Mutant p53 induces SH3BGRL expression to promote cell engulfment

Muller, Patricia; Dolma, Lobsang; Banyard, Antonia; Hall, Callum; Breitweiser, Wolfgang; Sahoo, Sudhakar; Weightman, John; Pazos Gil, Maria; Behan, Caron; Fullard, Nicola; Williams, Lewis; Ashton, Garry; Bell, Steven; Patterson, Mary

doi:10.1038/s41420-025-02582-x

Mutant p53 induces SH3BGRL expression to promote cell engulfment

Muller, Patricia; Dolma, Lobsang; Banyard, Antonia; Hall, Callum; Breitweiser, Wolfgang; Sahoo, Sudhakar; Weightman, John; Pazos Gil, Maria; Behan, Caron; Fullard, Nicola; Williams, Lewis; Ashton, Garry; Bell, Steven; Patterson, Mary

Authors

Dr Patricia Muller patricia.muller@durham.ac.uk
Associate Professor

Lobsang Dolma lobsang.dolma@durham.ac.uk
Academic Visitor

Antonia Banyard

Callum Hall

Wolfgang Breitweiser

Sudhakar Sahoo

John Weightman

Maria Pazos Gil

Caron Behan

Dr Nicola Fullard nicola.fullard@durham.ac.uk
Chief Experimental Officer

Lewis Williams

Garry Ashton

Steven Bell steven.bell@durham.ac.uk
Postdoctoral Research Associate

Mary Patterson mary.patterson@durham.ac.uk
PGR Student Master of Science

Abstract

Previously, we identified that mutant p53 expression in cancer cells promotes engulfment of neighbouring cancer cells to form cell-in-cell (CIC) structures. This process gave mutant p53 cells an advantage in tumour formation in mouse xenograft experiments. TP53 can be found mutated at nearly every amino acid in cancers and mutant p53 expression is associated with various GOF (Gain-of-function) processes, including cancer cell invasion, metastasis, stemness and drug resistance. In the current manuscript, we identified SH3BGRL (Src homology 3 binding glutamate rich protein like) as a mutant p53-regulated gene and investigated to what extent SH3BGRL expression and cell engulfment are responsible for mutant p53-dependent anchorage-independent growth and chemoresistance. We demonstrate that mutant p53 expression drives cell engulfment in which the mutant p53 host cell moves in the direction of the target internal cell to form CIC structures. This is therefore more reminiscent of cell engulfment rather than cell entosis, in which cells invade into host cells. Using NGS (Next Generation Sequencing), we identified novel target genes of mutant p53 and demonstrate that cell engulfment requires SH3BGRL expression. We generated mutant p53 and p53 KO cell lines that stably overexpressed SH3BGRL and determined that SH3BGRL promotes etoposide resistance in mutant p53 cells and anchorage-independent growth independent of mutant p53 expression. Through FACS sorting of pure cell engulfing (CIC) populations, we could also show that engulfing cells have an enhanced etoposide resistance. These data suggest that SH3BGRL and cell engulfment are required for certain GOFs of mutant p53.

Citation

Muller, P., Dolma, L., Banyard, A., Hall, C., Breitweiser, W., Sahoo, S., Weightman, J., Pazos Gil, M., Behan, C., Fullard, N., Williams, L., Ashton, G., Bell, S., & Patterson, M. (2025). Mutant p53 induces SH3BGRL expression to promote cell engulfment. Cell Death Discovery, 11, Article 288. https://doi.org/10.1038/s41420-025-02582-x

Journal Article Type	Article
Acceptance Date	May 12, 2025
Online Publication Date	Jul 1, 2025
Publication Date	Jul 1, 2025
Deposit Date	May 21, 2025
Publicly Available Date	Jul 1, 2025
Journal	Cell Death Discovery
Electronic ISSN	2058-7716
Publisher	Springer Nature
Peer Reviewed	Peer Reviewed
Volume	11
Article Number	288
DOI	https://doi.org/10.1038/s41420-025-02582-x
Public URL	https://durham-repository.worktribe.com/output/3957516