a nation-wide investigation with the aim of restoring vanilla production to its former levels. As a result, a mosaic-inducing virus was discovered infecting V. tahitensis that was distinct from Cymbidium mosaic virus (CyMV) and Odontoglossum ringspot virus (ORSV) but serologically related to dasheen mosaic virus (DsMV). The potyvirus was subsequently named vanilla mosaic virus (VanMV) and was later reported to infect V. tahitensis in the Cook Islands and V. planifolia in Fiji and Vanuatu. Attempts were made to mechanically inoculate VanMV to a number of plants that are susceptible to DsMV, but with no success. Based on a partial sequence analysis, VanMV-FP (French Polynesian isolate) and VanMV-CI (Cook Islands isolate) were later characterised as strains of DsMV exclusively infecting vanilla. Since its discovery, little information is known about how VanMV-CI acquired the ability to exclusively infect vanilla and lose its ability to infect natural hosts of DsMV or vice versa. The aims of this research were to characterise the VanMV genome and attempt to determine the molecular basis for host range specificity of VanMV-CI.
    [Show full text]
  • Characterization of a New Potyvirus Causing Mosaic and Flower Variegation in Catharanthus Roseus in Brazil
    New potyvirus causing mosaic and fl ower variegation in C. roseus 687 Note Characterization of a new potyvirus causing mosaic and fl ower variegation in Catharanthus roseus in Brazil Sheila Conceição Maciel1, Ricardo Ferreira da Silva1, Marcelo Silva Reis2, Adriana Salomão Jadão3, Daniel Dias Rosa1, José Segundo Giampan4, Elliot Watanabe Kitajima3, Jorge Alberto Marques Rezende3*, Luis Eduardo Aranha Camargo3 1USP/ESALQ – Programa de Pós-Graduação em Fitopatologia. 2Centro de Citricultura Sylvio Moreira/Bioinformática – 13490-970 – Cordeirópolis, SP – Brasil. 3USP/ESALQ – Depto. de Fitopatologia e Nematologia – C.P. 09 – 13418-900 – Piracicaba, SP – Brasil. 4IAPAR – Área de Proteção de Plantas – C.P. 481 - 86047-902 – Londrina, PR – Brasil. *Corresponding author <[email protected]> Edited by: Luís Reynaldo Ferracciú Alleoni ABSTRACT: Catharanthus roseus is a perennial, evergreen herb in the family Apocynaceae, which is used as ornamental and for popular medicine to treat a wide assortment of human diseases. This paper describes a new potyvirus found causing mosaic symptom, foliar malformation and flower variegation in C. roseus. Of 28 test-plants inoculated mechanically with this potyvirus, only C. roseus and Nicotiana benthamiana developed systemic mosaic, whereas Chenopodium amaranticolor and C. quinoa exhibited chlorotic local lesions. The virus was transmitted by Aphis gossypii and Myzus nicotianae. When the nucleotide sequence of the CP gene (768nt) was compared with other members of the Potyviridae family, the highest identities varied from 67 to 76 %. For the 3' UTR (286nt), identities varied from 16.8 to 28.6 %. The name Catharanthus mosaic virus (CatMV) is proposed for this new potyvirus. Keywords: RT-PCR, Apocynaceae, periwinkle, diagnose, genome sequencing Introduction Cucumis sativus, Cucurbita pepo cv.
    [Show full text]
  • Turnip Mosaic Virus Coat Protein Deletion Mutants Allow Defining Dispensable Protein Domains for ‘In Planta’ Evlp Formation
    viruses Communication Turnip Mosaic Virus Coat Protein Deletion Mutants Allow Defining Dispensable Protein Domains for ‘in Planta’ eVLP Formation Carmen Yuste-Calvo, Pablo Ibort y, Flora Sánchez and Fernando Ponz * Centro de Biotecnología y Genómica de Plantas, Universidad Politécnica de Madrid-Instituto Nacional de Investigación y Tecnología Agraria y Alimentaria (CBGP, UPM-INIA), Campus Montegancedo, Autopista M-40, km 38, Pozuelo de Alarcón, 28223 Madrid, Spain; [email protected] (C.Y.-C.); [email protected] (P.I.); fl[email protected] (F.S.) * Correspondence: [email protected] Present address: R&D Microbiology Department, Koppert Biological Systems, 2651 Berkel en Rodenrijs, y The Netherlands. Received: 28 May 2020; Accepted: 17 June 2020; Published: 19 June 2020 Abstract: The involvement of different structural domains of the coat protein (CP) of turnip mosaic virus, a potyvirus, in establishing and/or maintaining particle assembly was analyzed through deletion mutants of the protein. In order to identify exclusively those domains involved in protein–protein interactions within the particle, the analysis was performed by agroinfiltration “in planta”, followed by the assessment of CP accumulation in leaves and the assembly of virus-like particles lacking nucleic acids, also known as empty virus-like particles (eVLP). Thus, the interactions involving viral RNA could be excluded. It was found that deletions precluding eVLP assembly did not allow for protein accumulation either, probably indicating that non-assembled CP protein was degraded in the plant leaves. Deletions involving the CP structural core were incompatible with particle assembly. On the N-terminal domain, only the deletion avoiding the subdomain involved in interactions with other CP subunits was incorporated into eVLPs.
