StressMarq is pleased to introduce new active tau proteins in order to help researchers investigate tau aggregation, which is a hallmark of neurodegenerative diseases, including Alzheimer’s. StressMarq is the first to provide active tau preformed fibrils (PFFs) and filaments for neuroscience investigation.
The process of tau aggregation can be seeded by active tau PFFs, which recruit monomers to form bigger tau fibrils. This has been shown in thioflavin T assays where growth in fluorescence, suggestive of tau fibrillization, can be observed when active tau monomers are combined with active tau PFFs.
Particular tau PFFs have been injected into P301L mice, where they seed tau aggregation and induce tau pathology in the hippocampus. Fibrils and monomers are available both in the full-length isoform of the tau protein (2N4R or Tau-441) or a truncated form (K18). K18 tau has a molecular weight of approximately 15 kDa, whereas Tau-441 has a molecular weight of around 46 kDa.
Immunohistochemistry analysis of P301L mouse hippocampus injected with K18 P301L tau PFFs (SPR-330) shows seeding of tau pathology at injection site. AT8 (pSer202/pThr205) tau antibody shows tangle-like inclusions. Experiments performed at reMYND N.V. Image Credit: StressMarq Biosciences
dGAE is one of the core PHF subunits and is a fragment of the tau protein made up of amino acids 297-391.1 It includes both proline-rich regions and microtubule-binding domains, and assembles into PHF-like fibrils in vitro without templates or additives.2
Proteins are available with a number of mutations or as wild-type. P301S and P301L mutations happen in exon 10 and are linked with frontotemporal dementia. The P301L mutation promotes beta-sheet formation and the formation of PHFs and the P301S mutation decreases tau’s ability to assemble microtubules.
In tau research, both P301S and P301L mutant transgenic mouse models are employed. The K280 deletion mutation is also linked with frontotemporal dementia and in the absence of heparin and other inducers, promotes fibrillization into paired helical filaments (PHFs). The C322A mutation also heightens tau’s ability to form PHFs.2
PFFs induce tau aggregation; full-length PFFs may be more effective in seeding fibrillization, but a mixture of both can be especially toxic to neurons. Most tau types are fibrillized by utilizing a heparin scaffold; soluble tau filaments are fibrillized by utilizing a linear anionic scaffold. dGAE tau and K18 K280 deletion tau both fibrillize without scaffolds.
TEM of active recombinant Tau441 (2N4R), P301S mutant preformed fibrils (PFFs) (SPR-329). Image Credit: StressMarq Biosciences
TEM of active recombinant Tau (K18), P301L mutant preformed fibrils (PFFs) (SPR-330). Image Credit: StressMarq Biosciences
TEM of Human Recombinant Tau Protein Filaments (SPR-463). Image Credit: StressMarq Biosciences
StressMarq is in the process of developing new varieties of fibrils for neurodegenerative disease research in addition to thoroughly characterizing their current products. They currently possess multiple varieties of tau PFFs and filaments. The table below shows the differences between them.
Source: StressMarq Biosciences
| Catalog No. |
Protein |
Species |
Length/
Fragment |
Mutant |
Monomer
source |
Fibrillization
Scaffold |
In vivo
activity |
| SPR-329 |
2N4R,
P301S
PFFs |
Human |
2N4R
(441-amino acid)
Full length |
P301S |
SPR-327 |
Heparin |
Under Investigation |
| SPR-330 |
K18,
P301L
PFFs |
Human |
K18 (4R)
Truncated |
P301L |
SPR-328 |
Heparin |
Induces tau phosphorylation and aggregation in P301L transgenic mouse hippocampus |
| SPR-461 |
dGAE
PFFs |
Human |
dGAE (AA297-391)
Truncated |
WT |
SPR-444 |
|
Under Investigation |
| SPR-462 |
dGAE,
C322A
PFFs |
Human |
dGAE
(AA297-391)
Truncated |
C322A |
SPR-445 |
|
Under Investigation |
| SPR-463 |
2N4R,
P301S Filaments |
Human |
2N4R
(441-amino acid)
Full Length |
P301S |
SPR-327 |
Linear
Anionic
Scaffold |
Under Investigation |
| SPR-475 |
2N4R,
P301S
PFFs |
Mouse |
2N4R
(441-amino acid)
Full Length |
P301S |
SPR-474 |
Heparin |
Under Investigation |
| SPR-477 |
K18,
K280 Deletion PFFs |
Human |
K18 (4R)
Truncated |
ΔK280 |
SPR-476 |
|
Under Investigation |
References and Further Reading
- Novak, M. et al. (1993) EMBO J. 12, 365-370.
- Al-Hilaly, Y.K. et al. (2017) J. Mol. Biol. 429(23):3650-3665.
About StressMarq Biosciences
Established in 2007, StressMarq Biosciences Inc. is a supplier of life science products that operates out of Victoria, Canada with a small, but dedicated group of scientists. Headed by our CEO and President Dr. Ariel Louwrier, StressMarq provides the research community with high-quality reagents backed with rigorous quality control data, expert scientific support, and fast international delivery.
“Discovery through partnership, Excellence through quality”
With over 7,000 products, our growth can be attributed to the continual production of cutting edge research products. Our diverse portfolio of primary antibodies, antibody conjugates, proteins, immunoassay kits and small molecules bridges across the life sciences, including products for cancer research, cardiovascular disease, cell signaling and neuroscience. To aid research worldwide, StressMarq has an extensive network of international distributors that allow us to supply reagents to over 50 countries.
In the years to come, StressMarq will continue to aid life science research by providing “Discovery through partnership, and Excellence through quality”.
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