Retroviral RNA Nuclear Export Elements Regulate Protein Function and Viral Assembly

Retroviral RNA Nuclear Export Elements Regulate Protein Function and Viral Assembly PDF Author: Chad Michael Swanson
Publisher:
ISBN:
Category :
Languages : en
Pages : 181

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Retroviral RNA Nuclear Export Elements Regulate Protein Function and Viral Assembly

Retroviral RNA Nuclear Export Elements Regulate Protein Function and Viral Assembly PDF Author: Chad Michael Swanson
Publisher:
ISBN:
Category :
Languages : en
Pages : 181

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Book Description


Nuclear Export of Viral RNAs

Nuclear Export of Viral RNAs PDF Author: J. Hauber
Publisher: Springer Science & Business Media
ISBN: 3642565972
Category : Science
Languages : en
Pages : 148

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Book Description
In eukaryotic cells, the nuclear genome and its transcriptional apparatus is separated from the site of protein synthesis by the nuclear envelope. Thus, a constant flow of proteins and nucleic acids has to cross the nuclear envelope in both directions. This transport in and out of the nucleus is mediated by nuclear pore complexes (NPCs) and occurs in an energy and signal-dependent manner. Thus, nucleocytoplasmic translocation of macro molecules across the nuclear envelope appears to be a highly specific and regulated process. Viruses that replicate their genome in the cell nucleus are therefore forced to develop efficient ways to deal with the intracellulZlr host cell transport machinery. Historically, investigation of Polyomavirus replication allowed identification ofsequences that mediate nuclear import, which led subsequently to our detailed understanding of the cellular factors that are involved in nuclear import. Transport ofmacromolecules in the opposite direction, however, is less well understood. The investigation of retroviral gene expression in recent years pro vided the first insights into the cellular mechanisms that regulate nuclear export. In particular, the detailed dissection of the function of the human immunodeficiency virus type I (HIV-I) Rev trans-activator protein identified CRMI, as a hona fide nuclear export receptor. CRM I appears to be involved in the nucleocytoplasmic translocation of the vast majority of viral and cellular proteins that have subsequently been found to contain a Rev-type leucine-rich nuclear export signal (NES).

Retroviruses

Retroviruses PDF Author: John M. Coffin
Publisher: CSHL Press
ISBN: 9780879695712
Category : Electronic books
Languages : en
Pages : 856

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Book Description
For over 25 years the study of retroviruses has underpinned much of what is known about information transfer in cells and the genetic and biochemical mechanisms that underlie cell growth and cancer induction. Emergent diseases such as AIDS and adult T-cell lymphoma have widened even further the community of investigators directly concerned with retroviruses, a development that has highlighted the need for an integrated understanding of their biology and their unique association with host genomes. This remarkable volume satisfies that need. Written by a group of the field's most distinguished investigators, rigorously edited to provide a seamless narrative, and elegantly designed for clarity and readability, this book is an instant classic that demands attention from scientists and physicians studying retroviruses and the disorders in which they play a role.

Human Herpesviruses

Human Herpesviruses PDF Author: Ann Arvin
Publisher: Cambridge University Press
ISBN: 1139461648
Category : Medical
Languages : en
Pages : 1325

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Book Description
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.

Molecular Biology of the Cell

Molecular Biology of the Cell PDF Author:
Publisher:
ISBN: 9780815332183
Category : Cells
Languages : en
Pages : 0

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Regulation of RNA Metabolism by HIV-1 Rev

Regulation of RNA Metabolism by HIV-1 Rev PDF Author: Lia H. Campbell
Publisher:
ISBN:
Category :
Languages : en
Pages : 216

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Identification and Characterization of a Cellular Protein Involved in the Post-transcriptional Regulation of Retroviruses

Identification and Characterization of a Cellular Protein Involved in the Post-transcriptional Regulation of Retroviruses PDF Author: Hengli Tang
Publisher:
ISBN:
Category :
Languages : en
Pages : 242

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Conserved CIS-acting RNA Elements Regulate the Post-transcriptional Utilization of Retroviral and Cellular RNAs

Conserved CIS-acting RNA Elements Regulate the Post-transcriptional Utilization of Retroviral and Cellular RNAs PDF Author: Nicole M. Placek
Publisher:
ISBN:
Category : Cellular control mechanisms
Languages : en
Pages : 156

