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TARDBP

TAR DNA-binding protein 43 · UniProt Q13148

Length
414 aa
Mass
44.7 kDa
Annotated
2026-06-10
100 papers in source corpus 32 papers cited in narrative 32 extracted findings
Cross-family judge vs UniProt: Affinage preferred faithfulness: 8/8 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

TDP-43 (TARDBP) is a nuclear RNA/DNA-binding protein that governs post-transcriptional gene regulation through cryptic exon repression, alternative polyadenylation, mRNA stability control, miRNA biogenesis, and autoregulation of its own transcript (PMID:28153034, PMID:38313254, PMID:35495061). Its regulatory output is cell-type specific: conditional deletion reveals distinct cryptic exon programs in neurons versus myocytes, and stage-dependent requirements in the oligodendrocyte lineage where loss causes missplicing of myelination proteins and OPC death (PMID:28153034, PMID:35311646). Beyond splicing, TDP-43 represses tau mRNA via UG-rich 3'UTR binding through its C-terminal region, shapes alternative polyadenylation of pluripotency factors such as Sox2 in opposition to paraspeckle-mediated sequestration, and constrains transcription near Alu and LINE repetitive elements, with nuclear depletion driving chromatin decondensation, LINE1 retrotransposition, and dsRNA-triggered PKR innate-immune activation (PMID:28335005, PMID:31047794, PMID:31655156, PMID:31042469, PMID:31229690). TDP-43 function is mechanistically coupled to liquid-liquid phase separation: its C-terminal low-complexity domain drives homomeric condensation on UG-rich RNA clusters that is required to regulate a subset of transcripts including its own autoregulatory 3'UTR, while RNA binding itself antagonizes the aberrant low-complexity-domain interactions that produce pathological inclusions (PMID:34380047, PMID:35495061, PMID:30826182). Pathological aggregation proceeds by intra-condensate demixing requiring both up-concentration in stress granules and oxidative stress, via RRM1 unfolding and C-terminal hydrophobic interactions, generating filaments whose buried amyloid core (residues 282–360, a double-spiral fold) must be exposed by proteolytic cleavage to seed prion-like spreading (PMID:40412392, PMID:30826182, PMID:37248338). This phase behavior is tuned by HSP70/HSP90 chaperones that maintain liquidity in an ATP-dependent manner and by post-translational modifications—CK1δ phosphorylation, OGT O-GlcNAcylation, PIAS4-mediated SUMO2/3-ylation, and RRM acetylation—that modulate aggregation propensity and subcellular localization (PMID:33335017, PMID:36709343, PMID:35112738, PMID:33855783, PMID:39982984). Mislocalized TDP-43 also accumulates in mitochondria, where it binds ND3/ND6 mRNAs to cause complex I dysfunction and neuronal loss (PMID:27348499). Disease-relevant insults converge on TDP-43: C9orf72 poly(GR) sequesters it RNA-independently into cytoplasmic inclusions, the Perry-disease DCTN1 G71A mutation drives its cytoplasmic mislocalization, and enteroviral 3C protease cleaves it to promote aggregation (PMID:32878979, PMID:33924373, PMID:37039659).

Mechanistic history

Synthesis pass · year-by-year structured walk · 14 steps
  1. 2016 High

    Established a mitochondrial, non-canonical pathogenic activity for TDP-43, showing its damage extends beyond nuclear RNA processing to direct impairment of respiratory machinery.

    Evidence Mitochondrial fractionation, RNA immunoprecipitation, respiratory complex assays, and localization-blocking rescue in transgenic mutant TDP-43 mice

    PMID:27348499

    Open questions at the time
    • Mechanism of TDP-43 mitochondrial import not defined
    • Relationship between mitochondrial and nuclear loss-of-function pools unresolved
  2. 2017 High

    Defined TDP-43 as a regulator of mRNA stability and cell-type-specific cryptic splicing, linking its 3'UTR UG-binding to tau suppression and showing its splicing targets diverge across tissues.

    Evidence mRNA stability chase assays, RIP, domain mapping, transgenic mice, and conditional knockouts in neurons and myocytes with RNA-seq

    PMID:28153034 PMID:28335005

    Open questions at the time
    • Determinants of cell-type-specific cryptic exon selection unknown
    • Whether tau regulation contributes to disease phenotype not established
  3. 2019 High

    Showed RNA binding is protective against pathological phase transitions and that nuclear TDP-43 loss has genome-level consequences—repeat-element derepression, retrotransposition, and innate-immune activation.

    Evidence Optogenetic proteinopathy induction with oligonucleotide rescue, FACS-sorted TDP-43-negative nuclei with ATAC-seq/LINE1 assays, GRO-seq, and astrocyte knockdown with PKR epistasis

    PMID:30826182 PMID:31042469 PMID:31229690 PMID:31655156

    Open questions at the time
    • Causal contribution of retrotransposition and dsRNA-PKR signaling to neurodegeneration not demonstrated in vivo
    • Threshold of nuclear loss required for chromatin effects unclear
  4. 2019 Medium

    Implicated proteostasis and trafficking pathways—endocytosis and the VCP/Cdc48 segregase—in TDP-43 turnover and toxicity.

