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AB263889

Human ACE ELISA Kit

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(5 Publications)

Human ACE ELISA Kit is a single-wash 90-min Simplestep used to quantify Human ACE with a sensitivity of 0.15 ng/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 5 citations

View Alternative Names

CD143, DCP, DCP1, ACE, Angiotensin-converting enzyme, Dipeptidyl carboxypeptidase I, Kininase II

5 Images
Sandwich ELISA - Human ACE ELISA Kit (AB263889)
  • sELISA

Supplier Data

Sandwich ELISA - Human ACE ELISA Kit (AB263889)

Interpolated concentrations of native ACE in human serum and plasma samples.

The concentrations of ACE were measured in duplicates, interpolated from the ACE standard curves and corrected for sample dilution. Undiluted samples are as follows : serum 7.5%, plasma (citrate) 15%, plasma (EDTA) 7.5% and plasma (heparin) 15%. The interpolated dilution factor corrected values are plotted (mean +/- SD, n=2). The mean ACE concentration was determined to be 303 ng/mL in neat serum, 259 ng/mL in neat plasma (citrate), 312 ng/mL in neat plasma (EDTA) and 245 ng/mL in neat plasma (heparin).

Sandwich ELISA - Human ACE ELISA Kit (AB263889)
  • sELISA

Supplier Data

Sandwich ELISA - Human ACE ELISA Kit (AB263889)

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 ACE concentration was determined to be 273 ng/mL with a range of 200 – 418 ng/mL.

Sandwich ELISA - Human ACE ELISA Kit (AB263889)
  • sELISA

Supplier Data

Sandwich ELISA - Human ACE ELISA Kit (AB263889)

Interpolated concentrations of native ACE in human lung tissue extract sample based on a 125 μg/mL extract load.

The concentrations of ACE were measured in duplicate and interpolated from the ACE standard curve and corrected for sample dilution. The interpolated dilution factor corrected values are plotted (mean +/- SD, n=2). The mean ACE concentration was determined to be 30 ng/mL in sample.

Sandwich ELISA - Human ACE ELISA Kit (AB263889)
  • sELISA

Supplier Data

Sandwich ELISA - Human ACE ELISA Kit (AB263889)

Example of human ACE standard curve in Sample Diluent NS.

The ACE 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.

Sandwich ELISA - Human ACE ELISA Kit (AB263889)
  • sELISA

Supplier Data

Sandwich ELISA - Human ACE ELISA Kit (AB263889)

Human ACE standard curve comparison.

Standard Curve comparison between human ACE SimpleStep ELISA kit and traditional ELISA kit from leading competitor. SimpleStep ELISA kit shows comparable sensitivity.

Key facts

Detection method

Colorimetric

Sample types

Cell culture media, Heparin Plasma, Citrate plasma, Serum, Cell Lysate, EDTA Plasma

Reacts with

Human

Assay type

Sandwich (quantitative)

Sensitivity

= 0.15 ng/mL

Range

0.625 - 40 ng/mL

Assay time

1h 30m

Assay Platform

Pre-coated microplate (12 x 8 well strips)

Reactivity data

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Product details

Human ACE ELISA Kit (ab263889) is a single-wash 90 min sandwich ELISA designed for the quantitative measurement of ACE protein in cell culture media, cell lysate, cit plasma, edta plasma, hep plasma, and serum. It uses our proprietary SimpleStep ELISA® technology. Quantitate Human ACE with 0.15 ng/ml sensitivity.

SimpleStep ELISA® technology 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. Our SimpleStep ELISA® technology provides several benefits:

- Single-wash protocol reduces assay time to 90 minutes or less
- High sensitivity, specificity and reproducibility from superior antibodies
- Fully validated in biological samples
- 96-wells plate breakable into 12 x 8 wells strips

A 384-well SimpleStep ELISA® microplate (ab203359) is available to use as an alternative to the 96-well microplate provided with SimpleStep ELISA® kits.

ACE (Angiotensin-converting enzyme) is an enzyme that converts angiotensin I to angiotensin II by release of the terminal His-Leu, this results in an increase of the vasoconstrictor activity of angiotensin. It is present as plasma membrane and soluble forms. ACE is also able to inactivate bradykinin, a potent vasodilator. ACE has also a glycosidase activity which releases GPI-anchored proteins from the membrane by cleaving the mannose linkage in the GPI moiety.

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.