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Book Description
Abstract: Both retroviruses and cellular genes rely on post-transcriptional mechanisms to regulate the timing and abundance of their protein product. The post-transcriptional control element (PCE) has been identified in the 5' untranslated regions of mRNAs from selected retroviruses and the cellular gene JunD. PCE containing mRNAs rely on the DExH/D box helicase RNA helicase A (RHA) to specifically facilitate robust synthesis of their protein product. Study of retroviruses has developed approaches to understand both cellular control of gene expression and the dyregulation that contributes to cancer and immunodeficiency. JunD, a member of the activator protein -1 (AP-1) family of transcription factors, is important for transcriptional regulation of growth control genes. Dysregulation of JunD is implicated in cancer and metabolic disease via defects in cell- proliferation and disease-associated apoptosis and can also modulate viral persistence. Studies described here build on the previous characterization of SNV and JunD PCE function in HIV gag-pol reporter plasmids and investigate the parental SNV provirus. The results presented validate the role of PCE in combination with a newly identified a distal element, designated the I,II element, in regulation of balanced expression and translational utilization of SNV mRNA. A key conclusion is that PCE and the distal I,II element comprise a bipartite element that interacts with RNA helicase A to selectively modulate post-transcriptional expression of the unspliced SNV gag mRNA. This thesis also reviews the current and historical literature of JunD gene regulation. Three core areas are described and intriguing essential issues are discussed: i) transcription regulation by AP-1 complexes containing JunD protein, ii) post-translational modification of JunD by Jun-terminal kinase (Jnk) and protein:protein interactions, and iii) regulation of translation intiation by JunD PCE. Lessons learned from the study of retrovirus genes have produced essential knowledge of the JunD transcription factor and contributed to the characterization of a novel axis of transational control of complex RNAs.

Identification and Characterization of New and Distinct Functional Roles of Posttranscriptional Control Elements in Cytoplasmic Expression of Retroviral Rna

Identification and Characterization of New and Distinct Functional Roles of Posttranscriptional Control Elements in Cytoplasmic Expression of Retroviral Rna PDF Author: Stacey Lynn Hull
Publisher:
ISBN:
Category : RNA viruses
Languages : en
Pages :

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Book Description
Abstract: The central focus of this dissertation is the identification and characterization of retroviral posttranscriptional control elements that affect protein production from unspliced viral RNA. We identify and characterize a new posttranscriptional control element in the Mason-Pfizer monkey virus 52 long terminal repeat (LTR) that modulates translational efficiency by augmentation of translational initiation. MPMV RU5 is necessary for cytoplasmic expression of HIV-1 gag-pol reporter RNA and also enhances cytoplasmic expression of intronless luc RNA by stimulation of ribosome loading. MPMV RU5 functions independently of any viral proteins and instead directs functional interaction with cellular posttranscriptional modulators to facilitate translational enhancement. This research has illuminated an essential step in viral gene expression and provides a new paradigm for understanding cellular control of the translation process. Secondly, we tested the hypothesis that combination of the MPMV constitutive transport element (CTE) and the MPMV or spleen necrosis virus (SNV) RU5 translational enhancer on a single RNA synergistically augments posttranscriptional gene expression. MPMV CTE functions compatibly with MPMV and SNV RU5 to increase cytoplasmic expression of HIV-1 gag-pol reporter RNA in monkey COS, but not 293 cells. The CTE-interactive cellular proteins, Tap and NXT1, are necessary and sufficient to rescue increased cytoplasmic expression of HIV-1 gag-pol reporter RNA in 293 cells. This work produced the realization that differences in cellular posttranscriptional modulators dramatically affect retroviral protein production. Thirdly, we evaluated the role of SNV RU5 on metabolism of homologous SNV RNA. SNV RU5 increases SNV Gag-GFP fusion protein production from unspliced genomic RNA. The increase in protein is attributable, at least in part, to increased cytoplasmic accumulation of the unspliced SNV transcript. RU5 exerts a distinct effect on the spliced env transcript. Deletion of RU5 has no effect on cytoplasmic accumulation of env RNA, but increases splicing efficiency. Therefore, SNV RU5 modulates metabolism of both unspliced and spliced SNV transcripts and is speculated to contain a RNA splicing suppressor. In summary, this dissertation has identified and characterized a new posttranscriptional control element in MPMV and synergistic interactions among functionally distinct retroviral posttranscriptional control elements and their cellular protein partners. This work also demonstrated an important role for SNV RU5 in SNV genomic RNA.

Human Retroviruses

Human Retroviruses PDF Author: Bryan Cullen
Publisher: Oxford University Press
ISBN: 9780199633821
Category : Gene Expression Regulation.
Languages : en
Pages : 220

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Book Description
The first book to specifically cover the molecular biology of retroviruses - of immense importance since the high profile of HIV. International contributors provide detailed reviews of the latest knowledge. An excellent text for both medical and non-medical researchers, it also serves as an illuminating introduction for scientists active in other areas.