    Evidence Yeast and Drosophila genetic epistasis, co-IP in patient tissue, and endocytosis modulation assays

    PMID:29233983 PMID:31767634

    Open questions at the time
    • Direct biochemical link between endocytic machinery and TDP-43 clearance not defined
    • Cross-species relevance to human neurons untested
  5. 2019 Medium

    Mapped a pluripotency-stage RNA-regulatory role through alternative polyadenylation and paraspeckle reciprocity.

    Evidence ESC knockdown/overexpression RNA-seq, APA analysis, miRNA reporters, and mouse embryo phenotyping

    PMID:31047794

    Open questions at the time
    • Mechanism by which paraspeckles sequester TDP-43 not structurally defined
    • Generalizability beyond pluripotency unclear
  6. 2020 High

    Identified HSP70 chaperones as the ATP-dependent core that maintains TDP-43 condensate liquidity and showed RRM acetylation drives RNA-binding-deficient anisosome formation.

    Evidence Live-cell imaging, cryo-electron tomography, anisosome proteomics, and ATP-depletion experiments in neurons

    PMID:33335017

    Open questions at the time
    • Whether anisosomes are an intermediate to pathological aggregates in disease not established
    • Acetyltransferase responsible for RRM acetylation not identified
  7. 2020 Medium

    Showed a disease-specific driver—C9orf72 poly(GR)—sequesters TDP-43 into cytoplasmic inclusions independent of RNA.

    Evidence GFP-(GR)200 transgenic mice, co-IP, RNase treatment, and ASO rescue

    PMID:32878979

    Open questions at the time
    • Direct poly(GR)-TDP-43 binding interface not mapped
    • Contribution of nucleocytoplasmic transport disruption versus direct sequestration not separated
  8. 2021 High

    Determined the atomic structure of brain-derived TDP-43 filaments, revealing a disease-specific double-spiral fold distinct from in vitro fibrils.

    Evidence Cryo-EM of TDP-43 aggregates from two ALS-FTLD individuals and two brain regions

    PMID:34880495

    Open questions at the time
    • Pathway from soluble TDP-43 to this fold not reconstituted
    • Whether the fold differs across TDP-43 proteinopathy subtypes unknown
  9. 2021 High

    Established that condensation capacity, not merely sequence binding, is required for TDP-43 to regulate a subset of UG-rich transcripts including its own autoregulatory feedback.

    Evidence Graded-condensation CTD variants combined with in vitro phase separation, FRAP, iCLIP, and RNA-seq

    PMID:34380047 PMID:35495061

    Open questions at the time
    • Which transcripts strictly require condensation versus binding alone incompletely defined
    • Link between autoregulatory condensation and disease-causing mutations partially characterized
  10. 2021 Medium

    Defined post-translational control of TDP-43 phase behavior and localization through SUMOylation, O-GlcNAcylation, and chaperone interplay with the prion-like domain.

    Evidence Co-IP and K136R mutagenesis with SENP1 manipulation, OGT biochemical assays with Drosophila validation, and polyribosome fractionation in stress models

    PMID:33855783 PMID:34378050 PMID:34390468

    Open questions at the time
    • Interplay/hierarchy among the different PTMs not resolved
    • Stress-granule recruitment kinetics for each modification incomplete
  11. 2022 Medium

    Showed CK1δ phosphorylation reduces phase separation and aggregation without disrupting RNA function, and that oligodendrocyte-lineage TDP-43 loss causes stage-specific myelination defects.

    Evidence Phosphomimetic in vitro phase separation, kinase and FRAP assays, molecular dynamics simulations, and stage-specific conditional Tardbp deletion with EM

    PMID:35112738 PMID:35311646

    Open questions at the time
    • Cellular contexts where CK1δ phosphorylation is protective versus harmful not delineated
    • Upstream regulation of CK1δ activity on TDP-43 unclear
  12. 2023 High

    Dissected distinct aggregation routes (monomeric aggresome-dependent versus RNA-binding-deficient LLPS-driven) and showed seeding requires proteolytic exposure of the buried amyloid core; also resolved chaperone recognition of helical PLD elements.

    Evidence Structure-based variants in human neurons, recombinant filament seeding assays with brain-derived material, and NMR plus in vitro chaperone reconstitution

    PMID:36709343 PMID:37248338 PMID:37431963

    Open questions at the time
    • Identity of the physiological protease exposing the amyloid core not established
    • How co-chaperone selectivity (DNAJ isoforms) is regulated in vivo unknown
  13. 2023 Medium

    Identified additional disease-relevant modifiers of TDP-43 localization and aggregation, including the Perry-disease DCTN1 G71A mutation, enteroviral protease cleavage, and proteostasis kinase cascades.

    Evidence Domain-mapping co-IP for DCTN1, viral protease cleavage-site mapping at Q327, and Drosophila/cell kinase-screen epistasis (PTK2-TBK1-SQSTM1; CHMP2B-CK1)

    PMID:31690171 PMID:33924373 PMID:34726688 PMID:37039659

    Open questions at the time
    • Direct structural basis of DCTN1-TDP-43 binding not resolved
    • Whether these modifier pathways operate in human disease tissue not confirmed
  14. 2025 Medium

    Resolved the two-hit trigger for pathological aggregation (stress-granule up-concentration plus oxidative stress) and the RNA-antagonized PIAS4 SUMO2/3 pathway that stabilizes RNA-free TDP-43.

