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Tau (phospho T181) Mouse mAb (SDT-200-5)

货号: S0B3156

Datasheet COA
  • 价格: ¥5,000
  • 规格:
  • 数量:
斯达特大包装询价 大包装询价

产品介绍 引用文献(0) 评论(0)

产品规格
  • 宿主来源

    Mouse
  • 抗原名称

    Tau (phospho T181)
  • 分子别名

    p-Tau181, phospho T181
  • 免疫原

    Synthetic Peptide
  • Accession

    P10636
  • 克隆号

    SDT-200-5
  • 抗体类型

    Mouse mAb
  • 抗体同种型

    IgG1,k
  • 应用

    Sandwich ELISA
  • 反应种属 ?

    Hu, Ms
  • 预测反应种属
    (反应种属缩写表)

    Hu, Ms
  • 交叉反应

    Does not recognize total Tau
  • 纯化方式

    Protein G
  • 浓度

    5 mg/ml
  • 纯度

    >95% by HPLC
  • 标记

    Unconjugated
  • 性状

    Liquid
  • 缓冲体系

    PBS pH7.4, 0.03% Proclin 300
  • 储存条件

    12 months from date of receipt, 2 to 8 °C as supplied

稀释度
应用 稀释度
Sandwich ELISA N/A
背景介绍
  • Accumulation of intraneuronal neurofibrillary tangles (NFTs) containing paired helical filaments (PHFs) of the microtubule-associated protein tau is one of the defining neuropathological hallmarks of Alzheimer’s disease (AD). The tau protein has an N-terminal projection domain, a proline-rich region, a repeat region, and a C-terminal domain, with multiple potential phosphorylation sites along all regions. Studies using preparations of PHFs and immunohistochemical staining of postmortem brain tissue with specific tau antibodies established that PHF tau is hyperphosphorylated. High levels of p-tau and total tau (t-tau) have consistently been found in cerebrospinal fluid (CSF) of AD patients. However, while CSF t-tau is considered a non-specific biomarker of neuronal injury, p-tau may reflect AD-related tau pathology in the brain. The vast majority of CSF studies have used immunoassays detecting tau phosphorylated at threonine (Thr) 181 (p-tau181). During the last 2 decades, CSF p-tau181 together with total tau (t-tau) and amyloid-β 42 (Aβ42) have been extensively validated as biomarkers of AD and are currently widely used as diagnostic criteria in research studies, in clinical practice in some countries, and for patient selection in clinical trials. CSF p-tau181 (alone or in combination with Aβ42) accurately differentiates AD from controls and predicts cognitive decline in preclinical and prodromal disease stages. CSF p-tau181 levels are higher in AD compared with other tauopathies including frontotemporal dementia (FTD), progressive supranuclear palsy (PSP) and corticobasal degeneration (CBD) and, hence, CSF p-tau181 has also been proven useful in differential diagnosis of dementia.

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