Presenilin-1 Antibody, NT, clone hPS1-NT | EMD Millipore MAB1563 product information

This webpage contains legacy information. The product is either no longer available from the supplier or has been delisted at Labome.

product summary

company name :

EMD Millipore

other brands :

Oncogene Research Products, Calbiochem, Novagen, Merck, Upstate Biotechnology, Chemicon, LINCO, Novabiochem, Guava

product type :

antibody

product name :

Presenilin-1 Antibody, NT, clone hPS1-NT

catalog :

MAB1563

quantity :

100 μL

clonality :

monoclonal

host :

rat

conjugate :

nonconjugated

clone name :

hPS1-NT

reactivity :

hamsters, human, mouse

application :

western blot, ELISA, immunohistochemistry, immunoprecipitation

citations: 36

Published Application/Species/Sample/Dilution	Reference
western blot; human; 1:1000; loading ...; fig 4a	Gerber H, Mosser S, Boury Jamot B, Stumpe M, Piersigilli A, Goepfert C, et al. The APMAP interactome reveals new modulators of APP processing and beta-amyloid production that are altered in Alzheimer's disease. Acta Neuropathol Commun. 2019;7:13 pubmed publisher
western blot; hamsters; fig 6b immunoprecipitation; mouse; fig 4d western blot; mouse; fig 4b	Kuzuya A, Zoltowska K, Post K, Arimon M, Li X, Svirsky S, et al. Identification of the novel activity-driven interaction between synaptotagmin 1 and presenilin 1 links calcium, synapse, and amyloid beta. BMC Biol. 2016;14:25 pubmed publisher
western blot; human; fig 2	Chhibber Goel J, Coleman Vaughan C, Agrawal V, Sawhney N, Hickey E, Powell J, et al. Î³-Secretase Activity Is Required for Regulated Intramembrane Proteolysis of Tumor Necrosis Factor (TNF) Receptor 1 and TNF-mediated Pro-apoptotic Signaling. J Biol Chem. 2016;291:5971-85 pubmed publisher
western blot; hamsters; fig 4	Chen A, Kim S, Shepardson N, Patel S, Hong S, Selkoe D. Physical and functional interaction between the Î±- and Î³-secretases: A new model of regulated intramembrane proteolysis. J Cell Biol. 2015;211:1157-76 pubmed publisher
immunoprecipitation; human western blot; human	Marinangeli C, Tasiaux B, Opsomer R, Hage S, Sodero A, Dewachter I, et al. Presenilin transmembrane domain 8 conserved AXXXAXXXG motifs are required for the activity of the Î³-secretase complex. J Biol Chem. 2015;290:7169-84 pubmed publisher
immunoprecipitation; human; 1:1000 western blot; human	Chen W, Hsieh Y, Huang Y, Lin C, Lin Y, Liu Y, et al. G206D Mutation of Presenilin-1 Reduces Pen2 Interaction, Increases AÎ²42/AÎ²40 Ratio and Elevates ER Ca(2+) Accumulation. Mol Neurobiol. 2015;52:1835-1849 pubmed publisher
	Poppe L, Rue L, Timmers M, Lenaerts A, Storm A, Callaerts Vegh Z, et al. EphA4 loss improves social memory performance and alters dendritic spine morphology without changes in amyloid pathology in a mouse model of Alzheimer's disease. Alzheimers Res Ther. 2019;11:102 pubmed publisher
	Kwart D, Gregg A, Scheckel C, Murphy E, Paquet D, Duffield M, et al. A Large Panel of Isogenic APP and PSEN1 Mutant Human iPSC Neurons Reveals Shared Endosomal Abnormalities Mediated by APP β-CTFs, Not Aβ. Neuron. 2019;104:256-270.e5 pubmed publisher
	Petit D, Hitzenberger M, Lismont S, Zoltowska K, Ryan N, Mercken M, et al. Extracellular interface between APP and Nicastrin regulates Aβ length and response to γ-secretase modulators. EMBO J. 2019;: pubmed publisher
	Arber C, Toombs J, Lovejoy C, Ryan N, Paterson R, Willumsen N, et al. Familial Alzheimer's disease patient-derived neurons reveal distinct mutation-specific effects on amyloid beta. Mol Psychiatry. 2019;: pubmed publisher
	Chong C, Ke M, Tan Y, Huang Z, Zhang K, Ai N, et al. Presenilin 1 deficiency suppresses autophagy in human neural stem cells through reducing ?-secretase-independent ERK/CREB signaling. Cell Death Dis. 2018;9:879 pubmed publisher
	Hu J, Dziumbla S, Lin J, Bibli S, Zukunft S, de Mos J, et al. Inhibition of soluble epoxide hydrolase prevents diabetic retinopathy. Nature. 2017;552:248-252 pubmed publisher
	Guix F, Sannerud R, Berditchevski F, Arranz A, HorrÃ© K, Snellinx A, et al. Tetraspanin 6: a pivotal protein of the multiple vesicular body determining exosome release and lysosomal degradation of amyloid precursor protein fragments. Mol Neurodegener. 2017;12:25 pubmed publisher
	Li N, Liu K, Qiu Y, Ren Z, Dai R, Deng Y, et al. Effect of Presenilin Mutations on APP Cleavage; Insights into the Pathogenesis of FAD. Front Aging Neurosci. 2016;8:51 pubmed publisher
	Elad N, De Strooper B, Lismont S, Hagen W, Veugelen S, Arimon M, et al. The dynamic conformational landscape of gamma-secretase. J Cell Sci. 2015;128:589-98 pubmed
