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Monoclonal antibodies that bind to the Ly6 domain of GPIHBP1 abolish the binding of LPL

机译:与GPIHBP1的Ly6结构域结合的单克隆抗体消除了LPL的结合

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摘要

GPIHBP1, an endothelial cell protein, binds LPL in the interstitial spaces and shuttles it to its site of action inside blood vessels. For years, studies of human GPIHBP1 have been hampered by an absence of useful antibodies. We reasoned that monoclonal antibodies (mAbs) against human GPIHBP1 would be useful for 1) defining the functional relevance of GPIHBP1’s Ly6 and acidic domains to the binding of LPL; 2) ascertaining whether human GPIHBP1 is expressed exclusively in capillary endothelial cells; and 3) testing whether GPIHBP1 is detectable in human plasma. Here, we report the development of a panel of human GPIHBP1-specific mAbs. Two mAbs against GPIHBP1’s Ly6 domain, RE3 and RG3, abolished LPL binding, whereas an antibody against the acidic domain, RF4, did not. Also, mAbs RE3 and RG3 bound with reduced affinity to a mutant GPIHBP1 containing an Ly6 domain mutation (W109S) that abolishes LPL binding. Immunohistochemistry studies with the GPIHBP1 mAbs revealed that human GPIHBP1 is expressed only in capillary endothelial cells. Finally, we created an ELISA that detects GPIHBP1 in human plasma. That ELISA should make it possible for clinical lipidologists to determine whether plasma GPIHBP1 levels are a useful biomarker of metabolic or vascular disease
机译:GPIHBP1是一种内皮细胞蛋白,它在组织间隙中结合LPL,并将其穿梭到血管内的作用部位。多年来,由于缺乏有用的抗体而阻碍了人类GPIHBP1的研究。我们认为针对人GPIHBP1的单克隆抗体(mAb)可用于1)定义GPIHBP1的Ly6和酸性域与LPL结合的功能相关性; 2)确定人GPIHBP1是否仅在毛细血管内皮细胞中表达; 3)测试在人血浆中是否可检测到GPIHBP1。在这里,我们报告人类GPIHBP1特异性单克隆抗体的发展。针对GPIHBP1的Ly6结构域的两个单克隆抗体RE3和RG3消除了LPL结合,而针对酸性结构域的抗体RF4则没有。而且,mAbs RE3和RG3以降低的亲和力与突变体GPIHBP1结合,该突变体GPIHBP1含有消除LPL结合的Ly6域突变(W109S)。使用GPIHBP1 mAb进行的免疫组织化学研究表明,人GPIHBP1仅在毛细血管内皮细胞中表达。最后,我们创建了一种ELISA,可以检测人血浆中的GPIHBP1。 ELISA可以使临床脂质学家确定血浆GPIHBP1水平是否是代谢或血管疾病的有用生物标志物

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