AI Article Synopsis

  • The study focuses on the assembly of spliceosomal snRNP cores, comparing human and *S. pombe* (Sp) systems.
  • It identifies key chaperoning proteins, highlighting that while both systems need ICln and the SMN complex, there are notable differences in how specific proteins interact and form structures.
  • This research enhances our understanding of the molecular mechanisms of Sm core assembly and provides insights into the evolutionary variations in chaperone systems.

Article Abstract

The spliceosomal snRNP cores, each comprised of a snRNA and a seven-membered Sm ring (D1/D2/F/E/G/D3/B), are assembled by twelve chaperoning proteins in human. However, only six assembly-assisting proteins, ICln and the SMN complex (SMN/Gemin2/Gemin6-8), have been found in (Sp). Here, we used recombinant proteins to reconstitute the chaperone machinery and investigated the roles of these proteins systematically. We found that, like the human system, the assembly in requires ICln and the SMN complex sequentially. However, there are several significant differences. For instance, h_F/E/G forms heterohexamers and heterotrimers, while Sp_F/E/G only forms heterohexamers; h_Gemin2 alone can bind D1/D2/F/E/G, but Sp_Gemin2 cannot. Moreover, we found that Sp_Gemin2 is essential using genetic approaches. These mechanistic studies reveal that these six proteins are necessary and sufficient for Sm core assembly at the molecular level, and enrich our understanding of the chaperone systems in species variation and evolution.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10470402PMC
http://dx.doi.org/10.1016/j.isci.2023.107604DOI Listing

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