Amyloid-beta (N-term), Human, mAb VU17 - HM2325-20UG

Catalog #
HM2325-20UG
125,00 €
Antibody clone VU17, formerly known as αVU Aß 17, recognizes the N-terminus of human amyloid beta (i.e. in: Aβ1-38; Aβ1-39; Aβ1-40; Aβ1-42). Alzheimer disease (AD) is the most common form of dementia, and is characterized by the intra neuronal accumulation of the microtubule-associated protein tau (MAPT), and by extracellular deposits of amyloid beta (Aß) in the brain parenchyma. Aß deposits have different appearances, ranging from loosely organized to dense-cored, deposits, also called plaques, as well as deposits in the walls of small blood vessels. The Aβ peptides are a proteolytic cleavage product of the membrane bound amyloid precursor protein (APP), upon cleavage by APP-cleaving enzyme 1 (BACE1) and the γ-secretase complex. There are multiple cleavage sites in Aβ domain leading to various fragments of 36-43 amino acids in length. Aβ is produced by various cell types and is secreted into the interstitial fluid. Aß peptides are readily detectable in cerebrospinal fuid (CSF). Aβ terminating at residue 40 (Aβ40) being approximately 10 times more abundant than Aβ42. Whereas Aβ40 levels are unchanged in AD compared to control cases, Aβ42 levels in CSF are reduced. Therefore, Aβ42 levels and the Aβ42: Aβ40 ratio in CSF are of diagnostic importance. Assessment of Aβ levels and co-localization of Aβ with other factors and specific cell types in brain tissue is essential for investigating the molecular mechanisms underlying AD. Antibody VU17 detects all forms of Aβ deposits without the need for formic acid pre-treatment on paraffin sections and can be applied in a double staining strategy, making it suitable for investigating co-localization. Antibody VU17 is raised against synthetic Aβ1-17, and detects a region within the first six amino acids of the N-terminus of Aβ.
Weitere Informationen
Datasheet URL https://www.hycultbiotech.com/wp-content/uploads/2022/06/coa-tds_hm2325-20ug.pdf
Quantity 20 µg
Species Human
Alias Abeta, Aβ, β-Amyloid
Application Frozen sections, Immuno assays, Immuno precipitation, Paraffin sections, Western blot
Precautions For research use only. Not for use in or on humans or animals or for diagnostics. It is the responsibility of the user to comply with all local/state and federal rules in the use of this product. Hycult Biotech is not responsible for any patent infringements that might result from the use or derivation of this product.
References 1. Verwey, N et al; Immunohistochemical characterization of novel monoclonal antibodies against the N-terminus of amyloid β-peptide. Amyloid 2013, 20:3
2. Jongbloed, W et al; CSF Amyloid-ß oligomers in Alzheimer’s disease: Diagnostic value and relation to cognitive decline. J Alzheimer’s Dis. 2015 45:35
3. Rosenberger, A et al; Altered distribution of the EphA4 kinase in hippocampal brain tissue of patients with Alzheimer’s disease correlates with pathology. Acta Neuro Com 2014 2:79
4. Del Campo, M et al; BRI2-BRICHOS is increased in human amyloid plaques in early stages of Alzheimer’s disease. Neur Aging 2014 35:1596
5. Schuster, J et al; Methods for the Specific Detection and Quantitation of Amyloid-β Oligomers in Cerebrospinal Fluid. J Alzheimer Dis 2016, 53:53 (IA)
Disease Cardiology and metabolism, Neurological disorders
Applications
Application: Frozen sections Immuno assays Immuno precipitation Paraffin sections Western blot

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