Therapeutic targeting of the PLK1-PRC1-axis triggers cell death in genomically silent childhood cancer

Jing Li; Shunya Ohmura; Aruna Marchetto; Martin F Orth; Roland Imle; Marlene Dallmayer; Julian Musa; Maximilian M L Knott; Tilman L B Hölting; Stefanie Stein; Cornelius M Funk; Ana Sastre; Javier Alonso; Felix Bestvater; Merve Kasan; Laura Romero-Pérez; Wolfgang Hartmann; Andreas Ranft; Ana Banito; Uta Dirksen; Thomas Kirchner; Florencia Cidre-Aranaz; Thomas G P Grünewald

doi:10.1038/s41467-021-25553-z

Therapeutic targeting of the PLK1-PRC1-axis triggers cell death in genomically silent childhood cancer

Nat Commun. 2021 Sep 16;12(1):5356. doi: 10.1038/s41467-021-25553-z.

Authors

Jing Li^{1

2

3}, Shunya Ohmura^{1

2

3}, Aruna Marchetto¹, Martin F Orth¹, Roland Imle^{3

4

5

6}, Marlene Dallmayer^{1

7}, Julian Musa^{1

2

3

8}, Maximilian M L Knott¹, Tilman L B Hölting¹, Stefanie Stein¹, Cornelius M Funk^{1

2

3}, Ana Sastre⁹, Javier Alonso^{10

11}, Felix Bestvater¹², Merve Kasan¹, Laura Romero-Pérez^{1

2

3}, Wolfgang Hartmann¹³, Andreas Ranft^{14

15}, Ana Banito^{3

4}, Uta Dirksen^{14

15}, Thomas Kirchner^{1

16}, Florencia Cidre-Aranaz^{1

2

3}, Thomas G P Grünewald^{17

18

19

20}

Affiliations

¹ Max-Eder Research Group for Pediatric Sarcoma Biology, Institute of Pathology, Faculty of Medicine, LMU Munich, Munich, Germany.
² Division of Translational Pediatric Sarcoma Research, German Cancer Research Center (DKFZ), German Cancer Consortium (DKTK), Heidelberg, Germany.
³ Hopp Children's Cancer Center (KiTZ), Heidelberg, Germany.
⁴ Soft tissue sarcoma Junior Research Group, German Cancer Research Center (DKFZ), German Cancer Consortium (DKTK), Heidelberg, Germany.
⁵ Faculty of Biosciences, Heidelberg University, Heidelberg, Germany.
⁶ Division of Pediatric Surgery, Department of General, Visceral and Transplantation Surgery, Heidelberg University Hospital, Heidelberg, Germany.
⁷ Department of General Pediatrics, University Hospital Münster, Münster, Germany.
⁸ Department of General, Visceral and Transplantation Surgery, Heidelberg University Hospital, Heidelberg, Germany.
⁹ Unidad Hemato-oncología Pediátrica, Hospital Infantil Universitario La Paz, Madrid, Spain.
¹⁰ Pediatric Solid Tumour Laboratory, Institute of Rare Diseases Research (IIER), Instituto de Salud Carlos III, Madrid, Spain.
¹¹ Centro de Investigación Biomédica en Red de Enfermedades Raras, Instituto de Salud Carlos III (CB06/07/1009; CIBERER-ISCIII), Madrid, Spain.
¹² Light Microscopy Facility, German Cancer Research Center (DKFZ), Heidelberg, Germany.
¹³ Division of Translational Pathology, Gerhard-Domagk-Institute for Pathology, University Hospital Münster, Münster, Germany.
¹⁴ Pediatrics III, AYA Unit, West German Cancer Centre, University Hospital Essen, Essen, Germany.
¹⁵ German Cancer Consortium (DKTK), partner site Essen, Essen, Germany.
¹⁶ German Cancer Consortium (DKTK), partner site Munich, Munich, Germany.
¹⁷ Max-Eder Research Group for Pediatric Sarcoma Biology, Institute of Pathology, Faculty of Medicine, LMU Munich, Munich, Germany. t.gruenewald@kitz-heidelberg.de.
¹⁸ Division of Translational Pediatric Sarcoma Research, German Cancer Research Center (DKFZ), German Cancer Consortium (DKTK), Heidelberg, Germany. t.gruenewald@kitz-heidelberg.de.
¹⁹ Hopp Children's Cancer Center (KiTZ), Heidelberg, Germany. t.gruenewald@kitz-heidelberg.de.
²⁰ Institute of Pathology, Heidelberg University Hospital, Heidelberg, Germany. t.gruenewald@kitz-heidelberg.de.

Abstract

Chromosomal instability (CIN) is a hallmark of cancer¹. Yet, many childhood cancers, such as Ewing sarcoma (EwS), feature remarkably 'silent' genomes with minimal CIN². Here, we show in the EwS model how uncoupling of mitosis and cytokinesis via targeting protein regulator of cytokinesis 1 (PRC1) or its activating polo-like kinase 1 (PLK1) can be employed to induce fatal genomic instability and tumor regression. We find that the EwS-specific oncogenic transcription factor EWSR1-FLI1 hijacks PRC1, which physiologically safeguards controlled cell division, through binding to a proximal enhancer-like GGAA-microsatellite, thereby promoting tumor growth and poor clinical outcome. Via integration of transcriptome-profiling and functional in vitro and in vivo experiments including CRISPR-mediated enhancer editing, we discover that high PRC1 expression creates a therapeutic vulnerability toward PLK1 inhibition that can repress even chemo-resistant EwS cells by triggering mitotic catastrophe.Collectively, our results exemplify how aberrant PRC1 activation by a dominant oncogene can confer malignancy but provide opportunities for targeted therapy, and identify PRC1 expression as an important determinant to predict the efficacy of PLK1 inhibitors being used in clinical trials.

Publication types

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

MeSH terms

Animals
Apoptosis / genetics*
Cell Cycle Proteins / genetics*
Cell Cycle Proteins / metabolism
Cell Line, Tumor
Child
Gene Expression Profiling
Gene Expression Regulation, Neoplastic
HEK293 Cells
Humans
Kaplan-Meier Estimate
Mice
Mice, Inbred NOD
Mice, Knockout
Mice, SCID
Oncogene Proteins, Fusion / genetics*
Oncogene Proteins, Fusion / metabolism
Polo-Like Kinase 1
Protein Serine-Threonine Kinases / genetics*
Protein Serine-Threonine Kinases / metabolism
Proto-Oncogene Proteins / genetics*
Proto-Oncogene Proteins / metabolism
RNA Interference
RNAi Therapeutics / methods
Sarcoma, Ewing / genetics*
Sarcoma, Ewing / metabolism
Sarcoma, Ewing / therapy
Signal Transduction / genetics
Xenograft Model Antitumor Assays / methods

Substances

Cell Cycle Proteins
EWSR1-FLI1 fusion protein, human
Oncogene Proteins, Fusion
PRC1 protein, human
Proto-Oncogene Proteins
Protein Serine-Threonine Kinases