Back to Search Start Over

Anchorage-independent growth conditions reveal a differential SOS2 dependence for transformation and survival in RAS -mutant cancer cells.

Authors :
Sheffels E
Sealover NE
Theard PL
Kortum RL
Source :
Small GTPases [Small GTPases] 2021 Jan; Vol. 12 (1), pp. 67-78. Date of Electronic Publication: 2019 May 07.
Publication Year :
2021

Abstract

The RAS family of genes ( HRAS, NRAS , and KRAS ) is mutated in around 30% of human tumours. Wild-type RAS isoforms play an important role in mutant RAS-driven oncogenesis, indicating that RasGEFs may play a significant role in mutant RAS-driven transformation. We recently reported a hierarchical requirement for SOS2 in mutant RAS-driven transformation in mouse embryonic fibroblasts, with KRAS>NRAS>HRAS (Sheffels et al., 2018). However, whether SOS2 deletion differentially affects mutant RAS isoform-dependent transformation in human tumour cell lines has not been tested. After validating sgRNAs that efficiently deleted HRAS and NRAS , we showed that the differential requirement for SOS2 to support anchorage-independent (3D) growth, which we previously demonstrated in MEFs, held true in cancer cells. KRAS -mutant cells showed a high dependence on SOS2 for 3D growth, as previously shown, whereas HRAS -mutant cells did not require SOS2 for 3D growth. This differential requirement was not due to differences in RTK-stimulated WT RAS activation, as SOS2 deletion reduced RTK-stimulated WT RAS/PI3K/AKT signalling in both HRAS and KRAS mutated cell lines. Instead, this differential requirement of SOS2 to promote transformation was due to the differential sensitivity of RAS-mutated cancer cells to reductions in WT RAS/PI3K/AKT signalling. KRAS mutated cancer cells required SOS2/PI3K signaling to protect them from anoikis, whereas survival of both HRAS and NRAS mutated cancer cells was not altered by SOS2 deletion. Finally, we present an integrated working model of SOS signaling in the context of mutant KRAS based on our findings and those of others.

Details

Language :
English
ISSN :
2154-1256
Volume :
12
Issue :
1
Database :
MEDLINE
Journal :
Small GTPases
Publication Type :
Academic Journal
Accession number :
31062644
Full Text :
https://doi.org/10.1080/21541248.2019.1611168