Liu Chun-Xiang, Ranganathan Sripriya, Robinson Susan, Strickland Dudley K
Center for Vascular and Inflammatory Disease and the Department of Surgery, University of Maryland School of Medicine, Baltimore, Maryland 21201, USA.
J Biol Chem. 2007 Mar 9;282(10):7504-11. doi: 10.1074/jbc.M608088200. Epub 2007 Jan 16.
The low density lipoprotein receptor related protein 1B (LRP1B) is a large endocytic receptor that was first identified as a candidate tumor suppressor gene. In the current investigation we demonstrate that LRP1B undergoes regulated intramembrane proteolysis in a gamma-secretase-dependent process. The released intracellular domain (ICD) then translocates to the nucleus via a nuclear localization signal that is present within this domain. ICD release first requires shedding of the LRP1B ectodomain, which appears to be catalyzed by a member of the metalloproteinase family. Employing site-directed mutagenesis studies, we identified lysine residues 4432 and 4435 and arginine 4442 as key amino acids important for ectodomain shedding of LRP1B. We also demonstrate that an LRP1B minireceptor as well as the ICD domain alone suppresses anchorage-independent growth of LRP1B-deficient neuroglioma cells (H4 cells). Interestingly, abrogating ectodomain shedding resulted in a loss of the ability of LRP1B minireceptors to suppress anchorage-independent growth. Together, these studies reveal that LRP1B has tumor suppression function that is mediated by proteolytic processing of the receptor resulting in ICD release.
低密度脂蛋白受体相关蛋白1B(LRP1B)是一种大型内吞受体,最初被鉴定为候选肿瘤抑制基因。在当前研究中,我们证明LRP1B在γ-分泌酶依赖性过程中经历调节性膜内蛋白水解。释放的细胞内结构域(ICD)然后通过该结构域内存在的核定位信号转运到细胞核。ICD释放首先需要LRP1B胞外结构域的脱落,这似乎由金属蛋白酶家族的一员催化。通过定点诱变研究,我们确定赖氨酸残基4432和4435以及精氨酸4442是LRP1B胞外结构域脱落的关键氨基酸。我们还证明,LRP1B微型受体以及单独的ICD结构域可抑制LRP1B缺陷型神经胶质瘤细胞(H4细胞)的非贴壁依赖性生长。有趣的是,消除胞外结构域脱落导致LRP1B微型受体失去抑制非贴壁依赖性生长的能力。总之,这些研究表明LRP1B具有肿瘤抑制功能,该功能由受体的蛋白水解加工介导,导致ICD释放。
