Human Midkine ELISA Kit
- Recombinant
- SimpleStep
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(11 Publications)
Human Midkine ELISA Kit is a single-wash 90-min Simplestep used to quantify Human Midkine with a sensitivity of 14.4 pg/ml. The assay uses a simple mix-wash-read protocol with just one incubation and one wash step.
- Colorimetric Sandwich ELISA - 450 nm readout : works on any standard plate reader
- Design your own immunoassay: we also offer the conjugation-ready antibody pair
- Cited in over 10 citations
View Alternative Names
MK1, NEGF2, MDK, Midkine, MK, Amphiregulin-associated protein, Midgestation and kidney protein, Neurite outgrowth-promoting factor 2, Neurite outgrowth-promoting protein, ARAP
- ELISA
Supplier Data
ELISA - Human Midkine ELISA Kit (AB193761)
- sELISA
Supplier Data
Sandwich ELISA - Human Midkine ELISA Kit (AB193761)
Serum from ten individual healthy human male donors was measured in duplicate.
Interpolated dilution factor corrected values are plotted (mean +/- SD, n=2). The mean Midkine concentration was determined to be 164 pg/mL with a range of 69 – 594 pg/mL.
- sELISA
Supplier Data
Sandwich ELISA - Human Midkine ELISA Kit (AB193761)
Interpolated concentrations of native Midkine in human HepG2 and SH-SY5Y cell extract samples and samples based on a 50 μg/mL extract load.
The concentrations of Midkine were measured in duplicate and interpolated from the Midkine standard curve and corrected for sample dilution. The interpolated dilution factor corrected values are plotted (mean +/- SD, n=2). The mean Midkine concentration was determined to be 2641 pg/mL in HepG2 cell extract and 1179 pg/mL in SH-SY5Y cell extract.
- sELISA
Supplier Data
Sandwich ELISA - Human Midkine ELISA Kit (AB193761)
Interpolated concentrations of native Midkine in human cell culture supernatant samples.
The concentrations of Midkine were measured in duplicates, interpolated from the Midkine standard curves and corrected for sample dilution. Undiluted samples are as follows : HepG2 cell culture supernatant 2.5%. The interpolated dilution factor corrected values are plotted (mean +/- SD, n=2). The mean Midkine concentration was determined to be 6,242 pg/mL in serum.
- sELISA
Supplier Data
Sandwich ELISA - Human Midkine ELISA Kit (AB193761)
Interpolated concentrations of native Midkine in human serum, plasma samples.
The concentrations of Midkine were measured in duplicates, interpolated from the Midkine standard curves and corrected for sample dilution. Undiluted samples are as follows : serum 50%, plasma (EDTA) 50%, plasma (citrate) 25%, and plasma (heparin) 50%. The interpolated dilution factor corrected values are plotted (mean +/- SD, n=2). The mean Midkine concentration was determined to be 243 pg/mL in serum, 183 pg/mL in plasma (EDTA), 449 pg/mL plasma (citrate) and 303 pg/mL in plasma (heparin).
- sELISA
Unknown
Sandwich ELISA - Human Midkine ELISA Kit (AB193761)
Example of human Midkine standard curve in Sample Diluent NS.
The Midkine standard curve was prepared as described in Section 10. Raw data values are shown in the table. Background-subtracted data values (mean +/- SD) are graphed.
Reactivity data
Product details
Human Midkine ELISA Kit ab193761 is a rapid single-wash 90-min Sandwich ELISA to measure Human Midkine in cell culture extracts, cell culture supernatant, citrate plasma, EDTA plasma, heparin plasma, serum. This SimpleStep sensitivity is 14.4 pg/mL.
How the assay works
Human Midkine SimpleStep ELISA®employs capture antibodies conjugated to an affinity tag that is recognized by the monoclonal antibody used to coat our SimpleStep ELISA® plates. This approach to sandwich ELISA allows the formation of the antibody-analyte sandwich complex in a single step, significantly reducing assay time. See the SimpleStep ELISA® protocol summary in the image section for further details.
Assay Specificity
Our SimpleStep ELISA® kits use recombinant monoclonal antibodies rigorously validated to ensure the highest level of consistency and reproducibility, improved sensitivity and specificity and ease of scalability and security of supply.
