Your search keyword '"Gram, Helena Hagner"' showing total 5 results

1. MDC1 maintains active elongation complexes of RNA polymerase II

Author

Pappas, George, Munk, Sebastian Howen Nesgaard, Watanabe, Kenji, Thomas, Quentin, Gál, Zita, Gram, Helena Hagner, Lee, MyungHee, Gómez-Cabello, Daniel, Kanellis, Dimitris Christos, Olivares-Chauvet, Pedro, Larsen, Dorthe Helena, Gregersen, Lea Haarup, Maya-Mendoza, Apolinar, Galanos, Panagiotis, and Bartek, Jiri

Published

2023

2. MDC1 maintains active elongation complexes of RNA polymerase II

Author

Universidad de Sevilla. Departamento de Biología Celular, European Union (UE), Danish Cancer Society. Denmark, Lundbeck Foundation, Novo Nordisk Foundation, Swedish Research Council, Danish Council for Independent Research. Denmark, Japan Society for the Promotion of Science (JSPS), Independent Research Fund Denmark, Pappas, George, Munk, Sebastian Howen Nesgaard, Watanabe, Kenji, Thomas, Quentin, Gal, Zita, Gram, Helena Hagner, Lee, MyungHee, Gómez Cabello, Daniel, Bartek, Jiri, Universidad de Sevilla. Departamento de Biología Celular, European Union (UE), Danish Cancer Society. Denmark, Lundbeck Foundation, Novo Nordisk Foundation, Swedish Research Council, Danish Council for Independent Research. Denmark, Japan Society for the Promotion of Science (JSPS), Independent Research Fund Denmark, Pappas, George, Munk, Sebastian Howen Nesgaard, Watanabe, Kenji, Thomas, Quentin, Gal, Zita, Gram, Helena Hagner, Lee, MyungHee, Gómez Cabello, Daniel, and Bartek, Jiri

Abstract

The role of MDC1 in the DNA damage response has been extensively studied; however, its impact on other cellular processes is not well understood. Here, we describe the role of MDC1 in transcription as a regulator of RNA polymerase II (RNAPII). Depletion of MDC1 causes a genome-wide reduction in the abundance of actively engaged RNAPII elongation complexes throughout the gene body of protein-encoding genes under unperturbed conditions. Decreased engaged RNAPII subsequently alters the assembly of the spliceosome complex on chromatin, leading to changes in pre-mRNA splicing. Mechanistically, the S/TQ domain of MDC1 modulates RNAPII-mediated transcription. Upon genotoxic stress, MDC1 promotes the abundance of engaged RNAPII complexes at DNA breaks, thereby stimulating nascent transcription at the damaged sites. Of clinical relevance, cancer cells lacking MDC1 display hypersensitivity to RNAPII inhibitors. Overall, we unveil a role of MDC1 in RNAPII-mediated transcription with potential implications for cancer treatment.

Published

2023

3. MDC1 maintains active elongation complexes of RNA polymerase II

Author

European Commission, Danish Cancer Society Research Center, Danish Council for Independent Research, Lundbeck Foundation, Novo Nordisk Foundation, Swedish Research Council, Danish National Research Foundation, Japan Society for the Promotion of Science, Independent Research Fund Denmark, Pappas, George, Munk, Sebastian Howen Nesgaard, Watanabe, Kenji, Thomas, Quentin, Gál, Zita, Gram, Helena Hagner, Lee, MyungHee, Gómez-Cabello, Daniel, Kanellis, Dimitris C., Olivares-Chauvet, Pedro, Larsen, Dorthe Helena, Gregersen, Lea Haarup, Maya-Mendoza, Apolinar, Galanos, Panagiotis, Bartek, Jiri, European Commission, Danish Cancer Society Research Center, Danish Council for Independent Research, Lundbeck Foundation, Novo Nordisk Foundation, Swedish Research Council, Danish National Research Foundation, Japan Society for the Promotion of Science, Independent Research Fund Denmark, Pappas, George, Munk, Sebastian Howen Nesgaard, Watanabe, Kenji, Thomas, Quentin, Gál, Zita, Gram, Helena Hagner, Lee, MyungHee, Gómez-Cabello, Daniel, Kanellis, Dimitris C., Olivares-Chauvet, Pedro, Larsen, Dorthe Helena, Gregersen, Lea Haarup, Maya-Mendoza, Apolinar, Galanos, Panagiotis, and Bartek, Jiri

