In <i>Caenorhabditis elegans</i>, axon regeneration is activated by a signaling cascade through the receptor tyrosine kinase (RTK) SVH-2. Axonal injury induces <i>
svh-2</i> gene expression by degradation of the Mad-like transcription factor MDL-1. In this study, we identify the <i>
svh-24</i>/<i>
sdz-33</i> gene encoding a protein containing F-box and F-box associated domains as a regulator of axon regeneration in motor neurons. We find that <i>
sdz-33</i> is required for axon injury-induced <i>
svh-2</i> expression. SDZ-33 targets MDL-1 for poly-ubiquitylation and degradation. Furthermore, we demonstrate that SDZ-33 promotes axotomy-induced nuclear degradation of MDL-1, resulting in the activation of <i>
svh-2</i> expression in animals. These results suggest that the F-box protein is required for RTK signaling in the control of axon regeneration.<b>SIGNIFICANCE STATEMENT:</b>In <i>C. elegans</i>, axon regeneration is positively regulated by the growth factor SVH-1 and its receptor tyrosine kinase SVH-2. Expression of the <i>
svh-2</i> gene is induced by axonal injury via the Ets-like transcription factor ETS-4, whose transcriptional activity is inhibited by the Mad-like transcription factor MDL-1. Axon injury leads to the degradation of MDL-1, and this is linked to the activation of ETS-4 transcriptional activity. In this study, we identify the <i>
sdz-33</i> gene encoding a protein containing an F-box domain as a regulator of axon regeneration. We demonstrate that MDL-1 is poly-ubiquitylated and degraded through the SDZ-33-mediated 26S proteasome pathway. These results reveal that an F-box protein promotes axon regeneration by degrading the Mad transcription factor.