Your search keyword '"Hennig, Thomas"' showing total 6 results

1. Mechanism and consequences of herpes simplex virus 1-mediated regulation of host mRNA alternative polyadenylation.

Author

Wang, Xiuye, Liu, Liang, Whisnant, Adam W., Hennig, Thomas, Djakovic, Lara, Haque, Nabila, Bach, Cindy, Sandri-Goldin, Rozanne M., Erhard, Florian, Friedel, Caroline C., Dölken, Lars, and Shi, Yongsheng

Subjects

HERPES simplex virus, RNA polymerase II, VIRUS diseases, GENES, HERPES simplex

Abstract

Eukaryotic gene expression is extensively regulated by cellular stress and pathogen infections. We have previously shown that herpes simplex virus 1 (HSV-1) and several cellular stresses cause widespread disruption of transcription termination (DoTT) of RNA polymerase II (RNAPII) in host genes and that the viral immediate early factor ICP27 plays an important role in HSV-1-induced DoTT. Here, we show that HSV-1 infection also leads to widespread changes in alternative polyadenylation (APA) of host mRNAs. In the majority of cases, polyadenylation shifts to upstream poly(A) sites (PAS), including many intronic PAS. Mechanistically, ICP27 contributes to HSV-1-mediated APA regulation. HSV-1- and ICP27-induced activation of intronic PAS is sequence-dependent and does not involve general inhibition of U1 snRNP. HSV1-induced intronic polyadenylation is accompanied by early termination of RNAPII. HSV-1-induced mRNAs polyadenylated at intronic PAS (IPA) are exported into the cytoplasm while APA isoforms with extended 3' UTRs are sequestered in the nuclei, both preventing the expression of the full-length gene products. Finally we provide evidence that HSV-induced IPA isoforms are translated. Together with other recent studies, our results suggest that viral infection and cellular stresses induce a multi-faceted host response that includes DoTT and changes in APA profiles. Author summary: Viral infections profoundly alter host cell gene expression. It is important to understand both how viruses hijack the host cell machineries to express their own genes and how host cells respond to viral infection for defense. We have previously shown that herpes simplex virus-1 (HSV-1) blocks host cell transcription termination, at least in part, through the viral immediate early protein ICP27. Here we show that HSV-1 infection also alters mRNA 3' end formation and promotes the formation of truncated mRNAs. Some of these aberrant mRNAs are exported into the cytoplasm and translated. This viral activity requires ICP27 and other viral factors. Our study, together with other recent reports, suggests that viral infections and cellular stress elicit similar responses in mammalian cells. [ABSTRACT FROM AUTHOR]

Published

2021

2. Integrative functional genomics decodes herpes simplex virus 1.

Author

Whisnant, Adam W., Jürges, Christopher S., Hennig, Thomas, Wyler, Emanuel, Prusty, Bhupesh, Rutkowski, Andrzej J., L'hernault, Anne, Djakovic, Lara, Göbel, Margarete, Döring, Kristina, Menegatti, Jennifer, Antrobus, Robin, Matheson, Nicholas J., Künzig, Florian W. H., Mastrobuoni, Guido, Bielow, Chris, Kempa, Stefan, Liang, Chunguang, Dandekar, Thomas, and Zimmer, Ralf

Subjects

HERPES simplex virus, FUNCTIONAL genomics, CYTOSKELETAL proteins, VIRAL genes, DATA integration

Abstract

The predicted 80 open reading frames (ORFs) of herpes simplex virus 1 (HSV-1) have been intensively studied for decades. Here, we unravel the complete viral transcriptome and translatome during lytic infection with base-pair resolution by computational integration of multi-omics data. We identify a total of 201 transcripts and 284 ORFs including all known and 46 novel large ORFs. This includes a so far unknown ORF in the locus deleted in the FDA-approved oncolytic virus Imlygic. Multiple transcript isoforms expressed from individual gene loci explain translation of the vast majority of ORFs as well as N-terminal extensions (NTEs) and truncations. We show that NTEs with non-canonical start codons govern the subcellular protein localization and packaging of key viral regulators and structural proteins. We extend the current nomenclature to include all viral gene products and provide a genome browser that visualizes all the obtained data from whole genome to single-nucleotide resolution. Here, using computational integration of multi-omics data, the authors provide a detailed transcriptome and translatome of herpes simplex virus 1 (HSV-1), including previously unidentified ORFs and N-terminal extensions. The study also provides a HSV-1 genome browser and should be a valuable resource for further research. [ABSTRACT FROM AUTHOR]

