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RNA splicing and alternative splicing

RNA splicing and alternative splicing

RNA splicing and alternative splicing

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RNA Splicing - The Pre-mRNA Haircut

  • What: Process in the nucleus where introns (intragenic regions) are removed from pre-mRNA, and exons (expressed regions) are joined.
  • Who: Catalyzed by the spliceosome, a large complex of small nuclear RNAs (snRNAs) and proteins, forming snRNPs ("snurps").
  • How:
    • Recognizes specific splice sites.
    • 5' site: GU sequence.
    • 3' site: AG sequence.
    • Forms a lariat-shaped intermediate, which is then excised.

Spliceosome mechanism and lariat formation

⭐ Autoantibodies to spliceosomal snRNPs (anti-Smith antibodies) are highly specific for Systemic Lupus Erythematosus (SLE).

Splicing Mechanism - Cut, Lariat, Paste

  • Spliceosome: A large RNA-protein complex, composed of five snRNPs (U1, U2, U4, U5, U6) and other proteins, that removes introns from a pre-mRNA transcript.
  • Key Consensus Sequences:
    • 5' Splice Site: GU at the 5' end of the intron.
    • 3' Splice Site: AG at the 3' end of the intron.
    • Branch Point: An adenine (A) nucleotide ~20-50 bases upstream of the 3' site.

RNA Splicing: Lariat Formation and Exon Ligation

⭐ Splicing proceeds via two sequential transesterification reactions. While the reactions themselves don't consume ATP, ATP hydrolysis is required for spliceosome assembly and rearrangement on the pre-mRNA.

Alternative Splicing - One Gene, Many Proteins

  • Core Concept: A single gene's pre-mRNA can be processed in multiple ways to generate different mature mRNAs and, subsequently, different protein isoforms.
  • Mechanism:
    • Specific exons are selectively included or excluded from the final mRNA.
    • Regulated by tissue-specific splicing factors (proteins) that bind to enhancer or silencer sequences on the pre-mRNA.
  • Significance: Greatly increases the coding potential of the genome, allowing a single gene to produce a variety of proteins with different functions or properties.

RNA Splicing and Alternative Splicing Patterns

⭐ Tropomyosin and the calcitonin gene are classic examples. In the thyroid, the gene produces calcitonin; in the brain, it produces calcitonin gene-related peptide (CGRP).

Splicing Errors - When the Cut Goes Wrong

  • Mutations at splice sites (GU donor, AG acceptor) or branch point sequences disrupt intron removal.
  • Leads to:
    • Exon skipping: An exon is incorrectly spliced out.
    • Intron retention: An intron remains in the mature mRNA.
    • Cryptic splice site activation: A nearby, similar sequence is used instead of the correct splice site.
  • These errors often cause frameshift mutations and premature stop codons, yielding truncated or unstable proteins.
  • Clinical Correlates:
    • β-thalassemia
    • Gaucher disease
    • Myelodysplastic syndromes
    • Some forms of Marfan syndrome

⭐ In certain β-thalassemias, a mutation within an intron creates a new, cryptic splice acceptor site. This incorporates part of the intron into the mRNA, causing a frameshift and producing a nonfunctional β-globin protein.

High‑Yield Points - ⚡ Biggest Takeaways

  • Splicing removes introns and joins exons via the spliceosome, a complex of snRNPs.
  • Recognizes consensus sequences: GU at the 5' donor site and AG at the 3' acceptor site.
  • An intermediate lariat loop of the intron is formed and then excised.
  • Alternative splicing generates different protein isoforms from a single gene, increasing proteomic diversity.
  • Anti-Smith antibodies (specific for SLE) target snRNPs.
  • Splicing-site mutations can cause diseases like certain β-thalassemias.

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