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PRPF38A

Pre-mRNA-splicing factor 38A · UniProt Q8NAV1

Length
312 aa
Mass
37.5 kDa
Annotated
2026-06-10
21 papers in source corpus 13 papers cited in narrative 13 extracted findings
Cross-family judge vs UniProt: tie faithfulness: 7/7 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

PRPF38A (yeast Prp38) is an essential pre-mRNA splicing factor required for the catalytic activation of the spliceosome (PMID:1508195). It is recruited to the assembling spliceosome as part of a B-complex protein (BCP) subcomplex together with Snu23 and MFAP1 (metazoan ortholog of yeast Spp381), the three proteins binding and releasing as a unit after tri-snRNP association and dissociating predominantly after U4 snRNP release and NTC recruitment (PMID:39995036). Its N-terminal domain is built from three pairs of antiparallel α-helices and functions as a multi-interface protein–protein interaction hub that engages at least twelve other spliceosomal proteins through four distinct surfaces; excess of this domain stalls splicing at a pre-catalytic stage, whereas an interaction-deficient mutant does not (PMID:26673105). Within the assembled B complex, Prp38 contacts the Prp8 N-terminal domain and stabilizes the U6 ACAGAGA stem–pre-mRNA and Brr2–U4 snRNA interactions prior to catalytic activation, and in human B complex it contacts SNU23 and FBP21 around the U6/5' splice site helix (PMID:28530653, PMID:38383864). The Snu23–Prp38–MFAP1/Spp381 architecture is built on ER/K motif–stabilized single α-helices whose binding strength is tunable by helix stabilization, and is conserved across species (PMID:27773687, PMID:28335716). Functionally, loss of PRPF38A causes widespread intron retention and altered splicing of transcripts controlling protein homeostasis, mitosis, and apoptosis (PMID:28878028), and correct spatial positioning of PRPF38A within nuclear speckles is itself required for normal splicing, since mislocalization to the nuclear lamina induces intron retention (PMID:32609799, PMID:35869234). Independently, the ubiquitin-like protein Hub1/UBL5 binds non-covalently to a conserved HIND element in Prp38 to modulate splice-site usage and alternative splicing (PMID:21614000, PMID:36480405).

Mechanistic history

Synthesis pass · year-by-year structured walk · 13 steps
  1. 1992 High

    Established that Prp38 is an essential splicing factor acting specifically at the first catalytic step rather than during early assembly, defining its functional stage in the pathway.

    Evidence Temperature-sensitive genetic screen with in vitro splicing inactivation and complementation in yeast

    PMID:1508195

    Open questions at the time
    • Molecular mechanism by which Prp38 promotes the first cleavage-ligation step not defined
    • Connection between Prp38 loss and reduced U6 snRNA levels unexplained at the time
  2. 1999 High

    Identified Spp381 (MFAP1 ortholog) as a direct binding partner of the Prp38 C-terminal half and placed both in the tri-snRNP, linking Prp38 to U4 snRNA release.

    Evidence Dosage suppressor screen, yeast two-hybrid, co-immunoprecipitation, and in vitro splicing in yeast

    PMID:9858581

    Open questions at the time
    • Structural basis of the Prp38–Spp381 interface not resolved
    • Whether the interaction is direct in the assembled spliceosome not shown
  3. 2011 High

    Revealed a regulatory layer in which the ubiquitin-like Hub1 binds a conserved HIND element in Prp38, modulating alternative splice-site usage without disrupting the spliceosome.

    Evidence NMR/biochemical binding, domain mapping, and splicing assays in Hub1-deficient yeast and plants

    PMID:21614000

    Open questions at the time
    • Mechanism by which HIND binding alters splice-site selection not defined
    • Conservation in animals addressed only later
  4. 2015 High

    Defined the human PRPF38A N-terminal domain as a multi-interface interaction hub whose contacts are required to progress past a pre-catalytic stage, explaining how it organizes B-complex protein assembly.

    Evidence Crystal structure, alanine surface-scanning two-hybrid, in vitro binding, and splicing inhibition with domain mutants

    PMID:26673105

    Open questions at the time
    • Functional role of each of the four surfaces in vivo not dissected
    • Identities of all twelve binding partners not individually validated functionally
  5. 2016 High

    Showed the Snu23–Prp38–MFAP1 subcomplex is held together by ER/K-stabilized single α-helices whose affinity is tunable by helix stabilization, revealing a biophysical principle of its assembly.

