BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. rs4950928, BRAF, Fatty acid metabolic process, Inflammatory disorder, Intestine)
Bookmark Forward

A forward genetic screen in C. elegans identifies conserved residues of spliceosomal proteins PRP8 and SNRNP200/BRR2 with a role in maintaining 5' splice site identity.

Catiana H Cartwright-Acar, Kenneth Osterhoudt, Jessie M N G L Suzuki, Destiny R Gomez, Sol Katzman, Alan M Zahler

Nucleic acids research 2022 Nov 11


filter terms:
  • 5 splice site (5)
  • alleles (1)
  • factors (2)
  • genes (1)
  • human (2)
  • native (2)
  • nucleic acids (1)
  • protein c (1)
  • PRP8 (4)
  • research (1)
  • ribonucleoprotein u5 small nuclear (2)
  • ribonucleoproteins small nuclear (2)
  • rna (5)
  • rna helicases (2)
  • rna precursors (1)
  • rna precursors (2)
  • SNRNP200 (6)
  • U1snRNA (3)
  • U6snRNA (1)
  • yeast (1)
    • Sizes of these terms reflect their relevance to your search.

    The spliceosome undergoes extensive rearrangements as it assembles onto precursor messenger RNAs. In the earliest assembly step, U1snRNA identifies the 5' splice site. However, U1snRNA leaves the spliceosome relatively early in assembly, and 5' splice site identity is subsequently maintained through interactions with U6snRNA, protein factor PRP8, and other components during the rearrangements that build the catalytic site. Using a forward genetic screen in Caenorhabditis elegans, we have identified suppressors of a locomotion defect caused by a 5'ss mutation. Here we report three new suppressor alleles from this screen, two in PRP8 and one in SNRNP200/BRR2. mRNASeq studies of these suppressor strains indicate that they also affect specific native alternative 5'ss, especially for suppressor PRP8 D1549N. A strong suppressor at the unstructured N-terminus of SNRNP200, N18K, indicates a novel role for this region. By examining distinct changes in the splicing of native genes, examining double mutants between suppressors, comparing these new suppressors to previously identified splicing suppressors from yeast, and mapping conserved suppressor residues onto cryoEM structural models of assembling human spliceosomes, we conclude that there are multiple interactions at multiple stages in spliceosome assembly responsible for maintaining the initial 5'ss identified by U1snRNA for entry into the catalytic core. © The Author(s) 2022. Published by Oxford University Press on behalf of Nucleic Acids Research.

    Citation

    Catiana H Cartwright-Acar, Kenneth Osterhoudt, Jessie M N G L Suzuki, Destiny R Gomez, Sol Katzman, Alan M Zahler. A forward genetic screen in C. elegans identifies conserved residues of spliceosomal proteins PRP8 and SNRNP200/BRR2 with a role in maintaining 5' splice site identity. Nucleic acids research. 2022 Nov 11;50(20):11834-11857

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 36321655

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.