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| Sample Type(s) | serum, plasma, tissue homogenates |
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Background
Interleukin 12 (IL-12/P70) is a biological molecule commonly studied in immunology research. It is commonly discussed as part of cytokine signaling that coordinates immune and inflammatory responses.
Biological context
Researchers often monitor Interleukin 12 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 Interleukin 12 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.
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 Interleukin 12 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.
IL-12-Overexpressed Nanoparticles Suppress the Proliferation of Melanoma Through Inducing ICD and Activating DC, CD8+ T, and CD4+ T Cells
HH Shen,International journal of nanomedicine,2024
Gene engineered exosome reverses T cell exhaustion in cancer immunotherapy
X Qin,Bioactive materials,2024
YAP/STAT3 inhibited CD8+ T cells activity in the breast cancer immune microenvironment by inducing M2 polarization of tumor‐associated macrophages
C Wang,Cancer medicine,2023
Enforced mesenchymal stem cell tissue colonization counteracts immunopathology
D García-Bernal,NPJ Regenerative Medicine,2022
Secretions from hypochlorous acid-treated tumor cells delivered in a melittin hydrogel potentiate cancer immunotherapy
Y Zhou,Bioactive materials,2022
Secretions from hypochlorous acid-treated tumor cells delivered in a melittin hydrogel potentiate cancer immunotherapy
Y Zhou,Bioactive Materials,2021
Toxoplasma gondii ROP16I Deletion: The Exacerbated Impact on Adverse Pregnant Outcomes in Mice
W Cui,Front Microbiol.,2020
Gluthathione S-transferase-resuscitation-promoting factor B recombinant protein of Mycobacterium tuberculosis induces the production of interferon-γ and interleukin-12 in mice splenocytes
Rukmana A, et al,Medical Journal of Indonesia,2019
Directed self-assembly of herbal small molecules into sustained release hydrogels for treating neural inflammation
Zheng J, et al,Nature Communications,2019
A Polysaccharide from Amusium Pleuronectes Combined with Praziquantel Treatment Ameliorates Hepatic Fibrosis in Schistosoma Japonicum-Infected Mice
Tang X.et al,Med Sci Monit,2018
Vaccination with FasL-/TCL plus MHSP65 induces improved anti-lung cancer immunity in mice
Dong B.et al,Int Immunopharmacol,2018