不同兔肝细胞中的低密度脂蛋白受体
Low-density-lipoprotein receptors in different rabbit liver cells.
作者信息
Nenseter M S, Myklebost O, Blomhoff R, Drevon C A, Nilsson A, Norum K R, Berg T
机构信息
Institute for Nutrition Research, University of Oslo, Norway.
出版信息
Biochem J. 1989 Jul 15;261(2):587-93. doi: 10.1042/bj2610587.
Receptor-dependent uptake mechanisms for low-density lipoprotein (LDL) were studied in rabbit liver parenchymal and non-parenchymal cells. Hybridization studies with a cDNA probe revealed that mRNA for the apo (apolipoprotein) B,E receptor was present in endothelial and Kupffer cells as well as in parenchymal cells. By ligand-blotting experiments we showed that apo B,E-receptor protein was present in both parenchymal and non-parenchymal cells. Studies of binding of homologous LDL in cultured rabbit parenchymal cells suggested that about 63% of the specific LDL binding was mediated via the apo B,E receptor. Approx. 47% of the specific LDL binding was dependent on Ca2+, suggesting that specific Ca2+-dependent as well as Ca2+-independent LDL-binding sites exist in liver parenchymal cells. Methylated LDL bound to the parenchymal cells in a saturable manner. Taken together, our results showed that apo B,E receptors are present in rabbit liver endothelial and Kupffer cells as well as in the parenchymal cells, and that an additional saturable binding activity for LDL may exist on rabbit liver parenchymal cells. This binding activity was not inhibited by EGTA or reductive methylation of lysine residues in apo B. LDL degradation in parenchymal cells was mainly mediated via the apo B,E receptor.
在兔肝实质细胞和非实质细胞中研究了低密度脂蛋白(LDL)的受体依赖性摄取机制。用cDNA探针进行的杂交研究表明,载脂蛋白(apo)B、E受体的mRNA存在于内皮细胞、库普弗细胞以及实质细胞中。通过配体印迹实验,我们表明apo B、E受体蛋白存在于实质细胞和非实质细胞中。对培养的兔实质细胞中同源LDL结合的研究表明,约63%的特异性LDL结合是通过apo B、E受体介导的。约47%的特异性LDL结合依赖于Ca2+,这表明肝实质细胞中存在特异性的Ca2+依赖性和Ca2+非依赖性LDL结合位点。甲基化的LDL以饱和方式与实质细胞结合。综上所述,我们的结果表明,apo B、E受体存在于兔肝内皮细胞、库普弗细胞以及实质细胞中,并且兔肝实质细胞上可能存在另外一种对LDL的可饱和结合活性。这种结合活性不受EGTA或apo B中赖氨酸残基的还原甲基化的抑制。实质细胞中LDL的降解主要通过apo B、E受体介导。
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