Mouse Acetylcholinesterase(AChE)ELISA Kit
產(chǎn)品詳情
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產(chǎn)品描述:
This Mouse AChE ELISA Kit was designed for the quantitative measurement of Mouse AChE protein in serum, plasma, cell culture supernates, tissue homogenates. It is a Sandwich ELISA kit, its detection range is 0.312 mU/mL-20 mU/mL and the sensitivity is 0.078 mU/mL.
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別名:
Ache ELISA Kit; Acetylcholinesterase ELISA Kit; AChE ELISA Kit; EC 3.1.1.7 ELISA Kit
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縮寫:
AChE
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Uniprot No.:
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種屬:
Mus musculus (Mouse)
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樣本類型:
serum, plasma, cell culture supernates, tissue homogenates
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檢測范圍:
0.312 mU/mL-20 mU/mL
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靈敏度:
0.078 mU/mL
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反應(yīng)時間:
1-5h
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樣本體積:
50-100ul
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檢測波長:
450 nm
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研究領(lǐng)域:
Neuroscience
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測定原理:
quantitative
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測定方法:
Sandwich
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精密度:
Intra-assay Precision (Precision within an assay): CV%<8% | | | |
Three samples of known concentration were tested twenty times on one plate to assess. | |
Inter-assay Precision (Precision between assays): CV%<10% | | | |
Three samples of known concentration were tested in twenty assays to assess. | | |
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線性度:
To assess the linearity of the assay, samples were spiked with high concentrations of mouse AChE in various matrices and diluted with the Sample Diluent to produce samples with values within the dynamic range of the assay. |
| Sample | Serum(n=4) | |
1:100 | Average % | 90 | |
Range % | 84-96 | |
1:200 | Average % | 96 | |
Range % | 91-104 | |
1:400 | Average % | 95 | |
Range % | 90-100 | |
1:800 | Average % | 95 | |
Range % | 88-102 | |
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回收率:
The recovery of mouse AChE spiked to levels throughout the range of the assay in various matrices was evaluated. Samples were diluted prior to assay as directed in the Sample Preparation section. |
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Sample Type | Average % Recovery | Range | |
Serum (n=5) | 94 | 89-101 | |
EDTA plasma (n=4) | 98 | 92-104 | |
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標(biāo)準(zhǔn)曲線:
These standard curves are provided for demonstration only. A standard curve should be generated for each set of samples assayed. |
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mU/ml | OD1 | OD2 | Average | Corrected | | 20 | 2.313 | 2.413 | 2.363 | 2.260 | | 10 | 1.498 | 1.598 | 1.548 | 1.445 | | 5 | 0.840 | 0.830 | 0.835 | 0.732 | | 2.5 | 0.479 | 0.489 | 0.484 | 0.381 | | 1.25 | 0.306 | 0.316 | 0.311 | 0.208 | | 0.625 | 0.197 | 0.207 | 0.202 | 0.099 | | 0.312 | 0.135 | 0.146 | 0.141 | 0.038 | | 0 | 0.103 | 0.103 | 0.103 | | |
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本試劑盒所含材料:
- A micro ELISA plate --- The 96-well plate has been pre-coated with an anti-mouse AChE antibody. This dismountable microplate can be divided into 12 x 8 strip plates.
- Two vials lyophilized standard ---Dilute a bottle of the standard at dilution series, read the OD values, and then draw a standard curve.
- One vial Biotin-labeled AChE antibody (100 x concentrate) (120 μl/bottle) ---Act as the detection antibody.
- One vial HRP-avidin (100 x concentrate) (120 μl/bottle) ---Bind to the detection antibody and react with the TMB substrate to make the solution chromogenic.
- One vial Biotin-antibody Diluent (15 ml/bottle) ---Dilute the Biotin-antibody.
- One vial HRP-avidin Diluent (15 ml/bottle) ---Dilute the HRP-avidin solution.
