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Phospholipase D2 Localizes to the Plasma Membrane and Regulates Angiotensin II Receptor Endocytosis

机译:磷脂酶D2定位于血浆膜并调节血管紧张素II受体的内吞作用

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摘要

Phospholipase D (PLD) is a key facilitator of multiple types of membrane vesicle trafficking events. Two PLD isoforms, PLD1 and PLD2, exist in mammals. Initial studies based on overexpression studies suggested that in resting cells, human PLD1 localized primarily to the Golgi and perinuclear vesicles in multiple cell types. In contrast, overexpressed mouse PLD2 was observed to localize primarily to the plasma membrane, although internalization on membrane vesicles was observed subsequent to serum stimulation. A recent report has suggested that the assignment of PLD2 to the plasma membrane is in error, because the endogenous isoform in rat secretory cells was imaged and found to be present primarily in the Golgi apparatus. We have reexamined this issue by using a monoclonal antibody specific for mouse PLD2, and find, as reported initially using overexpression studies, that endogenous mouse PLD2 is detected most readily at the plasma membrane in multiple cell types. In addition, we report that mouse, rat, and human PLD2 when overexpressed all similarly localize to the plasma membrane in cell lines from all three species. Finally, studies conducted using overexpression of wild-type active or dominant-negative isoforms of PLD2 and RNA interference-mediated targeting of PLD2 suggest that PLD2 functions at the plasma membrane to facilitate endocytosis of the angiotensin II type 1 receptor.
机译:磷脂酶D(PLD)是多种类型的膜小泡运输事件的关键促进者。哺乳动物中存在两种PLD亚型,即PLD1和PLD2。基于过表达研究的初步研究表明,在静止细胞中,人类PLD1主要位于多种细胞类型中的高尔基体和核周囊泡中。相反,观察到过表达的小鼠PLD2主要定位于质膜,尽管在血清刺激后观察到膜囊泡的内在化。最近的报告表明,将PLD2分配至质膜是错误的,因为对大鼠分泌细胞中的内源同工型进行了成像并发现其主要存在于高尔基体中。我们已经通过使用对小鼠PLD2特异的单克隆抗体重新检查了这个问题,并发现,如最初使用过表达研究所报道的那样,在多种细胞类型中最容易在质膜上检测到内源性小鼠PLD2。此外,我们报告说,小鼠,大鼠和人PLD2过度表达时,所有三种物种的细胞系都相似地定位于质膜。最后,使用野生型PLD2活性或显性阴性同种型的过表达和RNA干扰介导的PLD2靶向进行的研究表明,PLD2在质膜起作用,促进血管紧张素II 1型受体的内吞。

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