SKN-1-independent transcriptional activation of glutathione S-transferase 4 (GST-4) by EGF signaling

Giel Detienne; Pieter Van de Walle; Wouter De Haes; Liliane Schoofs; Liesbet Temmerman

doi:10.1080/21624054.2016.1230585

SKN-1-independent transcriptional activation of glutathione S-transferase 4 (GST-4) by EGF signaling

Worm. 2016 Aug 31;5(4):e1230585. doi: 10.1080/21624054.2016.1230585. eCollection 2016.

Authors

Giel Detienne¹, Pieter Van de Walle¹, Wouter De Haes¹, Liliane Schoofs¹, Liesbet Temmerman¹

Affiliation

¹ Department of Biology , KU Leuven , Leuven, Belgium.

Abstract

In C. elegans research, transcriptional activation of glutathione S-transferase 4 (gst-4) is often used as a read-out for SKN-1 activity. While many heed an assumed non-exclusivity of the GFP reporter signal driven by the gst-4 promoter to SKN-1, this is also often ignored. We here show that gst-4 can also be transcriptionally activated by EOR-1, a transcription factor mediating effects of the epidermal growth factor (EGF) pathway. Along with enhancing exogenous oxidative stress tolerance, EOR-1 inde-pendently of SKN-1 increases gst-4 transcription in response to augmented EGF signaling. Our findings caution researchers within the C. elegans community to always rely on sufficient experimental controls when assaying SKN-1 transcriptional activity with a gst-4_p::gfp reporter, such as SKN-1 loss-of-function mutants and/or additional target genes next to gst-4.

Keywords: CL2166; EGFR; EOR-1; MRJP1; fluorescence; let-23; oxidative stress; royalactin; transcriptional GFP reporter.