Please refer to our protocol booklet for more details.
Human Midkine ELISA Kit ab193761 protocol summary
1. Mix: add samples/standards to the wells together with the capture and detector antibody cocktail. Incubate 1 hr at room temperature
2. Wash
3. Add TMB development solution - incubate for 10 min
4. Add Stop solution
5. Read the results on a plate reader at 450 nm
Design your own immunoassay
We offer the antibody pair used in this kit in a BSA and Azide-free format, ready for conjugation:
- Anti-Midkine antibody [EPR20371-14] - BSA and Azide free (Capture) ab259450
- Anti-Midkine antibody [EPR1143-68R] - BSA and Azide free (Detector) ab259450
Midkine (MK), also known as neurite growth-promoting factor 2 (NEGF2), is a 13kDa heparin-binding growth factor or cytokine composed of two domains: The N-terminally located N-domain and the C-terminally located C-domain, which are connected by a hinge. The C-domain plays a role in neuronal development, whereas the N-domain is important for protein stability and dimerization. MK is involved in development, reproduction, repair, inflammation, innate immunity, control of blood pressure and angiogenesis.
MK is strongly expressed during embryogenesis and due to its distribution in the embryo it has been proposed to play a role in neurogenesis, epithelial-mesenchymal interactions and mesoderm remodeling. Expression in adult tissues is restricted to the kidney, epidermis, bronchial epithelium, lymphocytes and macrophages, but it is strongly expressed in the brain, kidney, blood vessels and heart after tissue injury as well as during inflammation, infection and oncogenesis. During inflammation, substratum-bound MK enhances neutrophil and macrophage migration directly and through induction of chemokine expression. On the other hand, soluble MK is associated with differentiation of regulatory T-cells, induction of epithelial-mesenchymal transition, angiogenesis, fibrinolytic and anti-microbial activity.
MK signaling is mediated by cell surface receptors as well as membrane proteins such as Protein Tyrosine Phosphatase ζ (PTPζ), low density lipoprotein receptor-related proteins (LRP), Notch2, integrins, anaplastic lymphoma kinase (ALK) and neuroglycan C. Binding of MK to PTPζ induces tyrosine phosphorylation in β-catenin and Wnt signaling inhibition. Furthermore it induces phosphorylation of PI3K, MAPK, PKC and Src family kinase. Binding of MK to LRP leads to embryonic neuronal survival and prevention of hypoxic injury via Akt and HIF1α. Binding of MK to integrins activates focal adhesion kinase, paxillin and STAT1α pathway leading to increase invasiveness of cancer cells. Activation of ALK by MK leads to phosphorylation of IRS-1, MAPK, PI3K and activation of NF-κB.
Due to its multifunctionality, MK has become an emerging target of drug development for the treatment of multiple diseases. On the one hand, administration of MK ameliorates ischemic injury, enhances oocyte maturation and promotes neurogenesis therefore limiting the progression of neurodegenerative diseases. However on the other hand, due to its over-expression in malignant tumors and in inflammation, MK inhibitors may be useful in the treatment of cancer, multiple sclerosis, hypertension and osteoporosis.
REACH authorisation
Abcam has not and does not intend to apply for the REACH Authorisation of customers' uses of products that contain European Authorisation list (Annex XIV) substances.
It is the responsibility of our customers to check the necessity of application of REACH Authorisation, and any other relevant authorisations, for their intended uses.
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Publications (11)
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Nature communications 15:8447 PubMed39349474
2024
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Nature 625:557-565 PubMed38172636
2024
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Translational neurodegeneration 12:42 PubMed37667404
2023
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Nature communications 14:3620 PubMed37365178
2023
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Cell death discovery 9:92 PubMed36906597
2023
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Theranostics 11:2722-2741 PubMed33456569
2021
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Scientific reports 10:14499 PubMed32879333
2020
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EBioMedicine 41:185-199 PubMed30773478
2019
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Arthritis research & therapy 20:185 PubMed30115106
2018
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Journal of immunoassay & immunochemistry 39:84-98 PubMed29309212
2018
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