    Evidence Optogenetic concentration control, iPS-motor neurons, mouse and patient validation, engineered demixing-resistant variants, and SUMO conjugation assays with RNA-binding mutants

    PMID:39982984 PMID:40412392

    Open questions at the time
    • Therapeutic feasibility of blocking intra-condensate demixing untested clinically
    • How SUMO2/3-ylation and oxidative demixing are temporally coordinated unclear

Open questions

Synthesis pass · forward-looking unresolved questions
  • It remains unresolved how the protective nuclear condensation/RNA-regulatory functions are mechanistically converted into the cytoplasmic prion-like seeding cascade in human disease, and which single intervention point most effectively halts this transition.
  • No unified in vivo model linking nuclear loss-of-function to cytoplasmic gain-of-toxicity
  • Physiological protease, acetyltransferase, and PTM hierarchy controlling the switch not fully identified

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0003723 RNA binding 7 GO:0140098 catalytic activity, acting on RNA 3 GO:0140110 transcription regulator activity 2 GO:0003677 DNA binding 1
Localization
GO:0005634 nucleus 4 GO:0005829 cytosol 3 GO:0005730 nucleolus 1 GO:0005739 mitochondrion 1
Pathway
R-HSA-1643685 Disease 4 R-HSA-8953854 Metabolism of RNA 4 R-HSA-8953897 Cellular responses to stimuli 3 R-HSA-74160 Gene expression (Transcription) 2
Partners
CHMP2BCSNK1DDCTN1HSPA (HSP70)OGTPIAS4PTK2VCP
Complex memberships
TDP-43 anisosomeparaspecklestress granule