Precision

[ { "reproducibilityType": "Inter", "sample": "Serum", "replicates": 3, "mean": null, "standardDeviation": null, "coefficientOfVariability": "3" }, { "reproducibilityType": "Intra", "sample": "Serum", "replicates": 8, "mean": null, "standardDeviation": null, "coefficientOfVariability": "3.4" } ]

Recovery

[ { "sample": "Serum", "range": "78 - 96 %", "average": "= 87" }, { "sample": "EDTA Plasma", "range": "102 - 109 %", "average": "= 104" }, { "sample": "Cell culture media", "range": "80 - 85 %", "average": "= 82" }, { "sample": "Heparin Plasma", "range": "80 - 94 %", "average": "= 87" }, { "sample": "Citrate plasma", "range": "84 - 86 %", "average": "= 86" } ]

What's included?

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Properties and storage information

Shipped at conditions
Blue Ice
Appropriate short-term storage conditions
+4°C
Appropriate long-term storage conditions
+4°C
Storage information
+4°C

Supplementary information

This supplementary information is collated from multiple sources and compiled automatically.

Angiotensin Converting Enzyme 1 also known as ACE1 or ACE is an important enzyme in the renin-angiotensin system. This enzyme exhibits a significant role in blood pressure regulation. ACE1 is a zinc-metallopeptidase with a molecular weight of approximately 130 kDa. It converts angiotensin I into the potent vasoconstrictor angiotensin II a critical function in cardiovascular physiology. ACE1 is widely expressed in endothelial cells particularly in the lungs kidneys and the small intestine.
Biological function summary

The enzyme generates angiotensin II by cleaving angiotensin I. Angiotensin II an important effector peptide impacts cardiovascular and renal systems influencing vasoconstriction and fluid balance. While not directly forming a complex ACE1's activity increases the potency of angiotensin II which binds to angiotensin II receptors to exert its effects therefore indirectly forming a functional signaling complex.

Pathways

ACE1 plays a central role in the renin-angiotensin system and the kallikrein-kinin system. The enzyme's activity boosts angiotensin II production which connects it to the regulation of blood pressure via the renin-angiotensin pathway. ACE1 also indirectly interacts with proteins like bradykinin by degrading them modulating kinin-related functions and influencing inflammation and tension in vascular smooth muscle.

Understanding ACE1 is important for addressing hypertension and congestive heart failure. ACE1's conversion of angiotensin I to angiotensin II means overactivity can cause elevated blood pressure leading to hypertension. This makes ACE inhibitors such as lisinopril and ramipril therapeutic for these conditions. Furthermore its connection with aldosterone production places ACE1 in relevance to heart failure as excessive aldosterone can cause detrimental remodeling of cardiac tissue.

