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Phospho-Insulin Receptor Beta (Tyr1361) Rabbit pAb, PE-Cy5.5 conjugated
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原料试剂 研发实验室
价格
¥2980.00
品牌 Bioss博奥森生物
地区 中国,北京,北京市
货号 bs-20191R-PE-Cy5.5
产地 国产
选择规格
100ul
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Bioss博奥森生物
北京博奥森生物技术有限公司
北京
营业执照已审核
博奥森:专注科研,以优质抗体引领未来 博奥森生物,自2001年诞生以来,始终坚守在生命科学前沿,为全球科研人员提供卓越品质的免疫学试剂产品与服务。我们拥有资深的科学家团队、先进的抗体发现、验证与生产平台,始终坚持“自主研发、原始创新”的理念,确保每一款产品都能达到国际标准,持续提供“4R” 品质科研工具【Repeatable(可重复)、Replicable(可复制)、Reproducible(可再现)和Reliable(可靠的)】。
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产品规格 图文详情 技术文档
产品规格
品牌名称
Bioss博奥森生物
货号
bs-20191R-PE-Cy5.5
国产/进口
国产
规格
100ul
储存条件
Shipped at 4℃. Store at -20°C for one year. Avoid repeated freeze/thaw cycles.
使用范围
Flow-Cyt
货源
新品
图文详情
Application:Flow-Cyt
Reactivity: Human (predicted: Mouse,Rat,Rabbit,Sheep,Cow,Dog,Horse)
The human insulin receptor is a heterotetrameric membrane glycoprotein consisting of disulfide linked subunits in a beta-alpha-alpha-beta configuration. The beta subunit (95 kDa) possesses a single transmembrane domain, whereas the alpha subunit (135 kDa) is completely extracellular. The insulin receptor exhibits receptor tyrosine kinase (RTK) activity. RTKs are single pass transmembrane receptors that possess intrinsic cytoplasmic enzymatic activity, catalyzing the transfer of the gamma phosphate of ATP to tyrosine residues in protein substrates. RTKs are essential components of signal transduction pathways that affect cell proliferation, differentiation, migration and metabolism.
Included in this large protein family are the insulin receptor and the receptors for growth factors such as epidermal growth factor, fibroblast growth factor and vascular endothelial growth factor. Receptor activation occurs through ligand binding, which facilitates receptor dimerization and autophosphorylation of specific tyrosine residues in the cytoplasmic portion. The interaction of insulin with the alpha subunit of the insulin receptor activates the protein tyrosine kinase of the beta subunit, which then undergoes an autophosphorylation that increases its tyrosine kinase activity. Three adapter proteins, IRS1, IRS2 and Shc, become phosphorylated on tyrosine residues following insulin receptor activation. These three phosphorylated proteins then interact with SH2 domain containing signaling proteins.
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