Evidence

Reading pass · 32 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
2021 Cryo-EM structural determination of pathological TDP-43 filaments from ALS with FTLD brain revealed an amyloid-like filament comprising a single protofilament with a double-spiral-shaped fold spanning residues 282-360 in the low-complexity domain, showing no similarity to TDP-43 filaments formed in vitro and lacking classical cross-β amyloid structure. Cryo-electron microscopy of brain-derived TDP-43 aggregates Nature High 34880495
2019 RNA binding antagonizes neurotoxic phase transitions of TDP-43: aberrant interactions between low-complexity domains drive pathological inclusion formation, and this process is antagonized by RNA binding. Pathological inclusions can form outside stress granules. Treatment with oligonucleotides composed of TDP-43 target sequences prevents inclusions and rescues neurotoxicity. Optogenetic induction of TDP-43 proteinopathy in live cells with spatiotemporal control, live-cell imaging, neurotoxicity assays Neuron High 30826182
2016 TDP-43 accumulates in neuronal mitochondria in ALS/FTD. In mitochondria, wild-type and mutant TDP-43 preferentially bind mitochondria-transcribed mRNAs encoding respiratory complex I subunits ND3 and ND6, impairing their expression and causing specific complex I disassembly. Suppression of TDP-43 mitochondrial localization abolishes mitochondrial dysfunction and neuronal loss, and improves phenotypes in transgenic mutant TDP-43 mice. Mitochondrial fractionation, RNA immunoprecipitation, respiratory complex activity assays, transgenic mouse studies with TDP-43 mitochondrial localization signal blocking Nature medicine High 27348499
2020 HSP70 family chaperones are the primary components of the liquid core of TDP-43 'anisosomes' (intranuclear liquid spherical shells formed by RNA binding-deficient TDP-43). ATP-dependent HSP70 activity maintains the liquidity of both shells and cores. Reduction of ATP levels converts anisosomes to solid aggregates. Acetylation of RNA recognition motifs renders TDP-43 unable to bind RNA, driving anisosomes formation. Live-cell imaging, cryo-electron tomography, mathematical modeling, proteomics (mass spectrometry of anisosomes components), ATP depletion experiments, proteasome inhibition in neurons Science High 33335017
2021 TDP-43 condensation capacity (governed by C-terminal domain) is required for efficient assembly on subsets of RNA-binding regions containing long clusters of UG-rich motifs, promoting 'binding-region condensates' via homomeric CTD interactions, and is necessary for regulation of a subset of bound transcripts including TDP-43 mRNA autoregulation. Series of TDP-43 CTD variants with graded condensation propensity; in vitro phase separation assays; nuclear mobility (FRAP); iCLIP for RNA-binding regions; RNA-seq for transcriptome regulation Cell High 34380047
2022 Casein kinase 1δ-mediated TDP-43 hyperphosphorylation on C-terminal serine residues reduces TDP-43 phase separation and aggregation, rendering condensates more liquid-like and dynamic. Phosphomimetic mutations do not affect nuclear import or RNA regulatory functions but suppress accumulation in membrane-less organelles. Multi-scale molecular dynamics simulations reveal reduced homotypic interactions through enhanced solvation of phosphomimetic residues. In vitro phase separation assays with phosphomimetic TDP-43 variants; CK1δ kinase assays; FRAP; molecular dynamics simulations; cellular localization and RNA splicing assays The EMBO journal High 35112738
2025 TDP-43 aggregation requires two concurrent events: up-concentration within stress granules beyond a threshold AND oxidative stress. These collectively trigger intra-condensate demixing via RRM1 domain unfolding (enabling intermolecular disulfide bonds) and increased hydrophobic patch interactions in the C-terminal domain, generating a TDP-43-enriched phase within stress granules that transitions to pathological aggregates. TDP-43 variants resistant to intra-condensate demixing eliminate pathological aggregates. Live-cell imaging, optogenetic concentration control, iPS-motor neurons, disease mouse model validation, patient sample analysis, engineered TDP-43 variants resistant to demixing Cell High 40412392
2023 TDP-43 oligomerization and RNA binding govern TDP-43 stability, splicing functionality, LLPS, and subcellular localization. Oligomerization is modulated by RNA binding. Under impaired proteasomal activity: monomeric TDP-43 forms cytoplasmic inclusions via aggresome-dependent pathway, while RNA binding-deficient TDP-43 aggregates in the nucleus via LLPS-driven pathway. Structure-based TDP-43 variants in human neurons and cell lines; near-physiological expression; proteasome inhibition; co-immunoprecipitation; FRAP; imaging The EMBO journal High 37431963
2023 Seeding of TDP-43 aggregation requires post-fibrillization proteolytic cleavage to expose the β-sheet-rich amyloid core buried by flanking structured domains in full-length TDP-43 filaments. Only TDP-43 filaments with exposed amyloid core efficiently seeded aggregation of endogenous TDP-43 in cells and enhanced seeding by brain-derived TDP-43 aggregates. Recombinant full-length TDP-43 filament production; structural characterization; proteolytic cleavage assays; cell-based seeding assays with brain-derived aggregates Nature neuroscience High 37248338
2019 Loss of nuclear TDP-43 is associated with chromatin decondensation around long interspersed nuclear elements (LINEs) and increased LINE1 DNA content. Loss of TDP-43 leads to increased retrotransposition that can be inhibited with antiretroviral drugs. Subcellular fractionation, FACS enrichment of TDP-43-negative nuclei from post-mortem FTD-ALS brain, RNA-seq, ATAC-seq for chromatin accessibility, LINE1 retrotransposition assay Cell reports High 31042469
