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化工儀器網(wǎng)>產(chǎn)品展廳>試劑標(biāo)物>生化試劑>抗體/抗原>S0B3156 Tau (phospho T181) Mouse mAb (SDT-2...

S0B3156 Tau (phospho T181) Mouse mAb (SDT-200-5)

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  • 公司名稱 杭州斯達(dá)特生物科技有限公司
  • 品牌 Starter/斯達(dá)特
  • 型號(hào) S0B3156
  • 產(chǎn)地 浙江 杭州
  • 廠商性質(zhì) 生產(chǎn)廠家
  • 更新時(shí)間 2025/8/6 13:08:44
  • 訪問次數(shù) 53

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杭州斯達(dá)特是一家集研發(fā)、生產(chǎn)、銷售與技術(shù)服務(wù)為一體的高科技生物公司,志在為全球生物醫(yī)學(xué)研究、體外診斷企業(yè)、生物制藥企業(yè)提供優(yōu)質(zhì)的抗體、蛋白、試劑盒和定制服務(wù),包括科研抗體、CDx和IVD抗原和抗體原料、一步法ELISA試劑盒、鼠兔通用二抗試劑盒以及其他用途的免疫試劑整體解決方案。


公司核心團(tuán)隊(duì)深耕抗體研發(fā)十五年,具有成功開發(fā)數(shù)千種精準(zhǔn)醫(yī)學(xué)抗體、科研抗體的豐富經(jīng)驗(yàn)。公司建立了多物種單B細(xì)胞抗體開發(fā)平臺(tái)(兔單抗,鼠類單抗等)、傳統(tǒng)鼠單抗、重組蛋白表達(dá)平臺(tái)及完善的抗體應(yīng)用驗(yàn)證和檢測體系(包括免疫層析,酶聯(lián)免疫,流式分析,免疫組化,免疫印跡,免疫熒光,免疫沉淀等)。已正式通過歐盟98/79/EC認(rèn)證、ISO9001認(rèn)證和ISO13485認(rèn)證。


公司以加速人類、疾病診斷、為人類和動(dòng)物健康保駕護(hù)航為使命,以扎實(shí)的科學(xué)技術(shù)為基礎(chǔ),秉承向正向善向上的價(jià)值觀,以行業(yè)客戶需求為導(dǎo)向,愿與全球同仁精誠合作,共啟健康新篇章。


斯達(dá)特,專注于抗體研發(fā)和制造,您的最佳抗體優(yōu)選伙伴。

抗體,蛋白,試劑盒

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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