Human Major prion protein(PRNP) ELISA kit

Code CSB-EL018739HU
Size 96T,5×96T,10×96T
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Product Details

Target Name
prion protein
Alternative Names
Alternative prion protein, major prion protein ELISA Kit; AltPrP ELISA Kit; ASCR ELISA Kit; CD230 ELISA Kit; CD230 antigen ELISA Kit; CJD ELISA Kit; GSS ELISA Kit; KURU ELISA Kit; Major prion protein ELISA Kit; p27 30 ELISA Kit; PRIO_HUMAN ELISA Kit; Prion protein ELISA Kit; Prion related protein ELISA Kit; PRIP ELISA Kit; PRNP ELISA Kit; PrP ELISA Kit; PrP27 30 ELISA Kit; PrP27-30 ELISA Kit; PrP33-35C ELISA Kit; PrPC ELISA Kit; PrPSc ELISA Kit; Sinc ELISA Kit
Abbreviation
PRNP
Uniprot No.
Species
Homo sapiens (Human)
Sample Types
serum, plasma, tissue homogenates
Detection Range
0.312 ng/mL-20 ng/mL
Sensitivity
0.078 ng/mL
Assay Time
1-5h
Sample Volume
50-100ul
Detection Wavelength
450 nm
Research Area
Neuroscience
Assay Principle
quantitative
Measurement
Sandwich
Precision
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.
Linearity
To assess the linearity of the assay, samples were spiked with high concentrations of human PRNP in various matrices and diluted with the Sample Diluent to produce samples with values within the dynamic range of the assay.
SampleSerum(n=4)
1:1Average %87
Range %81-90
1:2Average %100
Range %96-104
1:4Average %93
Range %87-97
1:8Average %98
Range %91-103
Recovery
The recovery of human PRNP 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.
Sample TypeAverage % RecoveryRange
Serum (n=5) 9488-97
EDTA plasma (n=4)9387-98
Typical Data
These standard curves are provided for demonstration only. A standard curve should be generated for each set of samples assayed.
ng/mlOD1OD2AverageCorrected
202.502 2.444 2.473 2.331
102.089 2.024 2.057 1.915
51.426 1.411 1.419 1.277
2.50.930 0.939 0.935 0.793
1.250.588 0.568 0.578 0.436
0.6250.367 0.355 0.361 0.219
0.3120.281 0.287 0.284 0.142
00.140 0.144 0.142
Troubleshooting
and FAQs
Storage
Store at 2-8°C. Please refer to protocol.
Lead Time
3-5 working days after you place the order, and it takes another 3-5 days for delivery via DHL or FedEx
Description

This Human PRNP ELISA Kit was designed for the quantitative measurement of Human PRNP protein in serum, plasma, tissue homogenates. It is a Sandwich ELISA kit, its detection range is 0.312 ng/mL-20 ng/mL and the sensitivity is 0.078 ng/mL.