2017 TDP-43 suppresses tau expression by promoting mRNA instability through binding to UG repeats in the 3'-UTR of tau mRNA. The C-terminal region of TDP-43 is required for this function. ALS-causing TDP-43 mutations differentially affect tau mRNA instability. mRNA stability assays (actinomycin D chase), RNA immunoprecipitation, TDP-43 truncation mutants, in vivo TDP-43(M337V) transgenic mouse analysis, human brain correlation studies Nucleic acids research High 28335005
2021 TDP-43 is SUMOylated in the nuclear compartment both covalently (at lysine 136 via SUMO E3 ligase PIAS4, confirmed by SUMO-mutant K136R) and non-covalently in the RRM1 domain at a SUMO-interacting motif (residues 106-110). SUMOylation modifies TDP-43 splicing activity (specifically exon skipping), influences subcellular localization, and regulates recruitment to stress granules after oxidative stress. DeSUMOylation by SENP1 increases cytoplasmic TDP-43 localization. Co-immunoprecipitation of SUMO-TDP-43, site-directed mutagenesis (K136R), SENP1 overexpression, cell-permeable SENP1 peptide TS-1, splicing assays, immunofluorescence Molecular neurobiology Medium 34390468
2021 O-GlcNAc transferase (OGT)-mediated O-GlcNAcylation of TDP-43 suppresses TDP-43 aggregation and hyperphosphorylation and promotes TDP-43's mRNA splicing function. O-GlcNAcylation of TDP-43 promotes proper splicing of STMN2 mRNA, required for normal axonal outgrowth and regeneration. Biochemical O-GlcNAcylation assays, OGT inhibition/overexpression, splicing assays, Drosophila motor neuron overexpression with locomotion and lifespan readouts EMBO reports Medium 33855783
2019 TDP-43 in pluripotent cells represses formation of paraspeckles by enhancing the polyadenylated short isoform of Neat1 lncRNA. TDP-43 promotes pluripotency by regulating alternative polyadenylation of transcripts encoding pluripotency factors including Sox2, partially protecting its 3'UTR from miR-21-mediated degradation. Conversely, paraspeckles sequester TDP-43 from mRNAs to promote exit from pluripotency. RNA-seq, TDP-43 knockdown/overexpression in mouse embryonic stem cells, alternative polyadenylation analysis, miRNA reporter assays, mouse embryo patterning phenotypes Molecular cell Medium 31047794
2020 C9orf72-derived poly(GR) protein promotes aggregation of endogenous TDP-43 by mediating sequestration of full-length TDP-43 in an RNA-independent manner, inducing cytoplasmic TDP-43 inclusion formation. Poly(GR) also causes mislocalization of nucleocytoplasmic transport factors and nuclear pore complex proteins, resulting in aberrant cytoplasmic accumulation of TDP-43. GFP-(GR)200 transgenic mouse model; immunofluorescence; co-immunoprecipitation; antisense oligonucleotide treatment; RNase treatment to confirm RNA-independence Science translational medicine Medium 32878979
2019 TDP-43 knockdown in astrocytes causes accumulation of repetitive element transcripts (including endogenous retroviral sequences) and double-stranded RNA (dsRNA), which activates innate immune signaling through protein kinase R (PKR). Inhibition or knockdown of PKR blocks the pro-inflammatory response induced by TDP-43 loss. siRNA knockdown of TDP-43 in primary rat astrocytes, RNA-seq, immunofluorescence, immunoblotting, PKR chemical inhibition and siRNA knockdown Neurobiology of disease Medium 31229690
2017 TDP-43 regulates cryptic exon inclusion in a cell-type-specific manner. Conditional deletion of TDP-43 in excitatory neurons or skeletal myocytes revealed that the majority of TDP-43-repressed cryptic exons are cell type-specific, with only some shared across stem cells, neurons, and myocytes. Conditional knockout mouse models (excitatory neurons and skeletal myocytes), RNA-seq identification of cryptic exons Molecular neurodegeneration Medium 28153034
2022 Stage-specific genetic inactivation of Tardbp in oligodendrocyte lineage cells showed that OPCs require TDP-43 for survival (deletion causes cell loss and rapid regeneration), while oligodendrocytes become less sensitive as they mature. TDP-43 loss in oligodendrocytes causes missplicing of key myelination proteins (cryptic exon incorporation) and morphological defects including inappropriate wrapping of neuronal somata and blood vessels. Conditional in vivo Cre-lox deletion at specific oligodendrocyte lineage stages; transcriptional analysis; behavioral phenotyping; electron microscopy eLife Medium 35311646
2021 DCTN1 binds TDP-43 through its CAP-Gly-basic supradomain, dynactin domain, and C-terminal region, preferentially via TDP-43's C-terminal region. The Perry disease-linked DCTN1 p.G71A mutation impairs this interaction. Overexpression of DCTN1(G71A), the dynactin-domain fragment, or C-terminal fragment induces cytoplasmic mislocalization and aggregation of TDP-43. Co-immunoprecipitation, truncation mutant mapping, overexpression of disease mutant DCTN1, immunofluorescence for TDP-43 localization International journal of molecular sciences Medium 33924373
2019 TDP-43 turnover and toxicity depend in part upon the endocytosis pathway. TDP-43 inhibits endocytosis and co-localizes with endocytic proteins. Impairing endocytosis increases TDP-43 toxicity, aggregation, and protein levels, while enhancing endocytosis reverses these phenotypes. Locomotor dysfunction in a TDP-43 ALS fly model is exacerbated by endocytic impairment and suppressed by enhancement of endocytic function. Yeast genetics, Drosophila ALS model, co-localization with endocytic markers in ALS patient tissue, endocytosis modulation assays, protein level measurements Nature communications Medium 29233983
2020 Cdc48 (VCP in mammals) physically interacts and co-localizes with TDP-43 in ALS patient tissue, and regulates TDP-43 turnover and toxicity together with its cofactor Ubx3 (implicated in endocytic function) in yeast. TDP-43 expression impairs endocytic function. Yeast genetic screen, co-immunoprecipitation in yeast and ALS patient tissue, toxicity and protein turnover assays, endocytic function measurements Molecular and cellular biology Medium 31767634
