Bovenschen Niels, Mertens Koen, Hu Lihui, Havekes Louis M, van Vlijmen Bart J M
Department of Plasma Proteins, Sanquin Research at CLB, Plesmanlaan 125, 1066 CX Amsterdam, The Netherlands.
Blood. 2005 Aug 1;106(3):906-12. doi: 10.1182/blood-2004-11-4230. Epub 2005 Apr 19.
Low-density lipoprotein (LDL) receptor (LDLR) and LDLR-related protein (LRP) are members of the LDLR family of endocytic receptors. LRP recognizes a wide spectrum of structurally and functionally unrelated ligands, including coagulation factor VIII (FVIII). In contrast, the ligand specificity of LDLR is restricted to apolipoproteins E and B-100. Ligand binding to the LDLR family is inhibited by receptor-associated protein (RAP). We have previously reported that, apart from LRP, other RAP-sensitive mechanisms contribute to the regulation of FVIII in vivo. In the present study, we showed that the extracellular ligand-binding domain of LDLR interacts with FVIII in vitro and that binding was inhibited by RAP. The physiologic relevance of the FVIII-LDLR interaction was addressed using mouse models of LDLR or hepatic LRP deficiency. In the absence of hepatic LRP, LDLR played a dominant role in the regulation and clearance of FVIII in vivo. Furthermore, FVIII clearance was accelerated after adenovirus-mediated gene transfer of LDLR. The role of LDLR in FVIII catabolism was not secondary to increased plasma lipoproteins or to changes in lipoprotein profiles. We propose that LDLR acts in concert with LRP in regulating plasma levels of FVIII in vivo. This represents a previously unrecognized link between LDLR and hemostasis.
低密度脂蛋白(LDL)受体(LDLR)和LDLR相关蛋白(LRP)是内吞受体LDLR家族的成员。LRP能识别多种结构和功能上不相关的配体,包括凝血因子VIII(FVIII)。相比之下,LDLR的配体特异性仅限于载脂蛋白E和B-100。配体与LDLR家族的结合受受体相关蛋白(RAP)抑制。我们之前报道过,除LRP外,其他RAP敏感机制也在体内FVIII的调节中起作用。在本研究中,我们发现LDLR的细胞外配体结合结构域在体外与FVIII相互作用,且这种结合受RAP抑制。我们使用LDLR或肝脏LRP缺陷的小鼠模型研究了FVIII-LDLR相互作用的生理相关性。在缺乏肝脏LRP的情况下,LDLR在体内FVIII的调节和清除中起主导作用。此外,腺病毒介导的LDLR基因转移后,FVIII的清除加快。LDLR在FVIII分解代谢中的作用并非继发于血浆脂蛋白增加或脂蛋白谱改变。我们提出,LDLR与LRP协同作用以调节体内FVIII的血浆水平。这代表了LDLR与止血之间以前未被认识到的联系。