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Target Background

Function
(From Uniprot)
Its primary physiological function is unclear. May play a role in neuronal development and synaptic plasticity. May be required for neuronal myelin sheath maintenance. May promote myelin homeostasis through acting as an agonist for ADGRG6 receptor. May play a role in iron uptake and iron homeostasis. Soluble oligomers are toxic to cultured neuroblastoma cells and induce apoptosis (in vitro). Association with GPC1 (via its heparan sulfate chains) targets PRNP to lipid rafts. Also provides Cu(2+) or ZN(2+) for the ascorbate-mediated GPC1 deaminase degradation of its heparan sulfate side chains.
Gene References into Functions
  1. interaction site of peptide aptamer 8 in PrP and modeled the complex in silico to design targeted mutations in PA8 which presumably enhance binding properties. PMID: 29460268
  2. these data suggest that PrP protects cells against premature senescence induced by copper. PMID: 28800967
  3. These findings divulge a new cellular response that is activated upon CsA treatment to secrete misfolded PrP species from the cell and may underlie the spreading of toxic prions among cells and across tissues. PMID: 29127190
  4. Luman, a ubiquitous, non-canonical unfolded protein response (UPR), is identified as a novel regulator of endoplasmic reticulum stress-induced PRNP expression. PMID: 28205568
  5. These findings reveal that PrP enhances the responses to TNF-alpha, promoting proinflammatory cytokine production, which may contribute to inflammation and tumorigenesis. PMID: 28900035
  6. Bank vole asparagine and glutamine residues enable prion conversion of human and rabbit PrPC. PMID: 28931606
  7. Unlike the western populations, the diverse phenotypical presentations of D178N mutants of PRNP were not simply determined by the 129 genotypes in Chinese PMID: 29569252
  8. The octarepeat region within the PrP peptide markedly influences the effects of redox on the biochemical phenotypes of PrP, thus highlighting the importance of the number of octarepeats in the biological functions of PrP. PMID: 29393338
  9. Genetic prion diseases (gPrDs) are caused by autosomal-dominant mutations in the prion protein gene (PRNP). PMID: 29478593
  10. All these data suggest the possibility that hypoxiamediated PrPC serves an important role in angiogenesis. Therefore, the present review summarizes the characteristics of PrPC, which is produced by HIF1alpha in hypoxia, as it relates to angiogenesis PMID: 28901450
  11. This study is the first to demonstrate that tauroursodeoxycholic acid protects MSCs against ER stress via Akt-dependent PrP(C) and Akt-MnSOD pathway. PMID: 28004805
  12. The stabilization mechanism of specific binding compounds can be summarized as stabilizing both the flexible C-terminal of alpha2 and the hydrophobic core, or only the hydrophobic core, or the overall structure of PrP(C) by high binding affinity. N159 and Q160 play an major role in the specific binding of the studied compounds, all of which interact similarly with L130, P158, N159, Q160,H187, T190, T191. PMID: 28795797
  13. disease-associated mutations provide valuable insights into possible key structural determinants underlying misfolding of PrPC (review) PMID: 28838676
  14. This study reports a novel p.S17G mutation in a clinically diagnosed LOAD patient, suggesting that the PRNP mutation is present in Chinese Alzheimer's disease patients, whereas, M129V polymorphism is not a risk factor for Alzheimer's disease or frontotemporal dementia in the Chinese Han population. PMID: 27910931
  15. Those data indicate that the overexpression of PLK3-mediated degradation of abnormal PrP is largely dependent on chaperone-mediated autophagy pathway. PMID: 27344333
  16. biochemical characteristics of valine-to-isoleucine substitution at codon 180 (V180I) in PRNP gene from autopsied brains of patients with genetic Creutzfeldt-Jakob disease; findings indicate abnormal prion proteins in the neocortex are associated with toxicity resulting in severe spongiosis and that V180I is not a polymorphism, but is an authentic pathogenic mutation associated with specific biochemical characteristics PMID: 29382530
  17. mechanism of the unfolding of the human prion protein PMID: 28030950
  18. Here, we provide an overview of the increasingly multifaceted picture of prion protein proteolysis and shed light on physiological and pathological roles associated with these cleavages. PMID: 28693923
  19. the coordination bonds between the Methionine-Lysine-Histidine (Ac-MKH-NHMe) tripeptide model associated with the fifth metal binding site, which triggers the beta-sheet formation of human prion protein and the divalent metal cations such as Mn(2+), Cu(2+) and Zn(2+) were studied. PMID: 27611644
  20. Importantly, flies expressing human PrP showing a robust eye phenotype will allow performing genetic screens to uncover novel mechanisms mediating PrP neurotoxicity. PMID: 28415023
  21. Our results indicated, we found that PrP gene had an IRES-dependent translation initiation mechanism and we successfully identified the IRESs inside of the prion protein gene. PMID: 29107182
  22. the kinetics of prion replication occur in a prion protein codon 129 genotype-dependent manner, reflecting the genotype-dependent susceptibility to clinical variant Creutzfeldt-Jakob disease found in patients. PMID: 29141869
  23. the modulation of HOP-PrP(C) engagement or the decrease of PrP(C) and HOP expression may represent a potential therapeutic intervention in glioblastoma. PMID: 28412969
  24. a strong overexpression of PrP(C) is observed in human Merlin-deficient mesothelioma cell line TRA and in human Merlin-deficient meningiomas. PrP(C) contributes to increased proliferation, cell-matrix adhesion and survival in schwannoma cells acting via 37/67 kDa non-integrin laminin receptor (LR/37/67 kDa) PMID: 28692055
  25. Homozygous state of position 129 in the PRNP is not a risk factor for MSA. No other variants in the PRNP gene were associated with increased risk for MSA PMID: 27793473
