Human P-Selectin ELISA kit

SKU:BHE10504065
Overview
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Quantitative ELISA kit for measuring human P-Selectin (P-Selectin/CD62P) in serum, plasma, and tissue homogenates to support immunology studies. Sensitivity 0.225 ng/mL, detection range 0.9 ng/mL–60 ng/mL, typical assay time 1–5 h.
Target P Selectin
Species Homo sapiens (Human)
Sample Type(s) serum, plasma, tissue homogenates
Assay Type Sandwich ELISA (quantitative)
Sensitivity 0.225 ng/mL
Detection Range 0.9 ng/mL-60 ng/mL
Assay Time 1-5h
Options selector
Catalog no. Size
CSB-E04708h-96T 96 T
CSB-E04708h-96TX5 96 T×5
CSB-E04708h-96TX10 96 T×10
Available Options

Select from the available variant options shown for this product. Availability and lead time can vary by option.

  • Options: Size (96 T, 96 T×10, 96 T×5).
  • Lead time: options listed as "In Stock at Manufacturer" typically ship in 5–7 business days; other statuses may take longer.
  • Storage: refer to the product datasheet for storage and handling.
  • Sales terms and conditions: Please review prior to ordering.
Field Specification
Mfr No CSB-E04708h
Alternative Names Antigen CD62 ELISA Kit; CD62 ELISA Kit; CD62 antigen-like family member P ELISA Kit; CD62P ELISA Kit; GMP 140 ELISA Kit; GMP-140 ELISA Kit; GMP140 ELISA Kit; GMRP ELISA Kit; Granule membrane protein 140 ELISA Kit; Granulocyte membrane protein ELISA Kit; GRMP ELISA Kit; LECAM 3 ELISA Kit; LECAM3 ELISA Kit; Leukocyte endothelial cell adhesion molecule 3 ELISA Kit; Leukocyte-endothelial cell adhesion molecule 3 ELISA Kit; LYAM3_HUMAN ELISA Kit; P Selectin ELISA Kit; P-selectin ELISA Kit; PADGEM ELISA Kit; Platelet activation dependent granule-external membrane protein ELISA Kit; Platelet alpha granule membrane protein ELISA Kit; PSEL ELISA Kit; Selectin P (granule membrane protein 140kDa, antigen CD62) ELISA Kit; SELP ELISA Kit
Assay Time
  • 1-5h
Assay Type
  • Sandwich ELISA (quantitative)
Detection Range 0.9 ng/mL-60 ng/mL
Detection Wavelength 450 nm
Product Type
  • ELISA Kits
Reactivity
  • Human
Sample Type(s) serum, plasma, tissue homogenates
Sensitivity 0.225 ng/mL
Species Homo sapiens (Human)
Target P Selectin
UniProt # P16109

Background

P-Selectin (P-Selectin/CD62P) is a biological molecule commonly studied in immunology research. It is commonly used as a molecular readout in mechanistic and biomarker-focused studies.

UniProt: P16109

Biological context

Researchers often monitor P-Selectin in serum, plasma, and tissue homogenates to better understand themes such as innate and adaptive immune responses, cytokine signaling networks, and host–pathogen interactions. In many model systems, measured levels can shift with physiology, experimental perturbation, or disease-associated changes, making careful biological interpretation important.

Interpreting changes in measured levels

Depending on sample matrix and study design, increases or decreases in P-Selectin may reflect differences in expression, secretion, turnover, or compartmentalization rather than a single mechanism. Interpretation is typically strengthened by evaluating related molecules (for example, cytokines, chemokines, acute-phase proteins, and immune-cell activation markers) and by keeping pre-analytical variables consistent across groups.

Nomenclature

In publications and databases, P-Selectin may also appear under names such as Antigen CD62 and CD62. When comparing studies, confirm that the reported analyte refers to the same molecule and species context.

Why ELISA data are widely used

ELISA is a common approach for quantitative measurement of proteins and biomarkers in complex samples, enabling comparisons across experimental groups and time points. When integrating results with other readouts, consider species biology, sample type, and the broader pathway context that P-Selectin participates in.

Can’t Find What You’re Looking For? We can help you source the best match or customize an ELISA solution for your study. Options may include alternative target synonyms, different species reactivity, sample type/matrix compatibility (serum/plasma/lysate/supernatant), assay format (sandwich/competitive), sensitivity/range, detection chemistry (colorimetric/fluorescent/chemiluminescent), plate format (pre-coated/uncoated, strips vs full plate), and bulk or custom packaging. Click Talk to a Scientist to submit a request form, email us at support@biohippo.com, or explore our Research Services for additional support. Our team will be in contact with you shortly.

Proteomic insights into platelet dysregulation and pathogenic mechanisms of chronic thromboembolic pulmonary hypertension

L Sun, H Li, Y Li, X Li, H Tian, J Liu, M Liu,Journal of Translational Medicine,2025

PTH-Driven Modulation of Platelet Activity via the NOX2 Pathway in Postsurgical Hypoparathyroidism.

A D'Amico, G Tabacco, C Nocella, AM Naciu, A Nusca,Redox Biology,2025

Effect of Fixed-Angle and Horizontal Rotor Centrifugation on Optimized Platelet-Rich Plasma Preparation

M Xie, B Zhao, J Teng, L Yang, Z Wang, S Xu,Aesthetic Plastic Surgery,2025

Assessment of Some Platelet Activating Markers and Secretory Status with Clinical Manifestations in Multiple Sclerosis Iraqi Patients

KM Salih,Al-Mustansiriyah Journal of Science,2022

The COMPASS-COVID-19-ICU Study: Identification of Factors to Predict the Risk of Intubation and Mortality in Patients with Severe COVID-19

GT Gerotziafas,Hemato,2022

Platelet Surface CD62p and Serum Vitamin D Levels are Associated with Clopidogrel Resistance in Chinese Patients with Ischemic Stroke

Lu BC, et al,Journal Of Stroke & Cerebrovascular Diseases,2019

Longer procoagulant phospholipid-dependent clotting time, lower endogenous thrombin potential and higher tissue factor pathway inhibitor concentrations are associated with increased VTE occurrence in patients with newly diagnosed multiple myeloma: results

Fotiou D, et al,Blood Cancer Journal,2018

Procoagulant Phospholipid Dependent Clotting Time: A New Tool for the Identification of Multiple Myeloma Patients at Risk Poor Treatment Response

Fotiou Despina.et al,Blood,2017

Expression of P-selectin, TXA2, TGF-ß1 and PDGF-AB in the Presence of Bioadhesive Chitosan Derivatives

Mercy Halleluyah Periayah et al,Online International Interdisciplinary Research Journal,2014

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