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Post-transcriptional Regulation of HIV-1 Asp: Potential Control by a Series of Short Open Reading Frames

Post-transcriptional Regulation of HIV-1 Asp: Potential Control by a Series of Short Open Reading Frames
Author: Michael Salvatore Barbagallo
Publisher:
Total Pages: 426
Release: 2013
Genre:
ISBN:

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The positive sense strand of the HIV-1 genome encodes nine different proteins. These include structural proteins (Gag, Pol and Env), regulatory proteins (Tat and Rev) as well as accessory proteins (Vpu, Vpr, Vif and Nef). In addition to the nine positive sense genes, a negative sense gene, asp, has been identified opposite in orientation to env. Bioinformatic analyses suggest that asp encodes a hydrophobic, membrane associated protein of 189 aa. Negative sense transcription, regulated by LTR sequences, has been observed early in HIV-1 infection in vitro. However the mechanism of asp expression and function of the putative ASP protein still remain unclear. In some viral strains a series of six short open reading frames (sORFs) positioned upstream of the asp gene have the potential to regulate asp expression. This thesis examines the role of these sORFs in control of expression of downstream genes. All subtypes of HIV-1 were examined to detect the negative sense asp ORF, and to identify potential regulatory sequences. A series of strongly conserved upstream sORFs was identified. The sORF series was particularly well conserved amongst the A, B, C and D clade strains with sORFs I, V and VI being highly conserved across all the subtypes examined. This potential control region from HIV-1NL4-3, containing six sORFs, was cloned upstream of the reporter gene EGFP. Expression by transfection of HEK293 cells indicated that the introduction of this sORF region inhibits EGFP reporter expression; analysis of transcripts revealed no significant change in levels of EGFP mRNA, suggesting that regulation occurs post-transcription. RT-PCR analysis of transcripts further demonstrated that the upstream sORF region undergoes alternative splicing in vitro. The most abundant product (Spliced Variant 1) is spliced to remove sORFs I to V, leaving only the in-frame sORF VI. Sequence analysis revealed the presence and high conservation of typical splice donor and acceptor site motifs. Spliced Variant 2, containing sORFs I, II and VI; utilised a lesser well conserved donor in conjunction with the splice acceptor common to Spliced Variant 1. Cloning of Spliced Variant 2 enabled the detection of a third product, Spliced Variant 3. This Spliced Variant (3) presented an alternate initiation codon for sORF VI, designated VIalt. While Spliced Variants 1 and 2 inhibited, to varying extents, downstream expression; Spliced Variant 3 permitted expression. Mutation of the highly conserved splice donor and acceptor sites modulates, but does not fully relieve, inhibition of reporter EGFP production. These data were further supported by sequential mutation of the sORF initiation codons in which, to varying levels, each mutation alleviated the inhibitory nature of the sORF series, suggesting a translational mechanism for the control of asp expression. Toeprinting analysis of the sORF region also revealed the potential for ribosomes to initiate at sORFs I, II, IV, VI and VIalt, yet only weak toeprints were observed for sORF III and sORF V. Initiation at a cryptic CUG codon located 14 nucleotides downstream from sORF VIalt was also detected. These data suggest that the leaky scanning and/or termination reinitiation mechanisms of translation account for the mode of translation across the sORF transcript, and that sORF VI, alone, inhibits downstream translation. Upstream sORFs engage the ribosome, facilitating subsequent initiation downstream at sORF VI. Alternative splicing determines the presence or absence of upstream sORFs, therefore the efficiency of recognition of the sORF VI initiation codon and the degree of inhibition of downstream gene expression. These findings suggest a complex mechanism, involving both splicing and translational control, modulate asp gene expression. The strong conservation of asp and its sORFs across all HIV-1 subtypes suggests that the asp gene product may have a role in the pathogenesis of HIV-1 and requires tight regulation. This study promotes further examination of the negative sense transcript and its function in the HIV-1 viral life cycle.


