Dynamic PML Protein Nucleolar Associations with Persistent DNA Damage Lesions in Response to Nucleolar Stress and Senescence-inducing Stimuli

Overview

Journal Aging (Albany NY)

Specialty Geriatrics

Date 2019 Sep 8

PMID 31493766

Citations 8

Authors

Terezie Imrichova

Sona Hubackova

Alena Kucerova

Jan Kosla

Jiri Bartek

Zdenek Hodny

Pavla Vasicova

Affiliations

Soon will be listed here.

Abstract

Diverse stress insults trigger interactions of PML with nucleolus, however, the function of these PML nucleolar associations (PNAs) remains unclear. Here we show that during induction of DNA damage-induced senescence in human non-cancerous cells, PML accumulates at the nucleolar periphery simultaneously with inactivation of RNA polymerase I (RNAP I) and nucleolar segregation. Using time-lapse and high-resolution microscopy, we followed the genesis, structural transitions and destiny of PNAs to show that: 1) the dynamic structural changes of the PML-nucleolar interaction are tightly associated with inactivation and reactivation of RNAP I-mediated transcription, respectively; 2) the PML-nucleolar compartment develops sequentially under stress and, upon stress termination, it culminates in either of two fates: disappearance or persistence; 3) all PNAs stages can associate with DNA damage markers; 4) the persistent, commonly long-lasting PML multi-protein nucleolar structures (PML-NDS) associate with markers of DNA damage, indicating a role of PNAs in persistent DNA damage response characteristic for senescent cells. Given the emerging evidence implicating PML in homologous recombination-directed DNA repair, we propose that PNAs contribute to sequestration and faithful repair of the highly unstable ribosomal DNA repeats, a fundamental process to maintain a precise balance between DNA repair mechanisms, with implications for genomic integrity and aging.

Citing Articles

PML Nuclear Bodies and Cellular Senescence: A Comparative Study of Healthy and Premature Aging Syndrome Donors' Cells.

Smirnov E, Silonov S, Shmidt E, Nozdracheva A, Pleskach N, Kuranova M Cells. 2025; 13(24.

PMID: 39768166 PMC: 11674897. DOI: 10.3390/cells13242075.

Topological stress triggers persistent DNA lesions in ribosomal DNA with ensuing formation of PML-nucleolar compartment.

Urbancokova A, Hornofova T, Novak J, Salajkova S, Hubackova S, Uvizl A Elife. 2024; 12.

PMID: 39388244 PMC: 11466457. DOI: 10.7554/eLife.91304.

On the Prevalence and Roles of Proteins Undergoing Liquid-Liquid Phase Separation in the Biogenesis of PML-Bodies.

Silonov S, Mokin Y, Nedelyaev E, Smirnov E, Kuznetsova I, Turoverov K Biomolecules. 2023; 13(12).

PMID: 38136675 PMC: 10741438. DOI: 10.3390/biom13121805.

PML Body Biogenesis: A Delicate Balance of Interactions.

Silonov S, Smirnov E, Kuznetsova I, Turoverov K, Fonin A Int J Mol Sci. 2023; 24(23).

PMID: 38069029 PMC: 10705990. DOI: 10.3390/ijms242316702.

Dual signaling via interferon and DNA damage response elicits entrapment by giant PML nuclear bodies.

Scherer M, Read C, Neusser G, Kranz C, Kuderna A, Muller R Elife. 2022; 11.

PMID: 35319461 PMC: 8975554. DOI: 10.7554/eLife.73006.

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