Product protocols

Target data

Dipeptidyl carboxypeptidase that removes dipeptides from the C-terminus of a variety of circulating hormones, such as angiotensin I, bradykinin or enkephalins, thereby playing a key role in the regulation of blood pressure, electrolyte homeostasis or synaptic plasticity (PubMed : 15615692, PubMed : 20826823, PubMed : 2558109, PubMed : 4322742, PubMed : 7523412, PubMed : 7683654). Composed of two similar catalytic domains, each possessing a functional active site, with different selectivity for substrates (PubMed : 10913258, PubMed : 1320019, PubMed : 1851160, PubMed : 19773553, PubMed : 7683654, PubMed : 7876104). Plays a major role in the angiotensin-renin system that regulates blood pressure and sodium retention by the kidney by converting angiotensin I to angiotensin II, resulting in an increase of the vasoconstrictor activity of angiotensin (PubMed : 11432860, PubMed : 1851160, PubMed : 19773553, PubMed : 23056909, PubMed : 4322742). Also able to inactivate bradykinin, a potent vasodilator, and therefore enhance the blood pressure response (PubMed : 15615692, PubMed : 2558109, PubMed : 4322742, PubMed : 6055465, PubMed : 6270633, PubMed : 7683654). Acts as a regulator of synaptic transmission by mediating cleavage of neuropeptide hormones, such as substance P, neurotensin or enkephalins (PubMed : 15615692, PubMed : 6208535, PubMed : 6270633, PubMed : 656131). Catalyzes degradation of different enkephalin neuropeptides (Met-enkephalin, Leu-enkephalin, Met-enkephalin-Arg-Phe and possibly Met-enkephalin-Arg-Gly-Leu) (PubMed : 2982830, PubMed : 6270633, PubMed : 656131). Acts as a regulator of synaptic plasticity in the nucleus accumbens of the brain by mediating cleavage of Met-enkephalin-Arg-Phe, a strong ligand of Mu-type opioid receptor OPRM1, into Met-enkephalin (By similarity). Met-enkephalin-Arg-Phe cleavage by ACE decreases activation of OPRM1, leading to long-term synaptic potentiation of glutamate release (By similarity). Also acts as a regulator of hematopoietic stem cell differentiation by mediating degradation of hemoregulatory peptide N-acetyl-SDKP (AcSDKP) (PubMed : 26403559, PubMed : 7876104, PubMed : 8257427, PubMed : 8609242). Acts as a regulator of cannabinoid signaling pathway by mediating degradation of hemopressin, an antagonist peptide of the cannabinoid receptor CNR1 (PubMed : 18077343). Involved in amyloid-beta metabolism by catalyzing degradation of Amyloid-beta protein 40 and Amyloid-beta protein 42 peptides, thereby preventing plaque formation (PubMed : 11604391, PubMed : 16154999, PubMed : 19773553). Catalyzes cleavage of cholecystokinin (maturation of Cholecystokinin-8 and Cholecystokinin-5) and Gonadoliberin-1 (both maturation and degradation) hormones (PubMed : 10336644, PubMed : 2983326, PubMed : 7683654, PubMed : 9371719). Degradation of hemoregulatory peptide N-acetyl-SDKP (AcSDKP) and amyloid-beta proteins is mediated by the N-terminal catalytic domain, while angiotensin I and cholecystokinin cleavage is mediated by the C-terminal catalytic region (PubMed : 10336644, PubMed : 19773553, PubMed : 7876104).. Angiotensin-converting enzyme, soluble form. Soluble form that is released in blood plasma and other body fluids following proteolytic cleavage in the juxtamembrane stalk region.. Isoform Testis-specific. Isoform produced by alternative promoter usage that is specifically expressed in spermatocytes and adult testis, and which is required for male fertility (PubMed : 1651327, PubMed : 1668266). In contrast to somatic isoforms, only contains one catalytic domain (PubMed : 1651327, PubMed : 1668266). Acts as a dipeptidyl carboxypeptidase that removes dipeptides from the C-terminus of substrates (PubMed : 1668266, PubMed : 24297181). The identity of substrates that are needed for male fertility is unknown (By similarity). May also have a glycosidase activity which releases GPI-anchored proteins from the membrane by cleaving the mannose linkage in the GPI moiety. The GPIase activity was reported to be essential for the egg-binding ability of the sperm (By similarity). This activity is however unclear and has been challenged by other groups, suggesting that it may be indirect (By similarity).
See full target information ACE

Publications (5)

Recent publications for all applications. Explore the full list and refine your search

Frontiers in pharmacology 15:1484337 PubMed39555096

2024

Effects of inulin-type oligosaccharides (JSO) from . on behavioral deficits induced by chronic restraint stress in mice and associated molecular alterations.

Applications

Unspecified application

Species

Unspecified reactive species

Caihong Yao,Ning Jiang,Xinran Sun,Yiwen Zhang,Ruile Pan,Qinghu He,Qi Chang,Xinmin Liu

Journal of translational medicine 22:497 PubMed38796413

2024

Atox1 regulates macrophage polarization in intestinal inflammation via ROS-NLRP3 inflammasome pathway.

Applications

Unspecified application

Species

Unspecified reactive species

MingXian Chen,Yu Chen,Rui Fu,SaiYue Liu,HaiXia Li,TangBiao Shen

Pharmacy practice 21:2761 PubMed37090459

2023

The effect of omega-3 supplements on the serum levels of ACE/ACE2 ratio as a potential key in cardiovascular disease: A randomized clinical trial in participants with vitamin D deficiency.

Applications

Unspecified application

Species

Unspecified reactive species

Sara M Daboul,Mohammad Abusamak,Beisan A Mohammad,Ahmad R Alsayed,Maha Habash,Ibrahim Mosleh,Sami Al-Shakhshir,Reem Issa,Mahmoud Abu-Samak

Journal of the American Heart Association 11:e025989 PubMed35861811

2022

Renin-Angiotensin and Endothelin Systems in Patients Post-Takotsubo Cardiomyopathy.

Applications

Unspecified application

Species

Unspecified reactive species

Hilal Khan,Amelia Rudd,David T Gamble,Alice M Mezincescu,Lesley Cheyne,Graham Horgan,Neeraj Dhaun,David E Newby,Dana K Dawson

Drug design, development and therapy 16:2119-2132 PubMed35812134

2022

Palmatine Protects Against MSU-Induced Gouty Arthritis via Regulating the NF-κB/NLRP3 and Nrf2 Pathways.

Applications

Unspecified application

Species

Unspecified reactive species

Juan-Juan Cheng,Xing-Dong Ma,Gao-Xiang Ai,Qiu-Xia Yu,Xiao-Ying Chen,Fang Yan,Yu-Cui Li,Jian-Hui Xie,Zi-Ren Su,Qing-Feng Xie
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