    [Show full text]
  • Sweetpotato Virus C and Its Contribution to the Potyvirus Complex in Sweetpotato (Ipomoea Batatas) Favio E
    Louisiana State University LSU Digital Commons LSU Doctoral Dissertations Graduate School 11-12-2017 Sweetpotato Virus C and Its Contribution to the Potyvirus Complex in Sweetpotato (Ipomoea batatas) Favio E. Herrera Eguez Louisiana State University and Agricultural and Mechanical College, [email protected] Follow this and additional works at: https://digitalcommons.lsu.edu/gradschool_dissertations Part of the Agricultural Science Commons, Plant Pathology Commons, and the Virology Commons Recommended Citation Herrera Eguez, Favio E., "Sweetpotato Virus C and Its Contribution to the Potyvirus Complex in Sweetpotato (Ipomoea batatas)" (2017). LSU Doctoral Dissertations. 4146. https://digitalcommons.lsu.edu/gradschool_dissertations/4146 This Dissertation is brought to you for free and open access by the Graduate School at LSU Digital Commons. It has been accepted for inclusion in LSU Doctoral Dissertations by an authorized graduate school editor of LSU Digital Commons. For more information, please [email protected]. SWEETPOTATO VIRUS C AND ITS CONTRIBUTION TO THE POTYVIRUS COMPLEX IN SWEETPOTATO (IPOMOEA BATATAS) A Dissertation Submitted to the Graduate Faculty of the Louisiana State University and Agriculture and Mechanical College in partial fulfillment of the requirements for the degree of Doctor of Philosophy in The Department of Plant Pathology and Crop Physiology by Favio E. Herrera Eguez B.S., Pan American School of Agriculture Zamorano, 2010 M.S., Louisiana State University, 2014 December 2017 I To mom and dad, I love you both. ii ACKNOWLEDGEMENTS Thanks to God for giving the health and strength to accomplish (once again) an important step in my life. Thank you very much for my family who supports me from my beloved Ecuador.
    [Show full text]
  • Structure of Flexible Filamentous Plant Virusesᰔ Amy Kendall,1 Michele Mcdonald,1 Wen Bian,1 Timothy Bowles,1 Sarah C
    JOURNAL OF VIROLOGY, Oct. 2008, p. 9546–9554 Vol. 82, No. 19 0022-538X/08/$08.00ϩ0 doi:10.1128/JVI.00895-08 Copyright © 2008, American Society for Microbiology. All Rights Reserved. Structure of Flexible Filamentous Plant Virusesᰔ Amy Kendall,1 Michele McDonald,1 Wen Bian,1 Timothy Bowles,1 Sarah C. Baumgarten,1 Jian Shi,2† Phoebe L. Stewart,2 Esther Bullitt,3 David Gore,4 Thomas C. Irving,4 Wendy M. Havens,5 Said A. Ghabrial,5 Joseph S. Wall,6 and Gerald Stubbs1* Department of Biological Sciences and Center for Structural Biology, Vanderbilt University, Nashville, Tennessee 372351; Department of Molecular Physiology and Biophysics and Center for Structural Biology, Vanderbilt University, Nashville, Tennessee 372322; Department of Physiology and Biophysics, Boston University School of Medicine, Boston, Massachusetts 021183; BioCAT, CSRRI, and BCPS, Illinois Institute of Technology, Chicago, Illinois 604394; Plant Pathology Department, University of Kentucky, Lexington, Kentucky 405465; and Biology Department, Brookhaven National Laboratory, Upton, New York 119736 Received 29 April 2008/Accepted 17 July 2008 Flexible filamentous viruses make up a large fraction of the known plant viruses, but in comparison with those of other viruses, very little is known about their structures. We have used fiber diffraction, cryo-electron microscopy, and scanning transmission electron microscopy to determine the symmetry of a potyvirus, soybean mosaic virus; to confirm the symmetry of a potexvirus, potato virus X; and to determine the low-resolution structures of both viruses. We conclude that these viruses and, by implication, most or all flexible filamentous plant viruses share a common coat protein fold and helical symmetry, with slightly less than 9 subunits per helical turn.