The Epstein-Barr Virus

The Epstein-Barr Virus
Author: M. A. Epstein
Publisher: Springer Science & Business Media
Total Pages: 467
Release: 2012-12-06
Genre: Medical
ISBN: 3642672361

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The Epstein-Barr virus was discovered 15 years ago. Since that time an immense body of information has been accumu lated on this agent which has come to assume great signifi cance in many different fields of biological science. Thus, the virus has very special relevance in human medicine and oncology, in tumor virology, in immunology, and in mole cular virology, since it is the cause of infectious mononu cleosis and also the first human cancer virus, etiologically related to endemic Burkitt's lymphoma and probably to nasopharyngeal carcinoma. In addition, continuous human lymphoid cell lines initiated and maintained by the transform ing function of the virus genome provide a laboratory tool with wide and ever-growing applications. Innumerable papers on the Epstein-Barr virus have ap peared over recent years and reports of work with this agent now constitute a veritable flood. The present book provides the first and only comprehensive, authoritative over-view of all aspects of the virus by authors who have been the original and major contributors in their particular disciplines. A complete and up-to-date survey of this unique and important agent is thus provided which should be of great interest to experts, teachers, and students engaged in cancer research, virology, immunology, molecular biology, epide miology, and cell culture. Where topics have been dealt with from more than one of these viewpoints, some inevitable overlap and duplication has resulted; although this has been kept to a minimum, it has been retained in some places because of positive usefulness.


Human Herpesviruses

Human Herpesviruses
Author: Ann Arvin
Publisher: Cambridge University Press
Total Pages: 1325
Release: 2007-08-16
Genre: Medical
ISBN: 1139461648

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This comprehensive account of the human herpesviruses provides an encyclopedic overview of their basic virology and clinical manifestations. This group of viruses includes human simplex type 1 and 2, Epstein–Barr virus, Kaposi's Sarcoma-associated herpesvirus, cytomegalovirus, HHV6A, 6B and 7, and varicella-zoster virus. The viral diseases and cancers they cause are significant and often recurrent. Their prevalence in the developed world accounts for a major burden of disease, and as a result there is a great deal of research into the pathophysiology of infection and immunobiology. Another important area covered within this volume concerns antiviral therapy and the development of vaccines. All these aspects are covered in depth, both scientifically and in terms of clinical guidelines for patient care. The text is illustrated generously throughout and is fully referenced to the latest research and developments.


Epstein Barr Virus Volume 1

Epstein Barr Virus Volume 1
Author: Christian Münz
Publisher: Springer
Total Pages: 0
Release: 2015-10-12
Genre: Medical
ISBN: 9783319228211

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Epstein Barr virus (EBV) was discovered as the first human tumor virus around 50 years ago. Since its discovery in Burkitt’s lymphoma it has been associated with various other malignancies, infectious mononucleosis and even autoimmune diseases. The two book volumes on EBV summarize the first 50 years of research on this tumor virus, starting with historical perspectives on discovery, oncogenicity and immune control, reviewing the role that the virus plays in the various associated diseases and concluding with a discussion on how the immune system keeps persistent EBV infection under control in healthy EBV carriers and can be used to treat EBV associated diseases. The respective 32 chapters are written by international experts from three continents for health care providers, biomedical researchers and patients that are affected by EBV. The assembled knowledge should help to understand EBV associated diseases better and to develop EBV specific vaccination in the near future.


Stress-Activated Protein Kinases

Stress-Activated Protein Kinases
Author: Francesc Posas
Publisher: Springer Science & Business Media
Total Pages: 322
Release: 2008-01-24
Genre: Science
ISBN: 3540755691

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In this book leading researchers in the field discuss the state-of-the-art of many aspects of SAPK signaling in various systems from yeast to mammals. These include various chapters on regulatory mechanisms as well as the contribution of the SAPK signaling pathways to processes such as gene expression, metabolism, cell cycle regulation, immune responses and tumorigenesis. Written by international experts, the book will appeal to cell biologists and biochemists.


The CMS Hospital Conditions of Participation and Interpretive Guidelines

The CMS Hospital Conditions of Participation and Interpretive Guidelines
Author:
Publisher:
Total Pages: 546
Release: 2017-11-27
Genre:
ISBN: 9781683086857

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In addition to reprinting the PDF of the CMS CoPs and Interpretive Guidelines, we include key Survey and Certification memos that CMS has issued to announced changes to the emergency preparedness final rule, fire and smoke door annual testing requirements, survey team composition and investigation of complaints, infection control screenings, and legionella risk reduction.


HIV-1 Latency

HIV-1 Latency
Author: Guido Silvestri
Publisher: Springer
Total Pages: 253
Release: 2018-10-11
Genre: Medical
ISBN: 303002816X

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This volume summarizes recent advances in understanding the mechanisms of HIV-1 latency, in characterizing residual viral reservoirs, and in developing targeted interventions to reduce HIV-1 persistence during antiretroviral therapy. Specific chapters address the molecular mechanisms that govern and regulate HIV-1 transcription and latency; assays and technical approaches to quantify viral reservoirs in humans and animal models; the complex interchange between viral reservoirs and the host immune system; computational strategies to model viral reservoir dynamics; and the development of therapeutic approaches that target viral reservoir cells. With contributions from an interdisciplinary group of investigators that cover a broad spectrum of subjects, from molecular virology to proof-of-principle clinical trials, this book is a valuable resource for basic scientists, translational investigators, infectious-disease physicians, individuals living with HIV/AIDS and the general public.