Abstract

The role of MDC1 in the DNA damage response has been extensively studied; however, its impact on other cellular processes is not well understood. Here, we describe the role of MDC1 in transcription as a regulator of RNA polymerase II (RNAPII). Depletion of MDC1 causes a genome-wide reduction in the abundance of actively engaged RNAPII elongation complexes throughout the gene body of protein-encoding genes under unperturbed conditions. Decreased engaged RNAPII subsequently alters the assembly of the spliceosome complex on chromatin, leading to changes in pre-mRNA splicing. Mechanistically, the S/TQ domain of MDC1 modulates RNAPII-mediated transcription. Upon genotoxic stress, MDC1 promotes the abundance of engaged RNAPII complexes at DNA breaks, thereby stimulating nascent transcription at the damaged sites. Of clinical relevance, cancer cells lacking MDC1 display hypersensitivity to RNAPII inhibitors. Overall, we unveil a role of MDC1 in RNAPII-mediated transcription with potential implications for cancer treatment.

Published

2023

4. Lamin A/C impairments cause mitochondrial dysfunction by attenuating PGC1α and the NAMPT-NAD+ pathway

Author

Maynard, Scott, primary, Hall, Arnaldur, additional, Galanos, Panagiotis, additional, Rizza, Salvatore, additional, Yamamoto, Tatsuro, additional, Gram, Helena Hagner, additional, Munk, Sebastian H N, additional, Shoaib, Muhammad, additional, Sørensen, Claus Storgaard, additional, Bohr, Vilhelm A, additional, Lerdrup, Mads, additional, Maya-Mendoza, Apolinar, additional, and Bartek, Jiri, additional

Published

2022

5. Lamin A/C impairments cause mitochondrial dysfunction by attenuating PGC1 and the NAMPT-NAD+ pathway

Author

Maynard, Scott, Hall, Arnaldur, Galanos, Panagiotis, Rizza, Salvatore, Yamamoto, Tatsuro, Gram, Helena Hagner, Munk, Sebastian H.N., Shoaib, Muhammad, Sørensen, Claus Storgaard, Bohr, Vilhelm A., Lerdrup, Mads, Maya-Mendoza, Apolinar, Bartek, Jiri, Maynard, Scott, Hall, Arnaldur, Galanos, Panagiotis, Rizza, Salvatore, Yamamoto, Tatsuro, Gram, Helena Hagner, Munk, Sebastian H.N., Shoaib, Muhammad, Sørensen, Claus Storgaard, Bohr, Vilhelm A., Lerdrup, Mads, Maya-Mendoza, Apolinar, and Bartek, Jiri

Abstract

Mutations in the lamin A/C gene (LMNA) cause laminopathies such as the premature aging Hutchinson Gilford progeria syndrome (HGPS) and altered lamin A/C levels are found in diverse malignancies. The underlying lamin-associated mechanisms remain poorly understood. Here we report that lamin A/C-null mouse embryo fibroblasts (Lmna−/− MEFs) and human progerin-expressing HGPS fibroblasts both display reduced NAD+ levels, unstable mitochondrial DNA and attenuated bioenergetics. This mitochondrial dysfunction is associated with reduced chromatin recruitment (Lmna−/− MEFs) or low levels (HGPS) of PGC1, the key transcription factor for mitochondrial homeostasis. Lmna−/− MEFs showed reduced expression of the NAD+biosynthesis enzyme NAMPT and attenuated activity of the NAD+-dependent deacetylase SIRT1. We find high PARylation in lamin A/C-aberrant cells, further decreasing the NAD+ pool and consistent with impaired DNA base excision repair in both cell models, a condition that fuels DNA damage-induced PARylation under oxidative stress. Further, ATACsequencing revealed a substantially altered chromatin landscape in Lmna−/− MEFs, including aberrantly reduced accessibility at the Nampt gene promoter. Thus, we identified a new role of lamin A/C as a key modulator of mitochondrial function through impairments of PGC1 and the NAMPT-NAD+ pathway, with broader implications for the aging process.

Published

2022