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Creative Biolabs

Alzheimer's Disease Related Research Tools

Alzheimer's disease (AD) is the most common form of dementia, a complex neurodegenerative brain disorder characterized by the progressive impairment of cognitive functions, particularly memory, thinking, language, mood, and behavioral issues.

AD is biologically defined by the presence of β-amyloid (Abeta) -containing plaques and tau-containing neurofibrillary tangles. Abeta plaques are formed by the aggregation of beta-amyloid peptides, which are fragments of a larger protein called amyloid precursor protein (APP).

Tau tangles, on the other hand, result from the abnormal phosphorylation and aggregation of tau protein, which is normally involved in maintaining the stability of microtubules within neurons. In Alzheimer's disease, tau protein forms twisted filaments called neurofibrillary tangles.

The accumulation of beta-amyloid plaques and tau tangles initiates a cascade of events that contribute to the progressive neurodegeneration observed in AD. This includes the activation of immune cells (microglia), inflammation, impairment of synaptic connections, and disruption of various signaling pathways in the brain.

As the disease progresses, affected individuals experience a decline in cognitive abilities, memory loss, disorientation, language difficulties, and changes in behavior and personality.

Biological Processes and Targets Related to Alzheimer's Disease

Pathophysiology of Alzheimer's disease.Fig1. Pathophysiology of Alzheimer's disease. (Dhapola, 2021)

Biological processes Targets
Amyloid-beta plaques formation APP, Aβ, PSEN1, PSEN2, B2M, Gal-3, AICD, BACE1, RAGE, ADAM, ApoE4, NEP, IDE, GSK-3
Neurofibrillary tangle formation Tau, NF-kB, TNF-α, ILs, Cdc42, GSK-3β, CDK5, TPK-1, MARK, MAPK, AMPK, Dyrk1A, p53, PAC1R, ERK, CREB, CaMKII
Neuroinflammation TNF-α, TREM2, CD33, NF-κB, CD36, Calhm2, NLRP2, APOE, PGE2, IL-1, IL-2, IL-4, IL-1β, IL-6, IL-10, IFN-γ, TGF-β, SR-A, CR1, ABCA7, KMO, IFN-γ, P2X7R, TLR, CSF1R, miR-155, STAT3, CaSR, ABCA1, BACE1, Aqp4
Oxidative stress NRF2, NADPH, PGC1α, miRNA-485, SIRT-1, PPAR-α
Mitochondrial dysfunction PGC1α
Cholinergic insufficiency AChE, BuChE, NGF
Autophagy dysfunction PKA, Drp-1, Parkin, mTOR, AMPK, LOX
Neurovascular dysfunction GLUT1, LRP1, P-gp, RAGE, CypA-MMP9
Synapse loss and alterations NLRP3, RhoA, BDNF, PKCɛ, Jacob, NCAM, MAPK, ERK, NGF, ACSS2, CREB, NMDAR
Ferroptosis NRF2, GPX4, GSS
Lipid dyshomeostasis APOE, HMG-CoA, ACAT1
Genetic risk factor APOE4, APP, PSEN1, PSEN2

Creative Biolabs offers a wide range of cutting-edge research products geared toward the investigation of biological processes underlying Alzheimer's disease. Our products including antibodies, cell lines, proteins & peptides, and assay kits, are among the bio-reagents keenly sought by neuroscience researchers.

Reference

  1. Dhapola, R.; et al. Recent advances in molecular pathways and therapeutic implications targeting neuroinflammation for Alzheimer's disease. Inflammopharmacology. 2021, 29(6): 1669-1681.
For Research Use Only. Not For Clinical Use.

Target

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Host Species:
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Species Reactivity:
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Mouse
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Human; Mouse; Rat
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WB; DB; IHC; ICC; IF; ELISA
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Mouse Monoclonal [3F8] to Alpha Synuclein

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Species Reactivity:
Human; Mouse; Rat
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WB; DB; IHC; ICC; IF; ELISA
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Rabbit Monoclonal Antibody to Alpha-synuclein

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Rabbit
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