Downstream of oncogenic RAS, RALA is critical for cancer tumorigenesis, possibly regulated by phosphorylation of its Serine194 residue. We made CRISPR-Cas9 RALA knockout (RALA KO) in three RAS-dependent and two RAS-independent cancer cells. Detection of RALA S194 phosphorylation using the commercial anti-phospho-RALA antibody lacks specificity in all three RAS-dependent cancers. siRNA knockdown of RALA and AURKA inhibition by MLN8237 (VMLN) also did not affect pS194RALA detection in these cancers. RALA KO MiaPaCa2 (RAS-dependent) and MCF7 (RAS-independent) cells, stably reconstituted with WT-RALA and S194A-RALA mutants, showed no effect on RALA activation. Tumor growth was, however, restored partly by WT-RALA, but not S194A-RALA mutant. Thus, RALA S194 phosphorylation is needed for tumor formation, not affecting its activation, but possibly through its localization.
CRISPR-Cas9 mediated RALA knockout and reconstitution. Insights into the detection and role of RALA S194 phosphorylation in Ras-dependent and Ras-independent cancers
Open Access
- Award Group:
- Funder(s): Indian Council of Medical Research
- Award Id(s): 35/03/2019-NANO/BMS
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Mayuresh Vishwas Konde, Siddhi Inchanalkar, Tushar Manik Sherkhane, Nilesh Deshpande, Mishika Virmani, Kajal Singh, Manicham Jayakannan, Nagaraj Balasubramanian; CRISPR-Cas9 mediated RALA knockout and reconstitution. Insights into the detection and role of RALA S194 phosphorylation in Ras-dependent and Ras-independent cancers. Biol Open 2025; bio.061884. doi: https://doi.org/10.1242/bio.061884
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