Ddx54, also known as Dbp10, is a DEAD-box RNA helicase. It plays crucial roles in multiple biological processes. It is involved in ribosome biogenesis, where it initiates peptidyl transferase center formation during 60S ribosome biogenesis [4,5]. It also functions in post-transcriptional gene regulation, such as regulating transcriptome dynamics during the DNA damage response [3]. Additionally, it participates in signaling pathways like the p65 and AKT signaling pathway [1].

In a Ddx54 knockout mouse model (Ddx54fl/fl;MBP-Cre), after normal postnatal myelination, mice gradually develop behavioral and learning abnormalities, inner myelin sheath breakdown, loss of myelinated axons, oligodendrocyte apoptosis, astrocyte and microglia activation, and die within 7 months. This indicates that Ddx54 is indispensable for myelin homeostasis [2].

In conclusion, Ddx54 is essential for ribosome biogenesis, myelin homeostasis, and post-transcriptional gene regulation during DNA damage response. The Ddx54 knockout mouse model has provided insights into its role in myelin-related diseases, highlighting its importance in understanding the mechanisms underlying these conditions [2].