- One vial Sample Diluent (50 ml/bottle)---Dilute the sample to an appropriate concentration.
- One vial Wash Buffer (25 x concentrate) (20 ml/bottle) ---Wash away unbound or free substances.
- One vial TMB Substrate (10 ml/bottle) ---Act as the chromogenic agent. TMB interacts with HRP, eliciting the solution turns blue.
- One vial Stop Solution (10 ml/bottle) ---Stop the color reaction. The solution color immediately turns from blue to yellow.
- Four Adhesive Strips (For 96 wells) --- Cover the microplate when incubation.
- An instruction manual
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本試劑盒不含材料:
- A microplate reader capable of measuring absorbance at 450 nm, with the correction wavelength set at 540 nm or 570 nm.
- An incubator can provide stable incubation conditions up to 37°C±5°C.
- Centrifuge
- Vortex
- Squirt bottle, manifold dispenser, or automated microplate washer
- Absorbent paper for blotting the microtiter plate
- 50-300ul multi-channel micropipette
- Pipette tips
- Single-channel micropipette with different ranges
- 100ml and 500ml graduated cylinders
- Deionized or distilled water
- Timer
- Test tubes for dilution
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數(shù)據(jù)處理:
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貨期:
3-5 working days
引用文獻
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Myco-fabricated ZnO nanoparticles ameliorate neurotoxicity in mice model of Alzheimer’s disease via acetylcholinesterase inhibition and oxidative stress reduction
HA Abd Elmonem,Biometals,2023
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Potential therapeutic effects of antagonizing adenosine A2A receptor, curcumin and niacin in rotenone-induced Parkinson’s disease mice model
Motawi T K, et al,Molecular and Cellular Biochemistry,2019
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Effects of Phytochemicals on Blood Pressure and Neuroprotection Mediated Via Brain Renin-Angiotensin System
Hae Rin Kim, et al,Nutrients,2019
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Illumination with 630-nm red light reduces oxidative stress and restores memory by photo-activating catalase and formaldehyde dehydrogenase in SAMP8 mice
Miss Jingnan Zhang.et al,ANTIOXID REDOX SIGN,2018
產(chǎn)品評價
樣品類型:血清
樣品信息:小鼠
稀釋比:其他 1:10
產(chǎn)品評價: 我用CSB-E17521m檢測小鼠血清ACHE水平,其OD如圖所示,試劑盒樣本充足,樣本和稀釋液顏色對應(yīng)直觀,使用說明簡潔明了,操作容易上手,數(shù)據(jù)準(zhǔn)確,滿意。
靶點詳情
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功能:
Terminates signal transduction at the neuromuscular junction by rapid hydrolysis of the acetylcholine released into the synaptic cleft.
