Nuclear stabilization of p53 requires a functional nucleolar surveillance pathway

Katherine M Hannan; Priscilla Soo; Mei S Wong; Justine K Lee; Nadine Hein; Perlita Poh; Kira D Wysoke; Tobias D Williams; Christian Montellese; Lorey K Smith; Sheren J Al-Obaidi; Lorena Núñez-Villacís; Megan Pavy; Jin-Shu He; Kate M Parsons; Karagh E Loring; Tess Morrison; Jeannine Diesch; Gaetan Burgio; Rita Ferreira; Zhi-Ping Feng; Cathryn M Gould; Piyush B Madhamshettiwar; Johan Flygare; Thomas J Gonda; Kaylene J Simpson; Ulrike Kutay; Richard B Pearson; Christoph Engel; Nicholas J Watkins; Ross D Hannan; Amee J George

doi:10.1016/j.celrep.2022.111571

Nuclear stabilization of p53 requires a functional nucleolar surveillance pathway

Cell Rep. 2022 Nov 1;41(5):111571. doi: 10.1016/j.celrep.2022.111571.

Authors

Katherine M Hannan¹, Priscilla Soo², Mei S Wong³, Justine K Lee⁴, Nadine Hein², Perlita Poh², Kira D Wysoke², Tobias D Williams², Christian Montellese⁵, Lorey K Smith⁶, Sheren J Al-Obaidi², Lorena Núñez-Villacís², Megan Pavy², Jin-Shu He⁷, Kate M Parsons⁷, Karagh E Loring², Tess Morrison², Jeannine Diesch⁶, Gaetan Burgio², Rita Ferreira², Zhi-Ping Feng⁸, Cathryn M Gould⁹, Piyush B Madhamshettiwar⁹, Johan Flygare¹⁰, Thomas J Gonda¹¹, Kaylene J Simpson¹², Ulrike Kutay⁵, Richard B Pearson¹³, Christoph Engel¹⁴, Nicholas J Watkins⁴, Ross D Hannan¹⁵, Amee J George¹⁶

Affiliations

¹ ACRF Department of Cancer Biology and Therapeutics and Division of Genome Sciences and Cancer, John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia; Division of Research, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia; Department of Biochemistry and Molecular Biology, University of Melbourne, Parkville, VIC 3010, Australia.
² ACRF Department of Cancer Biology and Therapeutics and Division of Genome Sciences and Cancer, John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia.
³ ACRF Department of Cancer Biology and Therapeutics and Division of Genome Sciences and Cancer, John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia; Division of Research, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia; Sir Peter MacCallum Department of Oncology, University of Melbourne, Parkville, VIC 3010, Australia.
⁴ Institute for Cell and Molecular Biosciences, Newcastle University, Newcastle-Upon-Tyne, UK.
⁵ Department of Biology, Institute of Biochemistry, ETH Zurich, Zurich, Switzerland.
⁶ Division of Research, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia.
⁷ ANU Centre for Therapeutic Discovery, John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia.
⁸ The John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia.
⁹ Division of Research, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia; Victorian Centre for Functional Genomics, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia.
¹⁰ Lund Stem Cell Center, Lund University, BMC A12, Lund, Sweden.
¹¹ School of Pharmacy, University of Queensland, Brisbane, QLD 4102, Australia.
¹² Division of Research, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia; Sir Peter MacCallum Department of Oncology, University of Melbourne, Parkville, VIC 3010, Australia; Victorian Centre for Functional Genomics, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia.
¹³ ACRF Department of Cancer Biology and Therapeutics and Division of Genome Sciences and Cancer, John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia; Division of Research, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia; Department of Biochemistry and Molecular Biology, University of Melbourne, Parkville, VIC 3010, Australia; Sir Peter MacCallum Department of Oncology, University of Melbourne, Parkville, VIC 3010, Australia; Department of Biochemistry and Molecular Biology, Monash University, Clayton, VIC 3800, Australia.
¹⁴ Regensburg Center for Biochemistry, University of Regensburg, 93053 Regensburg, Germany.
¹⁵ ACRF Department of Cancer Biology and Therapeutics and Division of Genome Sciences and Cancer, John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia; Division of Research, Peter MacCallum Cancer Centre, Melbourne, VIC 3000, Australia; Department of Biochemistry and Molecular Biology, University of Melbourne, Parkville, VIC 3010, Australia; Department of Biology, Institute of Biochemistry, ETH Zurich, Zurich, Switzerland; Department of Biochemistry and Molecular Biology, Monash University, Clayton, VIC 3800, Australia; School of Biomedical Sciences, University of Queensland, St Lucia, QLD 4067, Australia. Electronic address: ross.hannan@anu.edu.au.
¹⁶ ACRF Department of Cancer Biology and Therapeutics and Division of Genome Sciences and Cancer, John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia; ANU Centre for Therapeutic Discovery, John Curtin School of Medical Research, Australian National University, Acton, ACT 2601, Australia; Department of Clinical Pathology, University of Melbourne, Parkville, VIC 3010, Australia. Electronic address: amee.george@anu.edu.au.

Abstract

The nucleolar surveillance pathway monitors nucleolar integrity and responds to nucleolar stress by mediating binding of ribosomal proteins to MDM2, resulting in p53 accumulation. Inappropriate pathway activation is implicated in the pathogenesis of ribosomopathies, while drugs selectively activating the pathway are in trials for cancer. Despite this, the molecular mechanism(s) regulating this process are poorly understood. Using genome-wide loss-of-function screens, we demonstrate the ribosome biogenesis axis as the most potent class of genes whose disruption stabilizes p53. Mechanistically, we identify genes critical for regulation of this pathway, including HEATR3. By selectively disabling the nucleolar surveillance pathway, we demonstrate that it is essential for the ability of all nuclear-acting stresses, including DNA damage, to induce p53 accumulation. Our data support a paradigm whereby the nucleolar surveillance pathway is the central integrator of stresses that regulate nuclear p53 abundance, ensuring that ribosome biogenesis is hardwired to cellular proliferative capacity.

Keywords: CP: Molecular biology; high-content screening; high-throughput screening; nucleolar surveillance pathway; nucleolus; p53; ribosomal proteins; ribosome biogenesis; stress.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Cell Nucleolus / metabolism
Proto-Oncogene Proteins c-mdm2* / genetics
Proto-Oncogene Proteins c-mdm2* / metabolism
Ribosomal Proteins / genetics
Ribosomal Proteins / metabolism
Signal Transduction / genetics
Tumor Suppressor Protein p53* / genetics
Tumor Suppressor Protein p53* / metabolism

Substances

Tumor Suppressor Protein p53
Proto-Oncogene Proteins c-mdm2
Ribosomal Proteins

Grants and funding

BB/R00143X/1/Biotechnology and Biological Sciences Research Council/United Kingdom