2019 TARDBP overexpression induces impairment of the ubiquitin proteasome system (UPS). PTK2/FAK is a suppressor of neurotoxicity induced by UPS impairment downstream of TDP-43. PTK2 activation promotes phosphorylation of SQSTM1/p62 at S403 via TBK1, impairing autophagic degradation of poly-ubiquitinated proteins. Non-phosphorylatable SQSTM1(S403A) reduces insoluble poly-ubiquitinated proteins and neurotoxicity caused by TDP-43 overexpression. Kinase inhibitor screen, Drosophila genetic model, site-directed mutagenesis (SQSTM1 S403A), co-immunoprecipitation, proteasome activity assays, TBK1 epistasis Autophagy Medium 31690171
2021 CHMP2B regulates TDP-43 phosphorylation and toxicity independent of autophagy via CK1. Downregulation of CHMP2B reduces TDP-43 phosphorylation and toxicity in Drosophila and mammalian cells. CHMP2B modulates CK1 protein levels by negatively regulating ubiquitination and proteasome-mediated turnover of CK1. Drosophila genetic screen, siRNA knockdown in mammalian cells, CK1 inhibition, ubiquitination assays, proteasome assays, immunoblotting The Journal of cell biology Medium 34726688
2019 TDP-43 broadly affects transcription of protein-coding genes and Alu retrotransposons genome-wide. Loss of TDP-43 results in increased transcription activity near repetitive Alu elements within expressed genes, with the highest densities in shorter genes (<30 kb) whose transcription is most affected by TDP-43. GRO-seq (global run-on sequencing), TDP-43 knockdown in HEK293T cells, ChIP for TDP-43 at transcribed regions Biochimica et biophysica acta Medium 31655156
2023 HSP70 and HSP90 chaperones promote TDP-43 phase separation, while HSP40 co-chaperones (DNAJA2, DNAJB1, DNAJB4, DNAJC7) show distinct effects on TDP-43 de-mixing. Chaperones and co-chaperones primarily recognize structured helical elements in TDP-43's prion-like domain. Methionine sulfoxidation of the second helical element impairs phase separation, amyloid formation, chaperone recognition, and alters phosphorylation by CK1δ. NMR structural characterization of TDP-43 prion-like domain, in vitro phase separation assays with purified chaperones, methionine sulfoxidation, kinase phosphorylation assays Nature communications Medium 36709343
2021 Cytoplasmic TDP-43 associates with polyribosomes in an SH-SY5Y cellular stress model and is detected on polyribosomes in FTD brain lysate, supporting a role for cytoplasmic TDP-43 in translational control during stress. Sorbitol-driven cytoplasmic TDP-43 accumulation followed by oxidative stress triggers PARP cleavage and cellular toxicity. Polyribosome fractionation, immunofluorescence, PARP cleavage assays, brain lysate analysis Human molecular genetics Medium 34378050
2022 TDP-43 oligomerization and phase separation properties are both essential for TDP-43 autoregulation (negative feedback via binding to its own 3'UTR). RNA binding to the central autoregulatory 3'UTR sequence induces TDP-43 condensation in cell lysates. ALS-associated mutation M337V disrupts liquid properties of TDP-43-RNA condensates and autoregulatory function, and decreases cellular clearance of TDP-43. Phase separation assays with purified TDP-43 variants, cell lysate condensation assays, autoregulatory reporter assays, FRAP, fluorescence anisotropy binding assays Frontiers in neuroscience Medium 35495061
2025 During oxidative stress, TDP-43 is SUMO2/3-ylated by the SUMO E3 ligase PIAS4 within stress granules. Inhibition of TDP-43 SUMO2/3-ylation or PIAS4 depletion leads to irreversible TDP-43 aggregation in stress granules. Binding of TDP-43 to UG-rich RNA antagonizes PIAS4-mediated SUMO2/3-ylation, while RNA dissociation promotes it. SUMO2/3-ylation stabilizes cytosolic RNA-free TDP-43 against aggregation. SUMO conjugation assays, PIAS4 knockdown/inhibition, stress granule assembly assays, RNA binding mutants, immunofluorescence, biochemical aggregation assays Science advances Medium 39982984
2024 TDP-43 loss of function induces cryptic alternative polyadenylation (APA) events including alternative last exons (ALE), 3'UTR extensions, and intronic polyadenylation. TDP-43 can have both repressive and enhancing action on APA. Cryptic 3'UTR extensions in transcription factors (e.g., ELK1, SIX3, TLX1) lead to increased RNA stability, higher cytoplasmic localisation, and increased wild-type protein translation. Custom bioinformatic APA pipeline, RNA-seq and Ribo-seq, TDP-43 depletion in cells, post-mortem ALS/FTD brain RNA-seq validation bioRxivpreprint Medium 38313254
2023 EV-D68 protease 3C cleaves TDP-43 at residue Q327, generating fragments with substantially decreased solubility that promote TDP-43 aggregation and cytotoxicity. EV-D68 protease 2A induces TDP-43 cytoplasmic translocation. Viral infection assays, protease activity assays, site-specific cleavage mapping (Q327), solubility fractionation, cytotoxicity assays, lopinavir inhibitor experiments Journal of virology Medium 37039659
2017 TDP-43 regulates the biogenesis of a number of miRNAs; TDP-43 knockdown alters miRNA expression profiles, miRNA isoform patterns (isomiRs), and miRNA arm selection. TDP-43 increases miR-500a-3p expression and binds the mature miR-500a-3p sequence. TDP-43 may promote lung cancer cell migration by regulating miR-423-3p. siRNA-mediated TDP-43 knockdown, small RNA-seq, RNA immunoprecipitation of mature miRNA sequence Protein & cell Low 28952053
2019 TDP-43 and FUS interactomes were determined in HEK293T cells before and after DNA damage. TDP-43 binds to multiple factors important for DNA repair mechanisms including replication-dependent and -independent pathways, with selected interactions validated by co-immunoprecipitation. Mass spectrometry interactome profiling, co-immunoprecipitation validation, DNA damage induction in HEK293T cells Journal of proteome research Low 31693373

