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Sumo-regulatory SENP2 controls the homeostatic squamous mitosis-differentiation checkpoint

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posted on 2025-04-10, 10:00 authored by J Galán-Vidal, L García-Gaipo, R Molinuevo, S Dias, A Tsoi, J Gómez-Román, JT Elder, Helfrid HocheggerHelfrid Hochegger, A Gandarillas
Squamous or epidermoid cancer arises in stratified epithelia but also is frequent in the non-epidermoid epithelium of the lung by unclear mechanisms. A poorly studied mitotic checkpoint drives epithelial cells bearing irreparable genetic damage into epidermoid differentiation. We performed an RNA-sequencing gene search to target unknown regulators of this response and selected the SUMO regulatory protein SENP2. Alterations of SENP2 expression have been associated with some types of cancer. We found the protein to be strongly localised to mitotic spindles of freshly isolated human epidermal cells. Primary cells rapidly differentiated after silencing SENP2 with specific shRNAs. Loss of SENP2 produced in synchronised epithelial cells delays in mitotic entry and exit and defects in chromosomal alignment. The results altogether strongly argue for an essential role of SENP2 in the mitotic spindle and hence in controlling differentiation. In addition, the expression of SENP2 displayed an inverse correlation with the immuno-checkpoint biomarker PD-L1 in a pilot collection of aggressive lung carcinomas. Consistently, metastatic head and neck cancer cells that do not respond to the mitosis-differentiation checkpoint were resistant to depletion of SENP2. Our results identify SENP2 as a novel regulator of the epithelial mitosis-differentiation checkpoint and a potential biomarker in epithelial cancer.

Funding

Exploiting chemical genetics to investigate the control of microtubule dynamics by mitotic kinases : CANCER RESEARCH UK | 14499

History

Publication status

  • Published

File Version

  • Published version

Journal

Cell Death and Disease

ISSN

2041-4889

Publisher

Springer Science and Business Media LLC

Issue

8

Volume

15

Article number

596

Department affiliated with

  • Sussex Centre for Genome Damage Stability Publications

Institution

University of Sussex

Full text available

  • Yes

Peer reviewed?

  • Yes