CipC, or CLOCK-interacting protein Circadian, is a negative-feedback regulator of the circadian clock. It is involved in various biological processes. In mammals, it has been associated with the regulation of the circadian clock machinery, and it may also play a role in cell cycle regulation through interactions with proteins like CAD and Erk [3,4].

Specific deletion of Cipc in satellite cells of mdx mice alleviates myopathy, improves muscle function, and reduces fibrosis. Cipc deficiency activates the ERK1/2 and JNK1/2 signaling pathways, which in turn activates the transcription factor SP1 to trigger the transcription of Pax7 and MyoD, promoting muscle regeneration [1]. In mice, inactivation of Cipc alters the expression of Per1 but does not affect circadian rhythms [2].

In conclusion, CipC plays a role as a negative regulator in satellite cell function and may have implications in muscle-related diseases as demonstrated by Cipc-deficient mouse models. Additionally, while it impacts the expression of certain clock-related genes, it is not critically required for basic circadian clock function in mice.