Source papers

Stage 0 corpus · 100 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2019 RNA Binding Antagonizes Neurotoxic Phase Transitions of TDP-43. Neuron 423 30826182
2016 The inhibition of TDP-43 mitochondrial localization blocks its neuronal toxicity. Nature medicine 344 27348499
2020 The role of TDP-43 mislocalization in amyotrophic lateral sclerosis. Molecular neurodegeneration 332 32799899
2016 Physiological functions and pathobiology of TDP-43 and FUS/TLS proteins. Journal of neurochemistry 306 27015757
2020 TDP-43 proteinopathies: a new wave of neurodegenerative diseases. Journal of neurology, neurosurgery, and psychiatry 281 33177049
2020 HSP70 chaperones RNA-free TDP-43 into anisotropic intranuclear liquid spherical shells. Science (New York, N.Y.) 269 33335017
2021 TDP-43 Pathology in Alzheimer's Disease. Molecular neurodegeneration 268 34930382
2021 Structure of pathological TDP-43 filaments from ALS with FTLD. Nature 254 34880495
2021 FUS and TDP-43 Phases in Health and Disease. Trends in biochemical sciences 245 33446423
2013 TARDBP and FUS mutations associated with amyotrophic lateral sclerosis: summary and update. Human mutation 222 23559573
2019 Loss of Nuclear TDP-43 Is Associated with Decondensation of LINE Retrotransposons. Cell reports 196 31042469
2021 TDP-43 condensation properties specify its RNA-binding and regulatory repertoire. Cell 187 34380047
2015 Functional Significance of TDP-43 Mutations in Disease. Advances in genetics 186 26410029
2011 TDP-43 and FUS: a nuclear affair. Trends in neurosciences 177 21700347
2018 Pathomechanisms of TDP-43 in neurodegeneration. Journal of neurochemistry 175 29486049
2020 C9orf72 poly(GR) aggregation induces TDP-43 proteinopathy. Science translational medicine 162 32878979
2022 Disease-linked TDP-43 hyperphosphorylation suppresses TDP-43 condensation and aggregation. The EMBO journal 153 35112738
2020 Neurotoxic microglia promote TDP-43 proteinopathy in progranulin deficiency. Nature 148 32866962
2009 Molecular neuropathology of TDP-43 proteinopathies. International journal of molecular sciences 128 19333444
2017 TDP-43 and FUS en route from the nucleus to the cytoplasm. FEBS letters 127 28380257
2008 ALS and FTLD: two faces of TDP-43 proteinopathy. European journal of neurology 113 18684309
2019 Cross-Regulation between TDP-43 and Paraspeckles Promotes Pluripotency-Differentiation Transition. Molecular cell 109 31047794
2016 TDP-43/FUS in motor neuron disease: Complexity and challenges. Progress in neurobiology 106 27693252
2012 Rodent models of TDP-43: recent advances. Brain research 100 22608070
2019 Cytoplasmic functions of TDP-43 and FUS and their role in ALS. Seminars in cell & developmental biology 95 31132467
2015 Inflammation Induces TDP-43 Mislocalization and Aggregation. PloS one 94 26444430
2019 The basis of clinicopathological heterogeneity in TDP-43 proteinopathy. Acta neuropathologica 90 31555895
2017 Tdp-43 cryptic exons are highly variable between cell types. Molecular neurodegeneration 90 28153034
2009 The molecular links between TDP-43 dysfunction and neurodegeneration. Advances in genetics 89 19737636
2017 Endocytosis regulates TDP-43 toxicity and turnover. Nature communications 82 29233983
2022 The Role of TDP-43 in Neurodegenerative Disease. Molecular neurobiology 81 35499795
2019 TDP-43 proteinopathy and mitochondrial abnormalities in neurodegeneration. Molecular and cellular neurosciences 81 31445085
2017 Phase to Phase with TDP-43. Biochemistry 80 28112502
2019 Tau and TDP-43 proteinopathies: kindred pathologic cascades and genetic pleiotropy. Laboratory investigation; a journal of technical methods and pathology 79 30742063
2025 Intra-condensate demixing of TDP-43 inside stress granules generates pathological aggregates. Cell 77 40412392
2023 Loss of TDP-43 oligomerization or RNA binding elicits distinct aggregation patterns. The EMBO journal 72 37431963
2023 Seeding the aggregation of TDP-43 requires post-fibrillization proteolytic cleavage. Nature neuroscience 68 37248338
2017 TDP-43 suppresses tau expression via promoting its mRNA instability. Nucleic acids research 67 28335005
2013 TARDBP mutation analysis in TDP-43 proteinopathies and deciphering the toxicity of mutant TDP-43. Journal of Alzheimer's disease : JAD 67 22751173
2022 TDP-43 pathology: From noxious assembly to therapeutic removal. Progress in neurobiology 65 35101542
2017 Biology and Pathobiology of TDP-43 and Emergent Therapeutic Strategies. Cold Spring Harbor perspectives in medicine 65 27920024
2021 Regulation of TDP-43 phosphorylation in aging and disease. GeroScience 64 34032984
2013 The role of TDP-43 in the pathogenesis of ALS and FTLD. Biochemical Society transactions 63 24256250
2023 Data-driven neuropathological staging and subtyping of TDP-43 proteinopathies. Brain : a journal of neurology 62 37150879
2011 TDP-43 and FUS/TLS: cellular functions and implications for neurodegeneration. The FEBS journal 59 21777389
2008 TDP-43 is a culprit in human neurodegeneration, and not just an innocent bystander. Mammalian genome : official journal of the International Mammalian Genome Society 58 18592312
2011 RNA-binding proteins in neurodegenerative disease: TDP-43 and beyond. Wiley interdisciplinary reviews. RNA 54 22028183
2021 Connecting TDP-43 Pathology with Neuropathy. Trends in neurosciences 50 33832769
2017 TDP-43 and Cytoskeletal Proteins in ALS. Molecular neurobiology 49 28466273
2019 TDP-43 knockdown causes innate immune activation via protein kinase R in astrocytes. Neurobiology of disease 48 31229690
2011 Progranulin and TDP-43: mechanistic links and future directions. Journal of molecular neuroscience : MN 47 21863317
