Affinage

MTUS2

Microtubule-associated tumor suppressor candidate 2 · UniProt Q5JR59

Length
1369 aa
Mass
150.2 kDa
Annotated
2026-06-10
17 papers in source corpus 6 papers cited in narrative 10 extracted findings
Cross-family judge vs UniProt: Affinage preferred faithfulness: 6/6 claims corpus-supported (100%)

Mechanistic narrative

Synthesis pass · prose summary of the discoveries below

MTUS2 (TIP150) is a microtubule plus-end tracking protein (+TIP) that couples plus-end machinery to chromosome segregation, entosis, and directional cell migration (PMID:19543227, PMID:24847103, PMID:27451391). It is recruited to growing microtubule plus ends through direct binding to EB1, where it assembles as a tetramer engaging an EB1 dimer via its C-terminal domain; EB1 is required for TIP150 plus-end targeting (PMID:19543227, PMID:23595990). Once localized, TIP150 directly binds the microtubule depolymerase MCAK and drives its EB1-dependent loading onto plus ends (PMID:19543227). This EB1–TIP150–MCAK module is dynamically regulated: Aurora B phosphorylation dissolves the TIP150–MCAK association, Aurora A phosphorylation of MCAK perturbs the intramolecular MCAK conformation needed for TIP150 binding, and PCAF-mediated acetylation of EB1 disrupts the TIP150–EB1 interface — perturbation of these interactions impairs metaphase chromosome alignment and activates the spindle checkpoint (PMID:19543227, PMID:23595990, PMID:24847103). The three proteins further compartmentalize the kinetochore–microtubule machinery by undergoing liquid–liquid phase separation at plus ends, which acetylation of EB1 Lys220 attenuates (PMID:38323478). Through a distinct C-terminal proline-rich region binding the cortactin SH3 domain at the cortical cytoskeleton, TIP150 also supports polarized cell migration, an interaction negatively regulated by EGF-driven cortactin tyrosine phosphorylation (PMID:27451391).

Mechanistic history

Synthesis pass · year-by-year structured walk · 8 steps
  1. 2009 High

    Established MTUS2/TIP150 as a bona fide +TIP and identified EB1 as the recruiting factor, defining how the protein reaches microtubule plus ends.

    Evidence In vitro EB1 binding, plus-end co-localization, and EB1 siRNA knockdown

    PMID:19543227

    Open questions at the time
    • Did not define the structural EB1-binding motif resolved later
    • No functional consequence of plus-end targeting yet established
  2. 2009 High

    Showed TIP150 directly binds and loads the depolymerase MCAK at plus ends, linking the +TIP to control of microtubule dynamics.

    Evidence In vitro binding plus TIP150 knockdown with MCAK localization readout

    PMID:19543227

    Open questions at the time
    • Quantitative effect on depolymerization kinetics not measured
    • Cellular phenotype of disrupted loading not yet defined
  3. 2009 Medium

    Identified Aurora B phosphorylation as a switch dissolving the TIP150-MCAK interaction, the first regulatory input on the module.

    Evidence In vitro kinase assay followed by binding assay

    PMID:19543227

    Open questions at the time
    • Phosphosites not mapped in vivo
    • Single lab in vitro reconstitution without cellular validation
  4. 2013 High

    Resolved the oligomeric architecture (TIP150 tetramer binding an EB1 dimer) and demonstrated that disrupting this interface arrests mitosis, establishing the interaction as essential for chromosome segregation.

    Evidence Oligomerization analysis, Co-IP, dominant-negative peptide and siRNA with mitotic phenotype

    PMID:23595990

    Open questions at the time
    • No atomic structure of the tetramer-dimer interface
    • Stoichiometry at native plus ends in vivo not directly quantified
  5. 2013 High

    Defined PCAF acetylation of EB1 as a second regulatory layer disrupting TIP150-EB1 binding and perturbing chromosome alignment, with BubR1 epistasis linking it to checkpoint control.

    Evidence In vitro acetylation, Co-IP, BubR1 siRNA epistasis, live-cell imaging

    PMID:23595990

    Open questions at the time
    • Endogenous acetylation dynamics during mitosis not tracked
    • Upstream signals controlling PCAF activity unknown
  6. 2014 High

    Extended the TIP150-MCAK module to entosis and showed Aurora A regulates an MCAK intramolecular conformation required for TIP150 binding, connecting plus-end dynamics to cell mechanical rigidity.

    Evidence Intramolecular association assay, in vitro kinase assay, Co-IP, optical trap, live-cell entosis assay

    PMID:24847103

    Open questions at the time
    • Mechanistic link between plus-end dynamics and cortical rigidity not fully resolved
    • Aurora A phosphosites on MCAK in this context not mapped
  7. 2016 High

    Identified a cortactin SH3-binding function for TIP150's C-terminal proline-rich region, establishing a microtubule-independent role in polarized cell migration regulated by EGF signaling.

