| Field | Specification |
|---|---|
| Mfr No | |
| Alternative Names | Neuron-specific enolase|NSE |
| Assay Time | |
| Detection Method | |
| Detection Range | |
| Product Type | |
| Reactivity | |
| Sample Type(s) | Serum, Plasma, Cell Culture Supernatant, cell or tissue lysate, Other liquid samples |
| Sensitivity | |
| Species | |
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| Target | |
| UniProt # |
Background
human NSE (Neuron-specific Enolase) high sensitivity is a molecular target commonly studied in biomedical research. Many proteins are studied as molecular readouts that can change with cellular state, tissue remodeling, or stress responses.
Biological role and mechanism
The biological role of NSE (Neuron-specific Enolase) high sensitivity is typically understood in terms of its molecular category and interaction network. Depending on the model system, it may participate in cell–cell communication, intracellular signaling, enzymatic processing, or regulation of gene expression programs. Mechanistic interpretation is often strengthened by considering upstream regulators and downstream readouts rather than relying on a single marker.
Expression and abundance of NSE (Neuron-specific Enolase) high sensitivity can vary by tissue, cell type, and physiological state. In many systems, levels are influenced by factors such as developmental stage, immune activation, metabolic status, and cellular stress. Because sample matrix and pre-analytical handling can affect measured concentrations, interpretation is typically strongest when experiments keep collection and processing consistent across groups.
Nomenclature and related terms
NSE (Neuron-specific Enolase) high sensitivity may also be referenced as Neuron-specific enolase and NSE in the literature or in databases. When comparing results across studies, confirm that the reported analyte refers to the same molecule, species context, and molecular form (e.g., precursor vs mature protein, or soluble vs membrane-associated forms).
Why it matters in research
- Understanding how NSE (Neuron-specific Enolase) high sensitivity relates to signal transduction, tissue homeostasis, stress responses, and disease-model biology in biomedical research.
- Interpreting shifts in NSE (Neuron-specific Enolase) high sensitivity levels alongside other pathway components or complementary markers.
- Connecting molecular changes to phenotypes such as inflammation, remodeling, metabolism shifts, or cell-state transitions (context-dependent).
Molecular forms and interpretation
For some targets, isoforms, proteolytic processing, or post-translational modifications (such as phosphorylation or glycosylation) can influence function and apparent abundance. If multiple molecular forms are expected in your model, align interpretation with the form most relevant to the biological question.
Disease and translational relevance
NSE (Neuron-specific Enolase) high sensitivity has been investigated across diverse physiological and disease contexts, and changes in its abundance have been reported in areas aligned with biomedical studies. These associations are interpreted as research findings rather than diagnostic or therapeutic claims, and they should be evaluated alongside model-specific covariates and study design.
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ENO2-derived phosphoenolpyruvate functions as an endogenous inhibitor of HDAC1 and confers resistance to antiangiogenic therapy
IF: 20.8 Journal: Nature Metabolism Author: State Key Laboratory of Bioactive Molecules and Druggability Assessment, Jinan University, Guangzhou, China Cited Date: 2023-09-08
Neuron specific enolase assay based on the perovskite CoSn(OH)6 for enhancing the anodic electrochemiluminescence of luminol
IF: 8.4 Journal: Sensors and Actuators: B. Chemical Author: Key Laboratory of Interfacial Reaction & Sensing Analysis in Universities of Shandong, School of Chemistry and Chemical Engineering, Collaborative Innovation Center for Green Chemical Manufacturing and Accurate Detection, University of Jinan, Jinan 250022 Cited Date: 2023-12-29
OGT-Mediated O-GlcNAcylation of ATF2 Protects Against Sepsis-Associated Encephalopathy by Inhibiting Microglial Pyroptosis
IF: 5.9 Journal: Neuroscience Bulletin Author: Medical Research Center, Affiliated Hospital 2 of Nantong University, Nantong, 226001, China. Cited Date: 2025-05-30
Alteration and clinical potential in gut microbiota in patients with cerebral small vessel disease
IF: 5.7 Journal: Frontiers in Cellular and Infection Microbiology Author: Department of Neurology, the Affiliated Wuxi People’s Hospital of Nanjing Medical University, Wuxi People’s Hospital, Wuxi Medical Center, Nanjing Medical University, Wuxi, China Cited Date: 2023-07-28
Ultrasensitive NSE detection by multisegmental nanowire modified immunosensor
IF: 5.1 Journal: Microchemical Journal Author: Ayd?n Adnan Menderes University, Faculty of Science, Department of Chemistry, Ayd?n, Türkiye Cited Date: 2025-10-11
Macrophage Migration Inhibitory Factor as a Potential Plasma Biomarker of Cognitive Impairment in Cerebral Small Vessel Disease
IF: 4.1 Journal: ACS Omega Author: Department of Neurology, the Affiliated Wuxi People's Hospital of Nanjing Medical University, Wuxi People's Hospital, Wuxi Medical Center, Nanjing Medical University, Wuxi 214023, China. Cited Date: 2024-04-12
Effects of Remote Ischemic Preconditioning on Postoperative Cognitive Dysfunction in Elderly Patients with Laparoscopic Cholecystectomy
IF: 2.145 Journal: International Journal of General Medicine Cited Date: 2023-03-24
Association between serum neuron-specific enolase levels and short-term brain injury in pediatric febrile convulsions: A cross-sectional study
IF: 1.4 Journal: Medicine Author: Department of Emergence, Maternal and Child Health Hospital of Hubei Province, Tongji Medical College, Huazhong University of Science and Technology, Wuhan, China. Cited Date: 2025-12-26