Untethering the TIR1 auxin receptor from the SCF complex increases its stability and inhibits auxin response

• Published in: Nature plants Vol. 1; no. 3
• Main Authors: Yu, Hong, Zhang, Yi, Moss, Britney L., Bargmann, Bastiaan O. R., Wang, Renhou, Prigge, Michael, Nemhauser, Jennifer L., Estelle, Mark
• Format: Journal Article
• Language: English
• Published: London Nature Publishing Group UK 16.02.2015; Nature Publishing Group
• Subjects: 631/449/1741/1576; Amino acids; Auxins; Biomedical and Life Sciences; Cullin; Degradation; Domains; Genomes; Hybrid systems; Life Sciences; Mutants; Mutation; Plant hormones; Plant Sciences; Receptors; Substrates; Ubiquitin; Yeast
• ISSN: 2055-0278; 2055-026X; 2055-0278
• DOI: 10.1038/nplants.2014.30

Plant genomes encode large numbers of F-box proteins (FBPs), the substrate recognition subunit of SKP1–CULLIN–F-box (SCF) ubiquitin ligases. There are ∼700 FBPs in Arabidopsis , most of which are uncharacterized. TIR1 is among the best-studied plant FBPs and functions as a receptor for the plant hormone auxin. Here we use a yeast two-hybrid system to identify novel TIR1 mutants with altered properties. The analysis of these mutants reveals that TIR1 associates with the CULLIN1 (CUL1) subunit of the SCF through the N-terminal H1 helix of the F-box domain. Mutations that untether TIR1 from CUL1 stabilize the FBP and cause auxin resistance and associated growth defects, probably by protecting TIR1 substrates from degradation. Based on these results we propose that TIR1 is subject to autocatalytic degradation when assembled into an SCF. Further, our results suggest a general method for determining the physiological function of uncharacterized FBPs. Finally, we show that a key amino acid variation in the F-box domain of auxin signalling F-box (AFB1), a closely related FBP, reduces its ability to form an SCF, resulting in an increase in AFB1 levels. The plant auxin receptor TIR1 needs to associate with the SCF complex to be functional and target substrates. Newly discovered mutations that can block this interaction suggest that TIR1 is autocatalytically degraded once assembled in the SCF complex.