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| Alternative Names | TDP-43, TDP43, TARDBP, TAR DNA-binding protein 43, Transactive response DNA-binding protein 43, ALS10, TDP43_N domain-containing protein, TADBP_HUMAN, TADBP_MOUSE, TADBP_PONAB, TADBP_XENTR, TADBP_CHICK, TBPH, dmTDP43, dtar, dTBPH, dTDP, dTDP-43, tbph, TDPH, CG10327, Dmel_CG10327 |
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Background
TDP-43 is provided as a recombinant protein reagent for research use only. It is commonly used as a defined molecular component in biochemical and cell-free systems where controlled protein input supports mechanistic study and assay development.
Protein identity context: TDP-43 (source species: Human).
Human Recombinant TDP-43 (W68S, W113S, W172S, W334S, W385S, W412S) Mutant Monomers
TAR DNA-binding protein 43 (TDP-43) is a ubiquitously expressed RNA/DNA-binding protein that plays a pivotal role in RNA processing, including RNA splicing, mRNA turnover, and microRNA biogenesis. Its pathological mislocalization from the nucleus to the cytoplasm, accompanied by aggregation and post-translational modifications, is a hallmark of several neurodegenerative diseases such as amyotrophic lateral sclerosis (ALS), frontotemporal lobar degeneration (FTLD), and Alzheimer’s disease. These TDP-43 proteinopathies disrupt nucleocytoplasmic transport and mitochondrial function, contributing to neuronal dysfunction and death. Recent studies have also highlighted TDP-43’s involvement in DNA repair and chromatin remodeling, expanding its relevance in neurobiology beyond RNA processing. Notably, Pokrishevsky et al. (2024) demonstrated that when all six tryptophans are mutated to serines (trpless), this significantly reduces the protein’s ability to cross-seed SOD1 aggregation. Our TDP-43 hexamutant monomers has shown a reduced propensity to aggregate.
Biological significance and function
TDP-43 is used in RUO research to interrogate molecular mechanisms, interaction networks, and pathway-linked phenotypes in experimental systems. This protein is frequently discussed in research themes such as Neuroscience and Neurodegeneration.
Molecular characteristics
Molecular characteristics: Key molecular attributes can influence binding behavior, stability, and assay background—especially for multimeric, disulfide-rich, or PTM-dependent proteins.
- Source species: Human
- Protein length: 413 AA
- Protein size: 44.61 kDa
- Purity: > 95% by A260/A280
- Expression system: E. coli
- Purification: Affinity Purified
- Storage buffer: 30mM Tris pH 7.4, 100 mM NaCl
Post-translational considerations: E. coli expression typically yields a non-glycosylated recombinant form. This is often appropriate for intracellular enzymes and many binding studies, but extracellular ligands/receptors or disulfide-rich proteins may show activity or stability differences when PTMs are required.
Expression and purification strategy
Expression system: E. coli. Expression host choice can influence folding and PTM state, which may affect binding or activity depending on protein class.
Purification strategy: Affinity Purified. Purification method and formulation help determine sample homogeneity and background in downstream biochemical assays.
Research interpretation
Research interpretation: Recombinant protein reagents can support controlled experiments such as reconstitution of molecular interactions, quantitative calibration, and mechanistic perturbation studies with defined inputs. Interpreting outcomes typically benefits from pairing the primary readout with orthogonal markers that report on pathway state, localization, and complex formation.
Other relevant information: Refer to the Neurodegenerative Protein Handling Instructions on our website, or the product datasheet for further information.
Certificate of Analysis: Certified 95% pure using A260/A280 analysis and western blot analysis. Low endotoxin <5 EU/mL @ 1 mg/mL.
Tariff Code: 3822.19.0030
UNSPSC Code: 12352202
ADR Code: Non-hazardous
UN Code for transport: Non-hazardous
Cite this Product: Human Recombinant TDP-43 Hexamutant (W→S) Monomers (StressMarq Biosciences | Victoria, BC CANADA | Catalog# SPR-522B)
Human Recombinant TDP-43 Hexamutant (W→S) Monomers (StressMarq Biosciences | Victoria, BC CANADA | Catalog# SPR-522C)
Human Recombinant TDP-43 Hexamutant (W→S) Monomers (StressMarq Biosciences | Victoria, BC CANADA | Catalog# SPR-522E)
What is the purity of TDP-43 Hexamutant (W→S) Monomers (Human)?
How should TDP-43 Hexamutant (W→S) Monomers (Human) be stored?
What expression system was used to produce this protein?
Is this protein biologically active?
What are the shipping conditions?
Is this protein approved for clinical or in vitro diagnostic use?
Can I request a custom size, tag variant, or formulation?
Can’t Find What You’re Looking For? We can help you source the best match or customize a recombinant protein solution for your study. Options may include species (human/mouse/rat), protein region/domain (full-length vs fragment), tag or label (His/GST/FLAG/biotin/fluorescent), expression system (E. coli/HEK293/insect), purity grade, formulation (buffer, carrier-free, glycerol-free), activity/functional validation (binding or enzymatic assays), endotoxin level (low-endotoxin for cell-based work), mutants/variants (point mutations, isoforms), and bulk or custom packaging. Click Talk to a Scientist to submit a request form, email us at support@biohippo.com, or explore our Research Services for additional support. Our team will be in contact with you shortly.
Meneses, A., Koga, S., O'Leary, J., Dickson, D. W., Bu, G., & Zhao, N. (2021). TDP-43 pathology in Alzheimer’s disease. Molecular Neurodegeneration, 16 (84). https://doi.org/10.1186/s13024-021-00503-x
Nilaver, B. I., & Urbanski, H. F. (2023). Mechanisms underlying TDP-43 pathology and neurodegeneration: An updated mini-review. Frontiers in Aging Neuroscience, 15: 1142617. https://doi.org/10.3389/fnagi.2023.1142617
Pokrishevsky, E., DuVal, M. G., McAlary, L., Louadi, S., Pozzi, S., Roman, A., Plotkin, S. S., Dijkstra, A., Julien, J. P., Allison, W. T., & Cashman, N. R. (2024). Tryptophan residues in TDP-43 and SOD1 modulate the cross-seeding and toxicity of SOD1. The Journal of biological chemistry, 300(5), 107207. https://doi.org/10.1016/j.jbc.2024.107207