    Evidence Co-IP, in vitro binding, TAT-CT150 peptide perturbation, siRNA, directional migration assay

    PMID:27451391

    Open questions at the time
    • Cortactin tyrosine phosphosites mediating regulation not pinpointed
    • Relationship between cortical and plus-end pools of TIP150 unresolved
  8. 2024 High

    Demonstrated that EB1, TIP150, and MCAK form phase-separated condensates at plus ends, providing a biophysical organizing principle for the kinetochore-MT machinery sensitive to EB1 acetylation.

    Evidence In vitro droplet phase-separation assay, competing peptide in cells and Drosophila embryos, EB1 acetylation mutagenesis, live-cell imaging

    PMID:38323478

    Open questions at the time
    • In vivo evidence that endogenous condensates form at native plus ends remains indirect
    • Material properties and turnover of condensates not characterized

Open questions

Synthesis pass · forward-looking unresolved questions
  • The developmental and tissue-specific functions of MTUS2 implied by its embryonic cardiac and neural expression remain mechanistically unconnected to its characterized +TIP roles.
  • No organismal phenotype links MTUS2 isoforms to cardiac or neural development
  • Functional difference between the 358- and 1354-aa isoforms uncharacterized

Mechanism profile

Synthesis pass · controlled-vocabulary classification · explore literature graph →
Molecular activity
GO:0008092 cytoskeletal protein binding 3 GO:0060090 molecular adaptor activity 2
Localization
GO:0005856 cytoskeleton 2 GO:0005815 microtubule organizing center 1
Pathway
R-HSA-1640170 Cell Cycle 3
Partners
AURKAAURKBCTTNEB1MCAKPCAF
Complex memberships
EB1-TIP150-MCAK plus-end complex

Evidence

Reading pass · 10 per-paper findings extracted from the source corpus
Year Finding Method Journal Conf PMIDs
2009 TIP150 (MTUS2) is a microtubule plus-end tracking protein (+TIP) that binds EB1 in vitro and co-localizes with EB1 at MT plus ends in vivo; EB1 suppression eliminates TIP150 plus-end localization, establishing EB1 as required for TIP150 targeting. In vitro binding assay, co-localization by immunofluorescence, siRNA knockdown of EB1 EMBO reports High 19543227
2009 TIP150 (MTUS2) directly binds MCAK (an MT depolymerase) and facilitates the EB1-dependent loading of MCAK onto MT plus ends; suppression of TIP150 diminishes MCAK plus-end localization. In vitro binding assay, siRNA knockdown of TIP150 with fluorescence microscopy readout of MCAK localization EMBO reports High 19543227
2009 Aurora B-mediated phosphorylation disrupts the TIP150-MCAK association in vitro, providing a regulatory mechanism for MT plus-end dynamics. In vitro kinase assay followed by binding assay EMBO reports Medium 19543227
2013 TIP150 (MTUS2) forms a tetramer and binds an EB1 dimer through its C-terminal domain; disruption of the TIP150-EB1 interface (by C-terminal TIP150 overexpression or membrane-permeable peptide) perturbs chromosome segregation and activates the spindle checkpoint. Biochemical oligomerization analysis, Co-IP, dominant-negative peptide perturbation, siRNA knockdown with mitotic phenotype readout The Journal of biological chemistry High 23595990
2013 PCAF acetylates EB1, and persistent EB1 acetylation disrupts the TIP150-EB1 interaction, perturbs metaphase chromosome alignment, and activates the spindle checkpoint; BubR1 suppression overrides this arrest but causes whole-chromosome aneuploidy. In vitro acetylation assay, Co-IP, siRNA epistasis (BubR1 knockdown), live-cell imaging of chromosome alignment The Journal of biological chemistry High 23595990
2014 TIP150 (MTUS2) cooperates with MCAK to govern entosis; MCAK forms an intra-molecular association required for TIP150 binding, and Aurora A-mediated phosphorylation of MCAK modulates this intra-molecular association to perturb the MCAK-TIP150 interaction in vitro and inhibit entosis in vivo. Biochemical intra-molecular association assay, in vitro kinase assay, co-IP, optical trap measurement of cell mechanical rigidity, live-cell entosis assay Journal of molecular cell biology High 24847103
2014 TIP150-MCAK interaction promotes microtubule dynamics and modulates the mechanical rigidity of live cells during entosis, as measured by optical trap. Optical trap mechanical measurement of live MCF7 cells with TIP150/MCAK perturbation Journal of molecular cell biology Medium 24847103
2016 TIP150 (MTUS2) interacts with cortactin via its C-terminal proline-rich region (CT150) binding to the SH3 domain of cortactin; EGF-elicited tyrosine phosphorylation of cortactin negatively regulates this interaction. Suppression of TIP150 or overexpression of phospho-mimicking cortactin inhibits polarized cell migration. Co-IP, in vitro binding assay, membrane-permeable TAT-CT150 peptide perturbation, siRNA knockdown, directional cell migration assay The Journal of biological chemistry High 27451391
2024 EB1, TIP150 (MTUS2), and MCAK form molecular condensates through liquid-liquid phase separation at microtubule plus ends, compartmentalizing the kinetochore-MT machinery; perturbation of EB1-TIP150 polymer formation by a competing peptide prevents phase separation and disrupts chromosome alignment in cultured cells and Drosophila embryos. Persistent acetylation of EB1 Lys220 attenuates phase separation of the EB1-TIP150-MCAK complex. In vitro phase separation assay (droplet formation), competing-peptide perturbation in cells and Drosophila embryos, acetylation mutagenesis of EB1, live-cell imaging of chromosome alignment Journal of molecular cell biology High 38323478
2009 The MTUS2/CAZIP protein contains a leucine-zipper domain at its C-terminus and has at least two isoforms (358 and 1354 amino acids); its mRNA is expressed during early cardiac development and later in the nervous system of mouse and chicken embryos. Whole-mount in situ hybridization, Northern blot, RT-PCR, bioinformatic domain analysis Developmental dynamics Medium 19806667