    Evidence Crystal structure with mutant-peptide binding assays and biophysical characterization (ITC/CD)

    PMID:27773687

    Open questions at the time
    • Whether helix tuning is exploited for regulation in vivo unknown
    • Dynamics of subcomplex assembly during spliceosome maturation not addressed
  6. 2017 High

    Placed Prp38 structurally in the pre-catalytic B complex, showing it binds the Prp8 N-terminal domain and stabilizes U6 ACAGAGA stem–pre-mRNA and Brr2–U4 interactions before catalytic activation.

    Evidence Near-atomic cryo-EM of the yeast B complex spliceosome

    PMID:28530653

    Open questions at the time
    • Order of contact formation during assembly not resolved from a static structure
    • How these contacts are remodeled at activation not shown
  7. 2017 Medium

    Established evolutionary equivalence of human MFAP1 to yeast Spp381 and conservation of the Snu23-Prp38-MFAP1/Spp381 subcomplex across species.

    Evidence In vitro cross-species binding assays, bioinformatics, and yeast prp38-1 complementation

    PMID:28335716

    Open questions at the time
    • Single-lab study
    • Only partial rescue of yeast growth defects achieved
  8. 2017 Medium

    Demonstrated a cellular requirement for PRPF38A in correct splicing of survival-relevant transcripts, linking its loss to intron retention and altered processing of homeostasis, mitosis, and apoptosis genes.

    Evidence siRNA knockdown with RNA-seq splicing analysis in human breast cancer cell lines

    PMID:28878028

    Open questions at the time
    • Direct vs. indirect splicing targets not distinguished
    • No mechanistic follow-up beyond the descriptive phenotype
  9. 2020 Medium

    Localized PRPF38A to nuclear speckles and showed it co-localizes with MFAP1 in droplet-like bodies that precede speckle formation during telophase, connecting the subcomplex to speckle biogenesis.

    Evidence Proximity labeling (TSA-MS) with live-cell imaging and telophase co-localization

    PMID:32609799

    Open questions at the time
    • Functional significance of pre-speckle droplet co-localization not tested
    • Whether speckle targeting is required for splicing addressed separately
  10. 2022 Medium

    Established that PRPF38A spatial positioning is itself functionally important, as forced re-localization to the nuclear lamina increases intron retention.

    Evidence Reversible chemical-dimerizer re-localization with RNA-seq intron-retention quantification in HEK293T cells

    PMID:35869234

    Open questions at the time
    • Single method, single cell line
    • Whether the effect reflects loss of speckle context or sequestration not distinguished
  11. 2022 Medium

    Confirmed the Hub1/UBL5–HIND–Prp38 regulatory axis operates in a multicellular animal, generalizing the splice-site regulation mechanism beyond yeast and plants.

    Evidence Biochemical binding, C. elegans ubl-5 mutant genetics, splicing assays, and yeast complementation

    PMID:36480405

    Open questions at the time
    • Only selected targets analyzed
    • Mechanism of splice-site modulation by the HIND interaction still undefined
  12. 2024 High

    Refined the human B-complex contacts of PRPF38A, resolving interactions with SNU23 and FBP21 around the U6/5' splice site helix and a MFAP1/UBL5 5' exon binding channel.

    Evidence Enhanced-resolution cryo-EM of human B complex dimers

    PMID:38383864

    Open questions at the time
    • Functional consequence of each refined contact not individually tested
    • Significance of the dimeric arrangement unclear
  13. 2025 High

    Resolved the recruitment dynamics, showing Prp38, Snu23, and Spp381 bind and release as a single BCP subcomplex after tri-snRNP binding, with release after U4 dissociation/NTC association, conserved between yeast and humans.

    Evidence Single-molecule colocalization spectroscopy (CoSMoS) of real-time binding/release dynamics in yeast

    PMID:39995036

    Open questions at the time
    • What triggers coordinated BCP release not defined
    • Human dynamics inferred from conservation rather than directly observed

Open questions

Synthesis pass · forward-looking unresolved questions
  • How the Hub1/UBL5-HIND regulatory input is integrated with PRPF38A's structural role in B-complex assembly to control specific splice-site choices in human cells remains open.
  • No mechanistic link established between HIND-mediated regulation and the multi-interface hub function
  • Direct human substrate/target rules for PRPF38A-dependent splicing not defined

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0060090 molecular adaptor activity 3 GO:0140098 catalytic activity, acting on RNA 2
Localization
GO:0005654 nucleoplasm 2 GO:0005634 nucleus 1
Pathway
R-HSA-8953854 Metabolism of RNA 4
Partners
FBP21MFAP1PRPF8SART1SNU23UBL5
Complex memberships
BCP (Snu23-Prp38-MFAP1/Spp381) subcomplexU4/U6.U5 tri-snRNPspliceosome B complex