	Fernandez M, Klutkowski J, Freret T, Wolfe M. Alzheimer presenilin-1 mutations dramatically reduce trimming of long amyloid Î²-peptides (AÎ²) by Î³-secretase to increase 42-to-40-residue AÎ². J Biol Chem. 2014;289:31043-52 pubmed publisher
	Mosser S, Alattia J, Dimitrov M, Matz A, Pascual J, Schneider B, et al. The adipocyte differentiation protein APMAP is an endogenous suppressor of AÎ² production in the brain. Hum Mol Genet. 2015;24:371-82 pubmed publisher
	He P, Li P, Hua Q, Liu Y, Staufenbiel M, Li R, et al. Chronic administration of anti-stroke herbal medicine TongLuoJiuNao reduces amyloidogenic processing of amyloid precursor protein in a mouse model of Alzheimer's disease. PLoS ONE. 2013;8:e58181 pubmed publisher
	Alattia J, Matasci M, Dimitrov M, Aeschbach L, Balasubramanian S, Hacker D, et al. Highly efficient production of the Alzheimer's ?-secretase integral membrane protease complex by a multi-gene stable integration approach. Biotechnol Bioeng. 2013;110:1995-2005 pubmed publisher
	Alattia J, Schweizer C, Cacquevel M, Dimitrov M, Aeschbach L, Oulad Abdelghani M, et al. Generation of monoclonal antibody fragments binding the native ?-secretase complex for use in structural studies. Biochemistry. 2012;51:8779-90 pubmed publisher
	Leroy K, Ando K, Laporte V, Dedecker R, Suain V, Authelet M, et al. Lack of tau proteins rescues neuronal cell death and decreases amyloidogenic processing of APP in APP/PS1 mice. Am J Pathol. 2012;181:1928-40 pubmed publisher
	Cacquevel M, Aeschbach L, Houacine J, Fraering P. Alzheimer's disease-linked mutations in presenilin-1 result in a drastic loss of activity in purified ?-secretase complexes. PLoS ONE. 2012;7:e35133 pubmed publisher
	Chávez Gutiérrez L, Bammens L, Benilova I, Vandersteen A, Benurwar M, Borgers M, et al. The mechanism of ?-Secretase dysfunction in familial Alzheimer disease. EMBO J. 2012;31:2261-74 pubmed publisher
	Guix F, Wahle T, Vennekens K, Snellinx A, Chávez Gutiérrez L, Ill Raga G, et al. Modification of ?-secretase by nitrosative stress links neuronal ageing to sporadic Alzheimer's disease. EMBO Mol Med. 2012;4:660-73 pubmed publisher
	Wang T, Wang C, Shan Z, Teng W, Wang Z. Clioquinol reduces zinc accumulation in neuritic plaques and inhibits the amyloidogenic pathway in A?PP/PS1 transgenic mouse brain. J Alzheimers Dis. 2012;29:549-59 pubmed publisher
	Wang C, Zheng W, Wang T, Xie J, Wang S, Zhao B, et al. Huperzine A activates Wnt/?-catenin signaling and enhances the nonamyloidogenic pathway in an Alzheimer transgenic mouse model. Neuropsychopharmacology. 2011;36:1073-89 pubmed publisher
	Wang C, Wang T, Zheng W, Zhao B, Danscher G, Chen Y, et al. Zinc overload enhances APP cleavage and A? deposition in the Alzheimer mouse brain. PLoS ONE. 2010;5:e15349 pubmed publisher
	Wu F, Schweizer C, Rudinskiy N, Taylor D, Kazantsev A, Luthi Carter R, et al. Novel gamma-secretase inhibitors uncover a common nucleotide-binding site in JAK3, SIRT2, and PS1. FASEB J. 2010;24:2464-74 pubmed publisher
	Chen A, Guo L, Ostaszewski B, Selkoe D, LaVoie M. Aph-1 associates directly with full-length and C-terminal fragments of gamma-secretase substrates. J Biol Chem. 2010;285:11378-91 pubmed publisher
	Oh S, Chen C, Abraham C. Cell-type dependent modulation of Notch signaling by the amyloid precursor protein. J Neurochem. 2010;113:262-74 pubmed publisher
	Eckert G, Muller W. Presenilin 1 modifies lipid raft composition of neuronal membranes. Biochem Biophys Res Commun. 2009;382:673-7 pubmed publisher
	Hemming M, Elias J, Gygi S, Selkoe D. Proteomic profiling of gamma-secretase substrates and mapping of substrate requirements. PLoS Biol. 2008;6:e257 pubmed publisher
	Matsuda S, Giliberto L, Matsuda Y, McGowan E, D ADAMIO L. BRI2 inhibits amyloid beta-peptide precursor protein processing by interfering with the docking of secretases to the substrate. J Neurosci. 2008;28:8668-76 pubmed publisher
	Kienlen Campard P, Tasiaux B, Van Hees J, Li M, Huysseune S, Sato T, et al. Amyloidogenic processing but not amyloid precursor protein (APP) intracellular C-terminal domain production requires a precisely oriented APP dimer assembled by transmembrane GXXXG motifs. J Biol Chem. 2008;283:7733-44 pubmed publisher
	Fuso A, Cavallaro R, Zampelli A, D Anselmi F, Piscopo P, Confaloni A, et al. gamma-Secretase is differentially modulated by alterations of homocysteine cycle in neuroblastoma and glioblastoma cells. J Alzheimers Dis. 2007;11:275-90 pubmed
	Shaughnessy L, Thomas M, Wakefield J, Chamblin B, Nair A, Koentgen F, et al. Lentiviral vector-based models of amyloid pathology: from cells to animals. Curr Alzheimer Res. 2005;2:239-47 pubmed