Source papers

Stage 0 corpus · 17 papers · ranked by NIH iCite citations
Year Title Journal Citations PMID
2009 TIP150 interacts with and targets MCAK at the microtubule plus ends. EMBO reports 76 19543227
2015 A genome-wide approach to link genotype to clinical outcome by utilizing next generation sequencing and gene chip data of 6,697 breast cancer patients. Genome medicine 70 26474971
2014 Aurora A orchestrates entosis by regulating a dynamic MCAK-TIP150 interaction. Journal of molecular cell biology 43 24847103
2013 Regulation of a dynamic interaction between two microtubule-binding proteins, EB1 and TIP150, by the mitotic p300/CBP-associated factor (PCAF) orchestrates kinetochore microtubule plasticity and chromosome stability during mitosis. The Journal of biological chemistry 34 23595990
2017 A Comparative Proteomic Analysis of Erinacine A's Inhibition of Gastric Cancer Cell Viability and Invasiveness. Cellular physiology and biochemistry : international journal of experimental cellular physiology, biochemistry, and pharmacology 32 28854418
2022 Integrative RNA profiling of TBEV-infected neurons and astrocytes reveals potential pathogenic effectors. Computational and structural biotechnology journal 31 35685361
2016 The Microtubule Plus End Tracking Protein TIP150 Interacts with Cortactin to Steer Directional Cell Migration. The Journal of biological chemistry 21 27451391
2023 Whole-genome sequencing identifies novel predictors for hematopoietic cell transplant outcomes for patients with myelodysplastic syndrome: a CIBMTR study. Journal of hematology & oncology 15 37041565
2024 Whole genome-wide sequence analysis of long-lived families (Long-Life Family Study) identifies MTUS2 gene associated with late-onset Alzheimer's disease. Alzheimer's & dementia : the journal of the Alzheimer's Association 14 38380866
2009 CAZIP, a novel protein expressed in the developing heart and nervous system. Developmental dynamics : an official publication of the American Association of Anatomists 11 19806667
2024 Organization of microtubule plus-end dynamics by phase separation in mitosis. Journal of molecular cell biology 10 38323478
2021 Fine-Scale Genetic Structure and Natural Selection Signatures of Southwestern Hans Inferred From Patterns of Genome-Wide Allele, Haplotype, and Haplogroup Lineages. Frontiers in genetics 8 34504517
2023 Extracellular vesicles-transmitted long non-coding RNA MTUS2-5 promotes proliferation and vascularization of human vascular endothelial cells in patients with Budd-Chiari syndrome. Journal of cellular and molecular medicine 4 37596794
2024 N6-methyladenosine modification of circular RNA circASH2L suppresses growth and metastasis in hepatocellular carcinoma through regulating hsa-miR-525-3p/MTUS2 axis. Journal of translational medicine 3 39543614
2026 Genomic Signatures Underlying Environmental Adaptation and Reproductive Traits in the Tibetan Pig. Animals : an open access journal from MDPI 0 41681490
2025 Alectinib efficacy in advanced lung adenocarcinoma with coexistence of a novel ALK-MTUS2 and STRN3-ALK double fusion: A case report and literature review. Oncology letters 0 40692742
2025 Decoding Fibroblast Heterogeneity in Osteoarthritis: Identification of a Fibrosis-Associated Subtype and Novel Diagnostic Biomarkers. Mediators of inflammation 0 41035938

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