Evidence

Reading pass · 13 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
1992 Yeast PRP38 encodes an essential pre-mRNA splicing factor required for the first cleavage-ligation step of intron excision; temperature-sensitive inactivation blocks the first step of splicing and causes a decrease in intracellular U6 snRNA levels. Genetic screen of temperature-sensitive mutants; in vitro splicing inactivation and complementation assays Molecular and cellular biology High 1508195
1999 Yeast Prp38p is required for U4 snRNA release from the spliceosome; dosage suppressor screen identified Spp381p (yeast ortholog of human MFAP1) as a direct binding partner that assists Prp38p function; the two-hybrid assay and immune precipitation showed Spp381p is present in the U4/U6.U5 tri-snRNP and directly interacts with the carboxyl half of Prp38p. Dosage suppressor screen; co-immunoprecipitation; yeast two-hybrid; in vitro splicing assay Molecular and cellular biology High 9858581
2011 The ubiquitin-like protein Hub1 binds non-covalently to a conserved HIND element present in spliceosomal proteins including Prp38 (in plants) and Snu66 (in yeast/mammals); this interaction modulates splice-site usage and alternative splicing without globally disrupting the spliceosome. Structural analysis (NMR/biochemical binding); genetic (splicing assays in Hub1-deficient yeast); domain mapping Nature High 21614000
2015 Human PRPF38A contains an N-terminal domain organized around three pairs of antiparallel α-helices that acts as a multi-interface protein-protein interaction hub, binding at least 12 other spliceosomal proteins (most recruited at the same stage) via four distinct surfaces; addition of excess PRPF38A N-terminal domain to in vitro splicing assays stalled splicing at a pre-catalytic stage, while an interaction-deficient mutant did not. Crystal structure of human PRPF38A N-terminal domain; yeast two-hybrid (alanine surface-scanning); in vitro binding assays with recombinant proteins; in vitro splicing inhibition assay with domain mutants RNA High 26673105
2016 Spliceosomal PRPF38A/Prp38 forms a complex with MFAP1 and Snu23; crystal structure analysis shows MFAP1 and Snu23 contact Prp38 via ER/K motif-stabilized single α-helices; helix-stabilizing mutations in the MFAP1 single α-helix reduce Prp38 binding affinity, demonstrating that the strength of these single-α-helix-based interactions can be tuned by helix stabilization in the unbound state. Crystal structure analysis; binding assays with mutant peptides; biophysical characterization (ITC/CD) Structure High 27773687
2017 In the cryo-EM structure of the yeast pre-catalytic B complex spliceosome, Prp38 (along with Snu23 and Spp381) binds the Prp8 N-terminal domain and stabilizes U6 ACAGAGA stem–pre-mRNA and Brr2-U4 snRNA interactions, providing a structural basis for Prp38's role in spliceosome stabilization prior to catalytic activation. Cryo-EM structure of yeast B complex spliceosome at near-atomic resolution Nature High 28530653
2017 Human MFAP1 is a cryptic ortholog of yeast Spp381; in vitro binding studies showed that MFAP1 and Spp381 bind their respective Prp38 proteins via equivalent interfaces and cross-interact with Prp38 from the other species; MFAP1 and Spp381 both form higher-order complexes that additionally include Snu23, constituting an equivalent Snu23-Prp38-MFAP1/Spp381 sub-complex; MFAP1 partially rescued growth defects of temperature-sensitive prp38-1 yeast. In vitro binding assays; bioinformatics (InParanoid, BLAST); yeast complementation assay BMC evolutionary biology Medium 28335716
2017 PRPF38A knockdown in breast cancer cells caused widespread intronic retention and altered splicing of transcripts involved in protein homeostasis, mitosis, and apoptosis, placing PRPF38A as required for normal splicing of transcripts essential for basal-like TNBC cell survival. siRNA knockdown followed by RNA-seq splicing analysis in multiple human breast cancer cell lines Molecular cancer therapeutics Medium 28878028
2020 PRPF38A localizes to nuclear speckles; PRPF38A is a binding partner of MFAP1, and co-localization of MFAP1 and PRPF38A in droplet-like nuclear bodies precedes formation of nuclear speckles during telophase. Proximity labeling (TSA-MS ratio); live-cell imaging; co-localization analysis during telophase The Journal of cell biology Medium 32609799
2022 Partial re-localization of PRPF38A to the nuclear lamina in HEK293T cells using a reversible chemical dimerizer induced a moderate increase in intron retention, demonstrating that spatial positioning of PRPF38A within the nucleus is functionally important for its splicing activity. Chemical dimerizer-based reversible re-localization to nuclear lamina; intron retention quantification by RNA-seq in HEK293T cells Communications biology Medium 35869234
2024 Cryo-EM structure of human spliceosomal B complex dimers revealed that PRPF38A (PRP38) makes molecular contacts with SNU23 and FBP21 around the U6/5' splice site helix, and that MFAP1 and UBL5 form a 5' exon binding channel in hB, refining the understanding of PRP38's interactions at this stage. Cryo-EM structure of human B complex dimers at enhanced resolution The EMBO journal High 38383864
2025 Single-molecule imaging (CoSMoS) showed that yeast Prp38, Snu23, and Spp381 bind to and release from spliceosomes simultaneously after tri-snRNP binding, forming a B complex protein (BCP) subcomplex; BCP release predominantly occurs after U4 snRNP dissociation and NineTeen Complex (NTC) association; under low ATP, BCP pre-associates with the tri-snRNP; this recruitment pathway is conserved between S. cerevisiae and humans. Colocalization Single Molecule Spectroscopy (CoSMoS) real-time imaging of Prp38, Snu23, and Spp381 dynamics during splicing Nucleic acids research High 39995036
2022 In C. elegans, the Hub1/UBL-5 ubiquitin-like protein binds to the HIND-containing splicing factor PRP-38 (C. elegans Prp38 ortholog) and Snu66/SART-1, and associates with other spliceosomal proteins; ubl-5 mutants show splicing defects for selected targets, demonstrating a conserved role of Hub1-Prp38 HIND interaction in pre-mRNA splicing in multicellular organisms. Biochemical binding assays; genetic analysis of C. elegans ubl-5 mutants; splicing assays; yeast complementation FEBS letters Medium 36480405