2023 CircTmeff1 Promotes Muscle Atrophy by Interacting with TDP-43 and Encoding A Novel TMEFF1-339aa Protein. Advanced science (Weinheim, Baden-Wurttemberg, Germany) 46 37088818
2022 TDP-43 Oligomerization and Phase Separation Properties Are Necessary for Autoregulation. Frontiers in neuroscience 46 35495061
2019 PTK2/FAK regulates UPS impairment via SQSTM1/p62 phosphorylation in TARDBP/TDP-43 proteinopathies. Autophagy 46 31690171
2022 Cell environment shapes TDP-43 function with implications in neuronal and muscle disease. Communications biology 45 35383280
2016 TDP-43 regulates endogenous retrovirus-K viral protein accumulation. Neurobiology of disease 44 27370226
2018 Biomarkers for diseases with TDP-43 pathology. Molecular and cellular neurosciences 42 30399416
2011 TDP-43 autoregulation: implications for disease. Journal of molecular neuroscience : MN 42 21681666
2021 SUMOylation Regulates TDP-43 Splicing Activity and Nucleocytoplasmic Distribution. Molecular neurobiology 41 34390468
2010 TDP-43 toxicity in yeast. Methods (San Diego, Calif.) 41 21115123
2008 TDP-43 in neurodegenerative disorders. Expert opinion on biological therapy 41 18549326
2021 Molecular, functional, and pathological aspects of TDP-43 fragmentation. iScience 40 34013172
2022 Stage-specific control of oligodendrocyte survival and morphogenesis by TDP-43. eLife 39 35311646
2022 Molecular Dissection of TDP-43 as a Leading Cause of ALS/FTLD. International journal of molecular sciences 39 36293362
2017 TDP-43 regulates cancer-associated microRNAs. Protein & cell 39 28952053
2019 Changes to the TDP-43 and FUS Interactomes Induced by DNA Damage. Journal of proteome research 37 31693373
2017 TDP-43 accelerates age-dependent degeneration of interneurons. Scientific reports 37 29097807
2018 TDP-43 Prions. Cold Spring Harbor perspectives in medicine 35 28108532
2021 DCTN1 Binds to TDP-43 and Regulates TDP-43 Aggregation. International journal of molecular sciences 33 33924373
2017 TDP-43 misexpression causes defects in dendritic growth. Scientific reports 33 29142232
2023 Metamorphism in TDP-43 prion-like domain determines chaperone recognition. Nature communications 30 36709343
2013 TDP-43 high throughput screening analyses in neurodegeneration: advantages and pitfalls. Molecular and cellular neurosciences 30 23500590
2024 HDGFL2 cryptic proteins report presence of TDP-43 pathology in neurodegenerative diseases. Molecular neurodegeneration 29 38539264
2022 TDP-43 Proteinopathy and Tauopathy: Do They Have Pathomechanistic Links? International journal of molecular sciences 29 36555399
2021 O-GlcNAcylation of TDP-43 suppresses proteinopathies and promotes TDP-43's mRNA splicing activity. EMBO reports 29 33855783
2019 18F-Flortaucipir in TDP-43 associated frontotemporal dementia. Scientific reports 28 30988363
2019 TDP-43 regulates transcription at protein-coding genes and Alu retrotransposons. Biochimica et biophysica acta. Gene regulatory mechanisms 28 31655156
2022 Expanding the TDP-43 Proteinopathy Pathway From Neurons to Muscle: Physiological and Pathophysiological Functions. Frontiers in neuroscience 27 35185458
2013 TDP-43 pathology in polyglutamine diseases: with reference to amyotrphic lateral sclerosis. Neuropathology : official journal of the Japanese Society of Neuropathology 26 23889603
2025 Amyotrophic lateral sclerosis caused by TARDBP mutations: from genetics to TDP-43 proteinopathy. The Lancet. Neurology 25 40252666
2020 Cdc48/VCP and Endocytosis Regulate TDP-43 and FUS Toxicity and Turnover. Molecular and cellular biology 25 31767634
2018 Mechanisms Associated with TDP-43 Neurotoxicity in ALS/FTLD. Advances in neurobiology 25 29916022
2021 Cytoplasmic TDP-43 is involved in cell fate during stress recovery. Human molecular genetics 24 34378050
2022 Functional implication of ubiquitinating and deubiquitinating mechanisms in TDP-43 proteinopathies. Frontiers in cell and developmental biology 23 36158183
2021 Metals in ALS TDP-43 Pathology. International journal of molecular sciences 23 34830074
2014 Targeting TDP-43 in neurodegenerative diseases. Expert opinion on therapeutic targets 23 24649927
2024 Elevated nuclear TDP-43 induces constitutive exon skipping. Molecular neurodegeneration 22 38853250
2021 CHMP2B regulates TDP-43 phosphorylation and cytotoxicity independent of autophagy via CK1. The Journal of cell biology 22 34726688
2020 TDP-43 Puts the STING in ALS. Trends in neurosciences 22 33353765
2019 Prion-like properties of assembled TDP-43. Current opinion in neurobiology 22 31862626
2025 SUMO2/3 conjugation of TDP-43 protects against aggregation. Science advances 21 39982984
2023 Enterovirus D68 Infection Induces TDP-43 Cleavage, Aggregation, and Neurotoxicity. Journal of virology 21 37039659
2020 The Role of HDAC6 in TDP-43-Induced Neurotoxicity and UPS Impairment. Frontiers in cell and developmental biology 21 33282865
2024 Decoding TDP-43: the molecular chameleon of neurodegenerative diseases. Acta neuropathologica communications 20 39736783
2021 TDP-43 and ER Stress in Neurodegeneration: Friends or Foes? Frontiers in molecular neuroscience 20 34759799
2019 Structural Transition, Function and Dysfunction of TDP-43 in Neurodegenerative Diseases. Chimia 20 31118120
2017 TDP-43 in the spectrum of MND-FTLD pathologies. Molecular and cellular neurosciences 20 28687523
2025 Single-cell RNA-sequencing reveals early mitochondrial dysfunction unique to motor neurons shared across FUS- and TARDBP-ALS. Nature communications 19 40389397
2024 TDP-43 loss induces extensive cryptic polyadenylation in ALS/FTD. bioRxiv : the preprint server for biology 19 38313254
2023 Reviewing the Potential Links between Viral Infections and TDP-43 Proteinopathies. International journal of molecular sciences 19 36675095

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