  26. Transgenic Creutzfeldt-Jakob disease (CJD) mice, expressing the mouse PrP (moPrP) homolog of human PrP D178N/V129 (moPrP D177N/V128), closely reproduce essential features of CJD. The mutant PrPs expressed in these mice are misfolded but unable to self-replicate. They accumulate in different compartments of the neuronal secretory pathway, impairing the membrane delivery of ion channels essential for neuronal function. PMID: 26864450
  27. Identified are several nuclear PrP(c) partners, which comprise gamma-catenin, one of its desmosomal partners, beta-catenin and TCF7L2, the main effectors of the canonical Wnt pathway, and YAP, one effector of the Hippo pathway. PMID: 27216988
  28. Rare mutation in PRNP leading to an exchange of amino acid from glutamic acid (E) to alanine (A) at codon 196 (E196A) is associated with Creutzfeldt-Jacob disease. PMID: 27310471
  29. This article discusses a framework for investigating the extended hypothesis that PrPC may be involved in major depression associated with neurodegenerative conditions, with focus on the Transmissible Spongiform Encephalopathies (TSEs, or Prion Diseases) and Alzheimer's Disease (AlzD). PMID: 27057694
  30. Expert commentary: Computational approaches provide novel insights into prion-like protein functions, their regulation and their role in disease. PMID: 28271922
  31. We suggest that reduction of PFN-1 expression by elevated levels of PrP(c) may contribute to protective effects PrP(c)-overexpressing SH-SY5Y cells confer against STS-induced apoptosis PMID: 28102851
  32. findings show that sPrPc is involved in the processes of HIV neuropathogenesis and contributes to inflammation and neuronal damage PMID: 28533442
  33. Copper(II) interaction with the Human Prion 103-112 fragment and its mutants has been studied with various techniques. The studied human prion fragment contains both histidine and methionine residues, while methionine residues are systematically replaced or displaced in the studied mutants PMID: 28260678
  34. these data indicate that the disruption of the PrP(C)-HOP complex could be a potential therapeutic target for modulating the migratory and invasive cellular properties that lead to metastatic Colorectal cancer (CRC). PMID: 27112151
  35. computational approach to elucidate in details the aggregation propensity of PrP protein systems including wild type, wild type treated at different [Ca2+] or E200K mutant; models for the self-assembly of either the E200K mutated or Ca2+-bound PrPC were sketched and discussed PMID: 27959938
  36. The results have unraveled a novel molecular pathway driven by interactions between prion protein (PrP) and Notch1 in the progression of pancreatic ductal adenocarcinoma (PDAC), supporting a critical tumor-promoting role of Notch1 in PrP-expressing PDAC tumors. PMID: 27639164
  37. The present findings unveil particular neuropathological and neuroinflammatory profiles in Fatal familial insomnia(FFI) and novel characteristics of natural prion protein in FFI, altered PrPres and Scrapie PrP (abnormal and pathogenic PrP) patterns and region-dependent putative capacity of PrP seeding PMID: 27056979
  38. the data indicate a four-rung beta-solenoid structure as a key feature for the architecture of infectious mammalian prions. PMID: 27606840
  39. Distinctive properties of plaque-type dura mater graft-associated Creutzfeldt-Jakob disease PrPSc proteins in cell-protein misfolding cyclic amplification. PMID: 26878132
  40. Molecular insights obtained through MD (molecular dynamics) simulations suggested that each bispidine-based peptidomimetic differently engages a conserved Tyr 169 residue at the alpha2-beta2 loop of HuPrP and affects the stability of alpha2 and alpha3 helices. PMID: 27803245
  41. These data identify a network of proteins implicated in PrP(C) trafficking and demonstrate the power of this assay for identifying modulators of PrP(C) trafficking. PMID: 28341739
  42. Active compounds do not alter total or cell-surface levels of PrP(C), and do not bind to recombinant PrP in surface plasmon resonance experiments, although at high concentrations they inhibit PrP(Sc)-seeded conversion of recombinant PrP to a misfolded state in an in vitro reaction (RT-QuIC). PMID: 27803163
  43. data provided molecular details about the interaction between HuPrP and the NCAM fibronectin domain, and revealed a new role of PrP(C) N terminus as a dynamic and functional element responsible for protein-protein interaction. PMID: 27535221
  44. This work sheds light on the amyloid core structures underlying prion strains and how I138M, I139M, and S143N affect prion protein aggregation kinetics. PMID: 27576687
  45. Data suggest second and third helices (H2 and H3) of C-terminal region of prion protein serve as Achilles heels of prion protein stability; separation of B1-H1-B2 and H2-H3 domains seems to play a key role, as well. (H1, H2, H3 denote the 3 alpha-helices; B1, B1 denote the 2 beta-sheets. Studies involved molecular dynamic simulations using nuclear magnetic resonance data obtained for N-terminal and C-terminal domains.) PMID: 28102071
  46. prion protein-derived cell-penetrating peptide cytotoxicity is modulated by pH but independent of amyloid formation PMID: 27818203
  47. effect of familial Creutzfeld-Jacob disease prion genes on prion protein conformation and secondary structure PMID: 27107654
  48. The two cases reported here of sporadic Creutzfeldt-Jakob disease belonged to the same family and carried the most common point mutation of the PRNP gene observed in Italy. PMID: 26268049
  49. The protonation state of histidine 111 regulates the aggregation of the evolutionary most conserved region of the human prion protein. PMID: 27184108
  50. This study demonstrated that Prion Protein-Hemin Interaction Upregulates Hemoglobin Synthesis. PMID: 26836195

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Involvement in disease
Creutzfeldt-Jakob disease (CJD); Fatal familial insomnia (FFI); Gerstmann-Straussler disease (GSD); Huntington disease-like 1 (HDL1); Kuru (KURU); Spongiform encephalopathy with neuropsychiatric features (SENF)
Subcellular Location
Cell membrane; Lipid-anchor, GPI-anchor. Golgi apparatus.
Protein Families
Prion family
Database Links

HGNC: 9449

OMIM: 123400

KEGG: hsa:5621

STRING: 9606.ENSP00000368752

UniGene: Hs.472010

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