Source papers

Stage 0 corpus · 21 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2017 Structure of a pre-catalytic spliceosome. Nature 180 28530653
2021 Genome-wide association study implicates novel loci and reveals candidate effector genes for longitudinal pediatric bone accrual. Genome biology 91 33397451
2011 Role of the ubiquitin-like protein Hub1 in splice-site usage and alternative splicing. Nature 81 21614000
1992 PRP38 encodes a yeast protein required for pre-mRNA splicing and maintenance of stable U6 small nuclear RNA levels. Molecular and cellular biology 75 1508195
2020 Tyramide signal amplification mass spectrometry (TSA-MS) ratio identifies nuclear speckle proteins. The Journal of cell biology 67 32609799
1993 Convergent transcripts of the yeast PRP38-SMD1 locus encode two essential splicing factors, including the D1 core polypeptide of small nuclear ribonucleoprotein particles. Proceedings of the National Academy of Sciences of the United States of America 60 8430095
2017 Basal-A Triple-Negative Breast Cancer Cells Selectively Rely on RNA Splicing for Survival. Molecular cancer therapeutics 46 28878028
2009 Plant-specific SR-related protein atSR45a interacts with spliceosomal proteins in plant nucleus. Plant molecular biology 37 19238562
2016 Scaffolding in the Spliceosome via Single α Helices. Structure (London, England : 1993) 28 27773687
2009 Spp382p interacts with multiple yeast splicing factors, including possible regulators of Prp43 DExD/H-Box protein function. Genetics 23 19581443
1999 Elevated levels of a U4/U6.U5 snRNP-associated protein, Spp381p, rescue a mutant defective in spliceosome maturation. Molecular and cellular biology 21 9858581
2015 Multiple protein-protein interactions converging on the Prp38 protein during activation of the human spliceosome. RNA (New York, N.Y.) 19 26673105
2024 Cryo-EM analyses of dimerized spliceosomes provide new insights into the functions of B complex proteins. The EMBO journal 14 38383864
2017 Human MFAP1 is a cryptic ortholog of the Saccharomyces cerevisiae Spp381 splicing factor. BMC evolutionary biology 14 28335716
2013 Prp22 and spliceosome components regulate chromatin dynamics in germ-line polyploid cells. PloS one 8 24244416
2022 The ubiquitin-like protein Hub1/UBL-5 functions in pre-mRNA splicing in Caenorhabditis elegans. FEBS letters 7 36480405
2025 Dynamics and evolutionary conservation of B complex protein recruitment during spliceosome activation. Nucleic acids research 5 39995036
2022 Recruitment of a splicing factor to the nuclear lamina for its inactivation. Communications biology 5 35869234
2017 Proteomic analysis of differentially expressed proteins in kidneys of brain dead rabbits. Molecular medicine reports 3 28534953
2025 Transcripts of splicing factors with time-varying associations with survival outcomes in colorectal cancer. American journal of cancer research 1 40814364
2024 Dynamics and Evolutionary Conservation of B Complex Protein Recruitment During Spliceosome Activation. bioRxiv : the preprint server for biology 0 39149324

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