Sequence — Evolution — Function

Sequence — Evolution — Function
Author: Eugene V. Koonin
Publisher: Springer Science & Business Media
Total Pages: 482
Release: 2013-06-29
Genre: Science
ISBN: 1475737831

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Sequence - Evolution - Function is an introduction to the computational approaches that play a critical role in the emerging new branch of biology known as functional genomics. The book provides the reader with an understanding of the principles and approaches of functional genomics and of the potential and limitations of computational and experimental approaches to genome analysis. Sequence - Evolution - Function should help bridge the "digital divide" between biologists and computer scientists, allowing biologists to better grasp the peculiarities of the emerging field of Genome Biology and to learn how to benefit from the enormous amount of sequence data available in the public databases. The book is non-technical with respect to the computer methods for genome analysis and discusses these methods from the user's viewpoint, without addressing mathematical and algorithmic details. Prior practical familiarity with the basic methods for sequence analysis is a major advantage, but a reader without such experience will be able to use the book as an introduction to these methods. This book is perfect for introductory level courses in computational methods for comparative and functional genomics.


The HLA FactsBook

The HLA FactsBook
Author: Steven G.E. Marsh
Publisher: Elsevier
Total Pages: 413
Release: 1999-12-13
Genre: Medical
ISBN: 0080542506

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The HLA FactsBook presents up-to-date and comprehensive information on the HLA genes in a manner that is accessible to both beginner and expert alike. The focus of the book is on the polymorphic HLA genes (HLA-A, B, C, DP, DQ, and DR) that are typed for in clinical HLA laboratories. Each gene has a dedicated section in which individual entries describe the structure, functions, and population distribution of groups of related allotypes. Fourteen introductory chapters provide a beginner's guide to the basic structure, function, and genetics of the HLA genes, as well as to the nomenclature and methods used for HLA typing. This book will be an invaluable reference for researchers studying the human immune response, for clinicians and laboratory personnel involved in clinical and forensic HLA typing, and for human geneticists, population biologists, and evolutionary biologists interested in HLA genes as markers of human diversity. Introductory chapters provide good general overview of HLA field for novice immunologists and geneticists Up-to-date, complete listing of HLA alleles Invaluable reference resource for immunologists, geneticists, and cell biologists Combines both structural and functional information, which has never been compiled in a single reference book previously Serological specificity of allotypes Identity of material sequenced including ethnic origin Database accession numbers Population distribution Peptide binding specificities T cell epitopes Amino acid sequences of allotypes Key references


Registries for Evaluating Patient Outcomes

Registries for Evaluating Patient Outcomes
Author: Agency for Healthcare Research and Quality/AHRQ
Publisher: Government Printing Office
Total Pages: 385
Release: 2014-04-01
Genre: Medical
ISBN: 1587634333

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This User’s Guide is intended to support the design, implementation, analysis, interpretation, and quality evaluation of registries created to increase understanding of patient outcomes. For the purposes of this guide, a patient registry is an organized system that uses observational study methods to collect uniform data (clinical and other) to evaluate specified outcomes for a population defined by a particular disease, condition, or exposure, and that serves one or more predetermined scientific, clinical, or policy purposes. A registry database is a file (or files) derived from the registry. Although registries can serve many purposes, this guide focuses on registries created for one or more of the following purposes: to describe the natural history of disease, to determine clinical effectiveness or cost-effectiveness of health care products and services, to measure or monitor safety and harm, and/or to measure quality of care. Registries are classified according to how their populations are defined. For example, product registries include patients who have been exposed to biopharmaceutical products or medical devices. Health services registries consist of patients who have had a common procedure, clinical encounter, or hospitalization. Disease or condition registries are defined by patients having the same diagnosis, such as cystic fibrosis or heart failure. The User’s Guide was created by researchers affiliated with AHRQ’s Effective Health Care Program, particularly those who participated in AHRQ’s DEcIDE (Developing Evidence to Inform Decisions About Effectiveness) program. Chapters were subject to multiple internal and external independent reviews.