product information

Catalog Number :

MAB1563

Subcategory :

Neuroscience

Product Name :

Anti-Presenilin-1 Antibody, NT, clone hPS1-NT

Product Type :

Antibodies

Clonality :

Monoclonal Antibody

Gene ID :

P49768

Host Name :

Rat

Antigen :

Presenilin-1

Clone :

hPS1-NT

Conjugate :

Culture Supernatant

Isotype :

IgG2a

Product Description :

Anti-Presenilin-1 Antibody, NT, clone hPS1-NT

Cross Reactivity :

Human

Immunogen :

A fusion protein antigen containing the N-terminus of human PS-1 (residues 21-80) fused to GST.

Specificity :

Recognizes Presenilin-1, human. By Western blot the antibody recognizes a predominant 32 kDa polypeptide in a variety of samples, including PC12 cells transfected with human PS1 complementary DNA, brain biopsy specimens from demented patients, and postmortem samples of frontal neucortex from Familial Alzheimer's Disease cases, late-onset Alzheimer's disease cases, and cases of other degenerative disorders. Immunohistochemical studies of control brains revealed that PS1 is expressed primarily in neurons, with the protein localizing in the soma and dendritic processes. In contrast in FAD and sporadic Alzheimer's disease cases, PS1 immunoreactivity was present in the neuritic component of senile plaques as well as in neurofibrillary tangles. Localization of PS1 immunoreactivity in familial and sporadic Alzheimer's disease suggest that genetically heterogeneous forms of the disease share a common pathophysiology involving PS1 protein.

Package Size :

100 μL

Uses :

ELISA;Immunohistochemistry;Immunoprecipitation;Western Blotting

Storage :

Maintain for 1 year at -20°C from date of shipment. Aliquot to avoid repeated freezing and thawing. For maximum recovery of product, centrifuge the original vial after thawing and prior to removing the cap.