| Field | Specification |
|---|---|
| Mfr No | |
| Alternative Names | COLEC 1 ELISA Kit; COLEC1 ELISA Kit; Collectin-1 ELISA Kit; HSMBPC ELISA Kit; Lectin; mannose-binding; soluble; 2 ELISA Kit; Mannan binding lectin ELISA Kit; Mannan binding protein ELISA Kit; Mannan-binding protein ELISA Kit; Mannose binding lectin (protein C) 2 soluble ELISA Kit; Mannose binding lectin (protein C) 2; soluble (opsonic defect) ELISA Kit; Mannose binding lectin (protein C) 2; soluble ELISA Kit; Mannose binding lectin 2 soluble ELISA Kit; Mannose binding lectin 2; soluble (opsonic defect) ELISA Kit; Mannose binding lectin ELISA Kit; Mannose binding lectin protein C2 soluble opsonic defect ELISA Kit; Mannose binding protein ELISA Kit; Mannose binding protein C ELISA Kit; Mannose binding protein C precursor ELISA Kit; Mannose binding protein; serum ELISA Kit; Mannose-binding lectin ELISA Kit; Mannose-binding protein C ELISA Kit; MBL 2 ELISA Kit; MBL ELISA Kit; MBL2 ELISA Kit; MBL2_HUMAN ELISA Kit; MBL2D ELISA Kit; MBP 1 ELISA Kit; MBP ELISA Kit; MBP C ELISA Kit; MBP-C ELISA Kit; MBP1 ELISA Kit; MBPB ELISA Kit; MBPC ELISA Kit; MBPD ELISA Kit; MGC116832 ELISA Kit; MGC116833 ELISA Kit; Opsonic defect ELISA Kit; protein C ELISA Kit; Soluble mannose binding lectin ELISA Kit |
| Assay Time | |
| Assay Type | |
| Detection Range | |
| Detection Wavelength | |
| Product Type | |
| Reactivity | |
| Sample Type(s) | serum, plasma, tissue homogenates. |
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| Species | |
| Target | |
| UniProt # |
Background
Mannma binding protein/mannan binding lectin (MBL2) is a biological molecule commonly studied in immunology research. It is commonly used as a molecular readout in mechanistic and biomarker-focused studies.
UniProt: P11226
Biological context
Researchers often monitor Mannma binding protein/mannan binding lectin 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 Mannma binding protein/mannan binding lectin 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, Mannma binding protein/mannan binding lectin may also appear under names such as COLEC 1 and COLEC1. 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 Mannma binding protein/mannan binding lectin participates in.
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Predictive value of soluble CD59 for poor 28-day neurological prognosis and all-cause mortality in patients after cardiopulmonary resuscitation: a prospective observatory study
L Wang,Journal of intensive care,2023
Lower level of complement component C3 and C3a in the plasma means poor outcome in the patients with hepatitis B virus related acute-on-chronic liver …
Q Li,BMC Gastroenterol,2020
High levels of urinary complement proteins are associated with chronic renal damage and proximal tubule dysfunction in IgA nephropathy
Lu Wen.et al,nephrology,2018
Interaction of mannose binding lectin and other pattern recognition receptors in human corneal epithelial cells during Aspergillus fumigatus infection
Xudong Peng, .et al,International Immunopharmacology,2018
Low levels of mannose-binding lectin at admission increase the risk of adverse neurological outcome in preterm infants: a 1-year follow-up study
Xue J. et al,J Matern Fetal Neonatal Med,2015
Prognostic Value of Mannose-Binding Lectin: 90-Day Outcome in Patients with Acute Ischemic Stroke
Zhang ZG et al,Mol Neurobiol,2014