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基因功能參考文獻:
- Results indicate that direct inhibition of acetylcholinesterase activity and up-regulation of m1 muscarinic acetylcholine receptor expression in the striatum might contribute to the beneficial effects of alpha-asarone on locomotor hyperactivity in Fmr1 knock out mice. PMID: 27316341
- Data show that 1-month of oral treatment with beta-asarone reduces AChE, Abeta42, APP and Beclin-1 levels and alleviates some behavioral impairments by inhibiting the autophagy via regulating the PI3K/Akt/mTOR pathway in APP/PS1 transgenic mice. The results further support the exploration of beta-asarone as a possible disease-modifying agent for the treatment of Alzheimer's disease. PMID: 27737765
- Results indicate that adult onset hypothyroidism caused significant memory impairment and increased fear/anxiety. Moreover, the activity of both isoforms of AChE was reduced in all brain regions examined in a brain region- and isoform-specific manner. PMID: 27317840
- Unusually high AChE activity may be an effect marker of exposure to ethanol. The relationship between AChE and apoptosis might represent a novel mechanism of ethanol-associated neuronal injury. PMID: 28427893
- Findings suggested the role of DNA methylation on acetylcholinesterase transcriptional regulation and provided insight in elucidating the DNA methylation-mediated regulatory mechanism on acetylcholinesterase expression during muscle differentiation. PMID: 27021952
- Nerolidol-loaded nanospheres reverse memory impairment and to prevent increased ROS and TBARS levels due to amelioration of Na(+), K(+)-ATPase and AChE activities and to activation of the antioxidant enzymes, respectively. PMID: 27807596
- the amounts of AChE activity, AChE catalytic subunit, structure subunit PRiMA and the amount of acetylcholine, in the brain were not, significantly, altered, suggesting the role of P2Y1R in neuron could have different function as that in muscle. PMID: 27378627
- In P2Y1R (-/-) mice, acetylcholinesterase expression in muscle was markedly decreased. The proline-rich membrane anchor subunit was reduced by 60 %; while the collagen tail subunit was reduced by 50 %. AChE molecular forms in the muscle were not changed. PMID: 26036470
- Our results are discussed in the context of AChE inhibitor therapy as used in dementia. PMID: 26506622
- Reduction of AChE levels in prion-infected heterozygous AChE knock-out mice leads to slightly but significantly prolonged incubation time. PMID: 25853328
- mRNA expressions of brain specific fatty acid protein 7 (fabp-7) and phospholipase A2 group IV (pla2g4) were significantly downregulated in AChE-deficient mice. PMID: 24573602
- In silico studies in probing the role of kinetic and structural effects of different drugs for the reactivation of tabun-inhibited AChE. PMID: 24312449
- AChE is regulated in two neuronal cell lines by APP in a manner independent of the generation of sAPPalpha, sAPPbeta, and AICD. PMID: 23897820
- Deficiency or inhibition of acetylcholinesterase can decrease apoptosis and protect dopaminergic neurons in the neurotoxin model of Parkinson's disease. PMID: 23201480
- Attribute stress-inducible cognitive impairments to cholinergic-mediated induction of miR-132 and consequently suppressed synaptic ACHE. PMID: 22246100
- assayed the relative activities of AChE and BChE in membrane fractions and culture medium of three different neuronal cell lines, namely the neuroblastoma cell lines SH-SY5Y and NB7 and the basal forebrain cell line SN56 PMID: 23047022
- Long-lasting stress-inducible changes in AChE's promoter choices, identify the chromatin changes that support this long-term transcriptional memory, and reveal HDAC4 as a mediator of these effects in the hippocampus. PMID: 23236169
- binding of AChE to laminin-1 alters AChE activity and leads to increased neurite growth in culture. A possible mechanism of the AChE effect on neurite outgrowth is proposed due to the interaction of AChE with laminin-1. PMID: 22570738
- The reduction of muscle end-plate AChE activity early during the onset of STZ-induced hyperglycemia may contribute to endplate pathology and subsequent muscle weakness during diabetes. PMID: 22739110
- Acetylcholinesterase is associated with apoptosis in beta cells and contributes to insulin-dependent diabetes mellitus pathogenesis PMID: 22236578
- Report effects of K074 and pralidoxime on antioxidant response and acetylcholinesterase reactivation in malathion-poisoned mice. PMID: 21723318
- Brain acetylcholinesterase activity in Dst(dt-J) mutants, revealed increases in the neostriatum, the habenula-interpeduncular pathway, the cholinergic pedunculopontine nucleus and its target structures. PMID: 21978551
