# Dominant suppressor genes of p53-induced apoptosis in Drosophila melanogaster

**Authors:** Tamás Szlanka, Tamás Lukacsovich, Éva Bálint, Erika Virágh, Kornélia Szabó, Ildikó Hajdu, Enikő Molnár, Yu-Hsien Lin, Ágnes Zvara, Ildikó Kelemen-Valkony, Orsolya Méhi, István Török, Zoltán Hegedűs, Brigitta Kiss, Beáta Ramasz, Laura M Magdalena, László Puskás, Bernard M Mechler, Adrien Fónagy, Zoltán Asztalos, Gábor Steinbach, Michal Žurovec, Imre Boros, István Kiss

PMC · DOI: 10.1093/g3journal/jkae149 · 2024-07-10

## TL;DR

This study identifies genes in fruit flies that suppress apoptosis caused by p53, a key protein in preventing cancer.

## Contribution

The study introduces a novel insertional mutagenesis method using a custom DEP transposon to identify p53 apoptosis suppressor genes in Drosophila.

## Key findings

- Seven genes were identified that suppress p53-induced apoptosis when overexpressed.
- Three of the identified genes are located near coexpressed gene clusters, suggesting a potential role in apoptosis suppression.
- qPCR experiments showed elevated expression levels of genes near DEP insertions, indicating an additive effect.

## Abstract

One of the major functions of programmed cell death (apoptosis) is the removal of cells that suffered oncogenic mutations, thereby preventing cancerous transformation. By making use of a Double-Headed-EP (DEP) transposon, a P element derivative made in our laboratory, we made an insertional mutagenesis screen in Drosophila melanogaster to identify genes that, when overexpressed, suppress the p53-activated apoptosis. The DEP element has Gal4-activatable, outward-directed UAS promoters at both ends, which can be deleted separately in vivo. In the DEP insertion mutants, we used the GMR-Gal4 driver to induce transcription from both UAS promoters and tested the suppression effect on the apoptotic rough eye phenotype generated by an activated UAS-p53 transgene. By DEP insertions, 7 genes were identified, which suppressed the p53-induced apoptosis. In 4 mutants, the suppression effect resulted from single genes activated by 1 UAS promoter (Pka-R2, Rga, crol, and Spt5). In the other 3 (Orct2, Polr2M, and stg), deleting either UAS promoter eliminated the suppression effect. In qPCR experiments, we found that the genes in the vicinity of the DEP insertion also showed an elevated expression level. This suggested an additive effect of the nearby genes on suppressing apoptosis. In the eukaryotic genomes, there are coexpressed gene clusters. Three of the DEP insertion mutants are included, and 2 are in close vicinity of separate coexpressed gene clusters. This raises the possibility that the activity of some of the genes in these clusters may help the suppression of the apoptotic cell death.

## Linked entities

- **Genes:** TP53 (tumor protein p53) [NCBI Gene 7157], Pka-R2 (Protein kinase, cAMP-dependent, regulatory subunit type 2) [NCBI Gene 36041], Rga (Regena) [NCBI Gene 40683], crol (crooked legs) [NCBI Gene 34592], SUPT5H (SPT5 homolog, DSIF elongation factor subunit) [NCBI Gene 6829], Orct2 (Organic cation transporter 2) [NCBI Gene 42890], POLR2M (RNA polymerase II subunit M) [NCBI Gene 81488], C6orf15 (chromosome 6 open reading frame 15) [NCBI Gene 29113]
- **Species:** Drosophila melanogaster (taxon 7227)

## Full-text entities

- **Genes:** Rga (Regena) [NCBI Gene 40683] {aka CG2138, CG2161, Dmel\CG2161, NOT2, Not2, l(3)03834}, p53 (p53) [NCBI Gene 2768677] {aka CG10873, CG31325, CG33336, D-p53, DMP53, Dm-P53}, Orct2 (Organic cation transporter 2) [NCBI Gene 42890] {aka CG13610, Dmel\CG13610, EP(3)1072, EP1072, cald}, crol (crooked legs) [NCBI Gene 34592] {aka CG14938, Dmel\CG14938, ORE-15, anon-EST:Liang-1.74, anon-EST:Liang-2.48, clone 1.74}, Spt5 (Spt5) [NCBI Gene 53442] {aka CG7626, DSIF, Dmel\CG7626, Dspt5, dDSIF, dSpt5}, Pka-R2 (Protein kinase, cAMP-dependent, regulatory subunit type 2) [NCBI Gene 36041] {aka BcDNA:GM01761, CG15862, Cos, Cos-1, Cos1, Dmel\CG15862}
- **Diseases:** eye (MESH:D005134)
- **Species:** Drosophila melanogaster (fruit fly, species) [taxon 7227]

## Figures

4 figures with captions in the complete paper: https://tomesphere.com/paper/PMC11373661/full.md

---
Source: https://tomesphere.com/paper/PMC11373661