    [Show full text]
  • Synthetic Viruses Risks and Benefits
    NSABB: Synthetic Viruses Risks and Benefits Objectives Virus Biothreat Lists Virus Classification Baltimore Scheme Virus Reverse Genetic Strategies Reverse Genetics and Synthetic Genomics Technical Barriers to Synthetic Genome Reconstruction Chimeras and Synthetic Viruses Summary Goal: Provide a theoretical framework to initiate a broad discussion regarding the relative risks and benefits of synthetic genome technology Biothreat Viruses HHS/CDC, USDA, Dept Commerce, NIH Category A-C (Lists of Biothreat Viruses) Very Heterogeneous group of viruses HHS/CDC, USDA, Dept Commerce (Lists of Biothreat Viruses) Different genome organizations + replication strategies different approaches are needed to develop infectious genomes Genomes dsDNA, ssRNA (+) polarity, ssRNA (-) polarity and dsRNA Simple classification scheme to understand virus reverse genetic strategies All viruses must transcribe genome into mRNA viral proteins. Baltimore Classification Scheme (Mix) mRNA dsDNA ssDNA (Group VI) (Group I) (Group II) Transcription (Not Infectious) (Not Infectious) dsRNA mRNA ssRNA (-) (Group III) (Group IV) (Group V) (Infectious) Translation Protein Genome Infectious?: Ability to induce mRNA expression and recover virus after injection of the genome into a cell Figure 1. Baltimore Classification Scheme. Baltimore Classification Scheme reverse transcription DNA Synthesis mRNA dsDNA ssDNA (Group VI) (Group I) (Group II) Transcription viral replicase and viral replicase and accessory proteins accessory proteins dsRNA mRNA ssRNA (-) (Group
    [Show full text]
  • RNA Sequence of Astrovirus: Distinctive Genomic Organization and a Putative Retrovirus-Like Ribosomal Frameshifting Signal That Directs the Viral Replicase Synthesis
    Proc. Natl. Acad. Sci. USA Vol. 90, pp. 10539-10543, November 1993 Microbiology RNA sequence of astrovirus: Distinctive genomic organization and a putative retrovirus-like ribosomal frameshifting signal that directs the viral replicase synthesis BAOMING JIANG*t, STEPHAN S. MONROE*, EUGENE V. KOONINt, SARAH E. STINE*, AND ROGER I. GLASS* *Viral Gastroenteritis Section, Centers for Disease Control and Prevention, Atlanta, GA 30333; and tNational Center for Biotechnology Information, National Institutes of Health, Bethesda, MD 20894 Communicated by Bernard Fields, July 27, 1993 ABSTRACT The genomic RNA of human astrovirus was In the present study, we have sequenced and analyzed the sequenced and found to contain 6797 nt organized into three entire genomic RNA of H-Ast2§ and compared the sequence open reading frames (la, lb, and 2). A potential ribosomal and genomic structure with those of other positive-strand frameshift site identified in the overlap region of open reading RNA viruses. The results highlight the specific genomic frames la and lb consists ofa "shifty" heptanucleotide and an organization of astroviruses and support their classification RNA stem-loop structure that closely resemble those at the in a separate virus family. gag-pro junction of some retroviruses. This translation frame- shift may result in the suppression of in-frame amber termi- nation at the end of open reading frame la and the synthesis of MATERIALS AND METHODS a nonstructural, fusion polyprotein that contains the putative Cells and Virus. LLCMK2 cells (ATCC CCL 7.1) were protease and RNA-dependent RNA polymerase. Comparative propagated in Earle's minimal essential medium (MEM) sequence analysis indicated that the protease and polymerase of supplemented with antibiotics-and 10% fetal bovine serum.
    [Show full text]