- Dietary restriction regulates brain acetylcholinesterase in female mice as a function of age. PMID: 21870149
- PUM2 binds to AChE mRNA and regulates AChE expression translationally at the neuromuscular synapse. PMID: 21865157
- Electrophysiological and ultrastructural studies were performed on phrenic nerve-hemidiaphragm preparations isolated from wild-type and acetylcholinesterase (AChE) knockout (KO) mice. PMID: 21538119
- Results confirm the results of previous molecular dynamics simulations, expand the view and suggest the probable reasons for the overall conformational behavior of AChE omega loop. PMID: 20919754
- AChE activity is present both in the primary cleft and in the secondary folds, whereas BChE activity appears to be almost absent in the primary cleft and to be concentrated in subsynaptic folds. PMID: 20805581
- the function and localization of AChE in mammalian systems PMID: 20153304
- RNA expression profiles of the muscles of AChE knockout mice compared with those of the wild-type siblings PMID: 20381477
- AChE may be a pro-apoptotic factor and the inhibition of AChE reduces renal ischemia-reperfusion injury. PMID: 20054652
- these findings identify the AChE mRNA-targeting miR-132 as a functional regulator of the brain-to-body resolution of inflammation. PMID: 20005135
- neuronal hypersensitivity under stress involves neuritic replacement of acetylcholinesterase-S with acetylcholinesterase-R PMID: 11799248
- The effects of porphyrinogenic drugs on the brain cholinergic system (Ache, Bche, and Chrm1 levels in various regions of the brain) were examined to establish a mechanism for neurological syndrome displayed in acute porphyrias. PMID: 11929041
- regulation of ACHE expression in developing muscle cells PMID: 12140295
- Inhibitors of different structure induce distinguishing conformations in the omega loop. PMID: 12196517
- ligand interactions of the enzyme at the peripheral anionic site PMID: 12505979
- Interaction with RACKq and PKCbeta II correlates with intensified fear-induced conflict behavior PMID: 12509514
- an analysis of the active site and conformation PMID: 12665427
- fluctuations of the Omega loop residues are not tightly coupled and residues in the Omega loop exhibit distinctive conformational fluctuations and therefore are likely to contribute to transient gorge enlargements in the non-liganded enzyme. PMID: 12759360
- Acetylcholinesterase[AChE] histochemistry revealed an abnormal distribution of AChE-positive cells in several areas of the reeler brain, including cortices; the strongest labelling was observed in cerebellum and hippocampus when compared with controls PMID: 14535959
- primary role for stress-induced alternative splicing of the AChE gene to elevated contextual fear and synaptic plasticity, and the AChE-R splice variant has a major role in this process. PMID: 14581933
- Molecular modeling studies suggest that E2020 interacts with the active-site and the peripheral anionic site in AChE PMID: 14622273
- Data suggest that alternative promoter usage combined with alternative splicing may lead to stress-dependent combinatorial complexity of acetylcholinesterase mRNA transcripts and their protein products. PMID: 15123727
- Data describe up-regulation of acetylcholinesterase activity and compensatory down-regulation of M2 muscarinic receptors in the striatal caudate putamen and nucleus accumbens of mu-opioid receptor knockout mice. PMID: 15207914
- biophysical diffusion reaction rate calculations of wild-type and mutant mouse acetylcholinesterase PMID: 15345536
- AChE is involved in regulating cell-matrix interactions in bone PMID: 15454088
- Impaired formation of the inner retina in an AChE knockout mouse results in degeneration of all photoreceptors. PMID: 15579149
- HuR interacts with the AChE 3'-UTR to regulate posttranscriptionally the expression of AChE mRNA during myogenic differentiation PMID: 15878846
- structural studies of active center gorge of AChe PMID: 16259971
- neuromuscular system exhibits a remarkable plasticity and adaptive responses to the chronic absence of AChE activity that has important consequences for the functioning of the neuromuscular junction PMID: 16274683
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亞細胞定位:
Cell junction, synapse. Secreted. Cell membrane; Peripheral membrane protein.; [Isoform H]: Cell membrane; Lipid-anchor, GPI-anchor; Extracellular side.
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蛋白家族:
Type-B carboxylesterase/lipase family
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組織特異性:
Predominates in most expressing tissues except erythrocytes where a glycophospholipid-attached form of ACHE predominates.
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