Published

2020

3. Herpes simplex virus blocks host transcription termination via the bimodal activities of ICP27.

Author

Wang, Xiuye, Hennig, Thomas, Whisnant, Adam W., Erhard, Florian, Prusty, Bhupesh K., Friedel, Caroline C., Forouzmand, Elmira, Hu, William, Erber, Luke, Chen, Yue, Sandri-Goldin, Rozanne M., Dölken, Lars, and Shi, Yongsheng

Subjects

HERPES simplex virus, RNA polymerase II, HERPES simplex, TRANSGENIC organisms, VIRUS diseases

Abstract

Infection by viruses, including herpes simplex virus-1 (HSV-1), and cellular stresses cause widespread disruption of transcription termination (DoTT) of RNA polymerase II (RNAPII) in host genes. However, the underlying mechanisms remain unclear. Here, we demonstrate that the HSV-1 immediate early protein ICP27 induces DoTT by directly binding to the essential mRNA 3' processing factor CPSF. It thereby induces the assembly of a dead-end 3' processing complex, blocking mRNA 3' cleavage. Remarkably, ICP27 also acts as a sequence-dependent activator of mRNA 3' processing for viral and a subset of host transcripts. Our results unravel a bimodal activity of ICP27 that plays a key role in HSV-1-induced host shutoff and identify CPSF as an important factor that mediates regulation of transcription termination. These findings have broad implications for understanding the regulation of transcription termination by other viruses, cellular stress and cancer. Herpes simplex virus-1 (HSV-1) infection disrupts transcription termination (DoTT) of host genes, but underlying mechanisms are unclear. Here, Wang et al. show that the HSV-1 immediate early protein ICP27 induces DoTT through interaction with the mRNA 3' processing factor CPSF and disruption of the processing complex. [ABSTRACT FROM AUTHOR]

Published

2020

4. A Review of the Multipronged Attack of Herpes Simplex Virus 1 on the Host Transcriptional Machinery.

Author

Hennig, Thomas, Djakovic, Lara, Dölken, Lars, and Whisnant, Adam W.

Subjects

*HERPES simplex virus, *RNA synthesis, *RNA polymerases, *VIRAL proteins, *VIRAL genes, *HISTONES

Abstract

During lytic infection, herpes simplex virus (HSV) 1 induces a rapid shutoff of host RNA synthesis while redirecting transcriptional machinery to viral genes. In addition to being a major human pathogen, there is burgeoning clinical interest in HSV as a vector in gene delivery and oncolytic therapies, necessitating research into transcriptional control. This review summarizes the array of impacts that HSV has on RNA Polymerase (Pol) II, which transcribes all mRNA in infected cells. We discuss alterations in Pol II holoenzymes, post-translational modifications, and how viral proteins regulate specific activities such as promoter-proximal pausing, splicing, histone repositioning, and termination with respect to host genes. Recent technological innovations that have reshaped our understanding of previous observations are summarized in detail, along with specific research directions and technical considerations for future studies. [ABSTRACT FROM AUTHOR]

Published

2021

5. Herpes simplex virus 1 inhibits phosphorylation of RNA polymerase II CTD serine-7.

Author

Whisnant, Adam W., Dionisi, Oliver Dyck, Sanchez, Valeria Salazar, Rappold, Julia M., Djakovic, Lara, Grothey, Arnhild, Marante, Ana Luiza, Fischer, Patrick, Shitao Peng, Wolf, Katharina, Hennig, Thomas, and Dölken, Lars

Subjects

*HUMAN herpesvirus 1, *RNA polymerase II, *VIRAL proteins, *HERPES simplex virus, *GENE expression

