Your search keyword '"Per Arne Aas"' showing total 4 results

1. The G2-phase enriched lncRNA SNHG26 is necessary for proper cell cycle progression and proliferation

Author

Helle Samdal, Nina-Beate Liabakk, Per Arne Aas, Bjørnar Sporsheim, Konika Chawla, Pål Sætrom, and Siv Anita Hegre

Subjects

biology, Downregulation and upregulation, Chemistry, Gene expression, biology.protein, RNA, RNA polymerase II, Cell cycle, Gene, ChIP-sequencing, Cell cycle phase, Cell biology

Abstract

Long noncoding RNAs (lncRNAs) are involved in the regulation of cell cycle, although only a few have been functionally characterized. By combining RNA sequencing and ChIP sequencing of cell cycle synchronized HaCaT cells we have previously identified lncRNAs highly enriched for cell cycle functions. Based on a cyclic expression profile and an overall high correlation to histone 3 lysine 4 trimethylation (H3K4me3) and RNA polymerase II (Pol II) signals, the lncRNA SNHG26 was identified as a top candidate. In the present study we report that downregulation of SNHG26 affects mitochondrial stress, proliferation, cell cycle phase distribution, and gene expression in cis- and in trans, and that this effect is reversed by upregulation of SNHG26. We also find that the effect on cell cycle phase distribution is cell type specific and stable over time. Results indicate an oncogenic role of SNHG26, possibly by affecting cell cycle progression through the regulation of downstream MYC-responsive genes.

Published

2021

2. The lncRNA EPB41L4A-AS1 regulates gene expression in the nucleus and exerts cell type-dependent effects on cell cycle progression

Author

Per Arne Aas, Siv Anita Hegre, Helle Samdal, Nina-Beate Liabakk, Konika Chawla, Pål Sætrom, and Bjørnar Sporsheim

Subjects

Cell type, Gene expression, Repressor, Cell cycle, Biology, Gene, Overlapping gene, Cell biology, Cell cycle phase, ChIP-sequencing

Abstract

The long non-coding RNA (lncRNA) EPB41L4A-AS1 is aberrantly expressed in various cancers and has been reported to be involved in metabolic reprogramming and as a repressor of the Warburg effect. Although the biological relevance of EPB41L4A-AS1 is evident, its functional role seems to vary depending on cell type and state of disease. By combining RNA sequencing and ChIP sequencing of cell cycle synchronized HaCaT cells we previously identified EPB41L4A-AS1 to be one of 59 lncRNAs with potential cell cycle functions. Here, we demonstrate that EPB41L4A-AS1 exists as bright foci and regulates gene expression in the nucleus in both cis and trans. Specifically, we find that EPB41L4A-AS1 positively regulates its sense overlapping gene EPB41L4A and influences expression of hundreds of other genes, including genes involved in cell proliferation. Finally, we show that EPB41L4A-AS1 affects cell cycle phase distribution, though these effects vary between cell types.

Published

2021

3. Identification of novel antiviral drug combinations in vitro and tracking their development

Author

Mart Ustav, Aleksandr Ianevski, Evgeny Kulesskiy, Gaily Kivi, Kirsti Løseth, Andres Männik, Mona H. Fenstad, Marc P. Windisch, Kristiina Kurg, Eva Zusinaite, Tanel Tenson, Jaewon Yang, Per Arne Aas, Denis E. Kainov, Valentyn Oksenych, Svetlana Biza, Astra Vitkauskiene, Magnar Bjørås, Svein Arne Nordbø, Eunji Jo, Hilde Lysvand, Nastassia Shtaida, Anu Planken, Rouan Yao, and Eva-Maria Tombak

Subjects

0303 health sciences, education.field_of_study, Sofosbuvir, 030306 microbiology, medicine.drug_class, business.industry, Population, virus diseases, Lamivudine, Pharmacology, 3. Good health, 03 medical and health sciences, chemistry.chemical_compound, Nelfinavir, chemistry, Homoharringtonine, medicine, Antiviral drug, education, business, Niclosamide, 030304 developmental biology, Obatoclax, medicine.drug

Abstract

Combination therapies have become a standard for the treatment for HIV and HCV infections. They are advantageous over monotherapies due to better efficacy and reduced toxicity, as well as the ability to prevent the development of resistant viral strains and to treat viral co-infections. Here, we identify several new synergistic combinations against emerging and re-emerging viral infections in vitro. We observed synergistic activity of nelfinavir with investigational drug EIDD-2801 and convalescent serum against SARS-CoV-2 infection in human lung epithelial Calu-3 cells. We also demonstrated synergistic activity of vemurafenib combination with emetine, homoharringtonine, gemcitabine, or obatoclax against echovirus 1 infection in human lung epithelial A549 cells. We also found that combinations of sofosbuvir with brequinar and niclosamide were synergistic against HCV infection in hepatocyte derived Huh-7.5 cells, whereas combinations of monensin with lamivudine and tenofovir were synergistic against HIV-1 infection in human cervical TZM-bl cells. Finally, we present an online resource that summarizes novel and known antiviral drug combinations and their developmental status. Overall, the development of combinational therapies could have a global impact improving the preparedness and protection of the general population from emerging and re-emerging viral threats.

Published

2020

4. 'Alkyladenine DNA glycosylase associates with transcription elongation to coordinate DNA repair with gene expression'

Author

Stefano Bradamante, Pål Sætrom, Antonia Furrer, Barbara van Loon, Sarah L. Fordyce Martin, Leona D. Samson, Marcel Rösinger, Alessandro Brambilla, Nicola P. Montaldo, Magnar Bjørås, Diana L. Bordin, Karine Øian Bjørås, Lene Christin Olsen, Marit Otterlei, and Per Arne Aas

Subjects

Genome instability, chemistry.chemical_compound, biology, chemistry, DNA repair, RNA polymerase, Gene expression, biology.protein, RNA polymerase II, Base excision repair, Gene, Chromatin, Cell biology

Abstract

Base excision repair (BER) initiated by alkyladenine DNA glycosylase (AAG; aka MPG) is essential for removal of aberrantly methylated DNA bases. Genome instability and accumulation of aberrant bases accompany multiple diseases including cancer and neurological disorders. While BER is well studied on naked DNA, it remains unclear how BER efficiently operates on chromatin. Here we show that AAG binds to chromatin and forms complex with active RNA polymerase (pol) II. This occurs through direct interaction with Elongator and results in transcriptional co-regulation. Importantly, at co-regulated genes aberrantly methylated bases accumulate towards 3’end, in regions enriched for BER enzymes AAG and APE1, Elongator and active RNA pol II. Active transcription and functional Elongator are further crucial to ensure efficient BER, by promoting AAG and APE1 chromatin recruitment. Our findings provide novel insights to maintaining genome stability in actively transcribing chromatin, and reveal roles of aberrantly methylated bases in regulation of gene expression.

Published

2019