Snu13-flox Mouse

Snu13, a key component of the assembling spliceosome, is essential for pre-mRNA splicing, a crucial process in gene expression. It is conserved across species, with its structure being highly similar in the red alga Cyanidioschyzon merolae, yeast, and humans [1]. Snu13 binds specifically to the U14 C/D box snoRNA K-turn sequence motif, which is a prerequisite for the assembly of the ribonucleoprotein (RNP) complex containing NOP58/Nop58, NOP56/Nop56, and the 2'-O-methyl-transferase Fibrillarin/Nop1p [3].

In ovarian cancer, the spliceosomal protein Snu13 promotes therapy resistance. Molecules secreted by ovarian cancer cells upon therapy, which are enriched with spliceosomal components including Snu13, enhance cisplatin resistance and DNA damage repair in recipient cancer cells [2]. In acute ischemic stroke, Snu13 was identified as one of the hub metabolism-related genes. Its expression level is related to the infiltration levels of multiple immune cells, and it may play a role in the molecular mechanisms of acute ischemic stroke [4].

In conclusion, Snu13 is vital for pre-mRNA splicing and RNP assembly. Its role in promoting therapy resistance in ovarian cancer and its association with immune cell infiltration in acute ischemic stroke, as revealed through these studies, highlight its significance in disease-related biological processes. Understanding Snu13's functions may provide new insights into the mechanisms of these diseases and potential therapeutic strategies.