Abstract

Transcriptional activity of RNA polymerase II (Pol II) is influenced by post-translational modifications of the C-terminal domain (CTD) of the largest Pol II subunit, RPB1. Herpes simplex virus type 1 (HSV-1) usurps the cellular transcriptional machinery during lytic infection to efficiently express viral mRNA and shut down host gene expression. The viral immediate-early protein ICP22 interferes with serine 2 phosphorylation (pS2) by targeting CDK9 and other CDKs, but the full functional implications of this are not well understood. Using Western blotting, we report that HSV-1 also induces a loss of serine 7 phosphorylation (pS7) of the CTD during lytic infection, requiring expression of the two immediate-early proteins ICP22 and ICP27. ICP27 has also been proposed to target RPB1 for degradation, but we show that pS2/S7 loss precedes the drop in total protein levels. Cells with the RPB1 polyubiquitination site mutation K1268R, preventing proteasomal degradation during transcription-coupled DNA repair, displayed loss of pS2/S7 but retained higher overall RPB1 protein levels later in infection, indicating this pathway is not involved in early CTD dysregulation but may mediate bulk protein loss later. Using α-amanitin-resistant CTD mutants, we observed differential requirements for Ser2 and Ser7 for the production of viral proteins, with Ser2 facilitating viral immediate-early genes and Ser7 appearing dispensable. Despite dysregulation of CTD phosphorylation and different requirements for Ser2/7, all CTD modifications tested could be visualized in viral replication compartments with immunofluorescence. These data expand the known means that HSV employs to create pro-viral transcriptional environments at the expense of host responses. [ABSTRACT FROM AUTHOR]

Published

2024

6. Dissecting Herpes Simplex Virus 1-Induced Host Shutoff at the RNA Level.

Author

Friedel, Caroline C., Whisnant, Adam W., Djakovic, Lara, Rutkowski, Andrzej J., Friedl, Marie-Sophie, Kluge, Michael, Williamson, James C., Sai, Somesh, Vidal, Ramon Oliveira, Sauer, Sascha, Hennig, Thomas, Grothey, Arnhild, Milic, Andrea, Prusty, Bhupesh K., Lehner, Paul J., Matheson, Nicholas J., Erhard, Florian, and Dölken, Lars

Subjects

*HERPES simplex virus, *RNA metabolism, *INTEGRINS, *RNA, *DNA replication, *EXTRACELLULAR matrix

Abstract

Herpes simplex virus 1 (HSV-1) induces a profound host shutoff during lytic infection. The virion host shutoff (vhs) protein plays a key role in this process by efficiently cleaving host and viral mRNAs. Furthermore, the onset of viral DNA replication is accompanied by a rapid decline in host transcriptional activity. To dissect relative contributions of both mechanisms and elucidate gene-specific host transcriptional responses throughout the first 8 h of lytic HSV-1 infection, we used transcriptome sequencing of total, newly transcribed (4sU-labeled) and chromatinassociated RNA in wild-type (WT) and Δvhs mutant infection of primary human fibroblasts. Following virus entry, vhs activity rapidly plateaued at an elimination rate of around 30% of cellular mRNAs per hour until 8 h postinfection (p.i.). In parallel, host transcriptional activity dropped to 10 to 20%. While the combined effects of both phenomena dominated infection-induced changes in total RNA, extensive gene-specific transcriptional regulation was observable in chromatin-associated RNA and was surprisingly concordant between WT and Δvhs infections. Both induced strong transcriptional upregulation of a small subset of genes that were poorly expressed prior to infection but already primed by H3K4me3 histone marks at their promoters. Most interestingly, analysis of chromatin-associated RNA revealed vhsnuclease-activity-dependent transcriptional downregulation of at least 150 cellular genes, in particular of many integrin adhesome and extracellular matrix components. This was accompanied by a vhs-dependent reduction in protein levels by 8 h p.i. for many of these genes. In summary, our study provides a comprehensive picture of the molecular mechanisms that govern cellular RNA metabolism during the first 8 h of lytic HSV-1 infection. IMPORTANCE The HSV-1 virion host shutoff (vhs) protein efficiently cleaves both host and viral mRNAs in a translation-dependent manner. In this study, we model and quantify changes in vhs activity, as well as virus-induced global loss of host transcriptional activity, during productive HSV-1 infection. In general, HSV-1-induced alterations in total RNA levels were dominated by these two global effects. In contrast, chromatin-associated RNA depicted gene-specific transcriptional changes. This revealed highly concordant transcriptional changes in WT and -vhs infections, confirmed DUX4 as a key transcriptional regulator in HSV-1 infection, and identified vhsdependent transcriptional downregulation of the integrin adhesome and extracellular matrix components. The latter explained seemingly gene-specific effects previously attributed to vhs-mediated mRNA degradation and resulted in a concordant loss in protein levels by 8 h p.i. for many of the respective genes. [ABSTRACT FROM AUTHOR]

Published

2021