首页> 外文期刊>Blood: The Journal of the American Society of Hematology >The tetraspanin CD63 is involved in granule targeting of neutrophil elastase.
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The tetraspanin CD63 is involved in granule targeting of neutrophil elastase.

机译:四跨膜蛋白CD63参与嗜中性粒细胞弹性蛋白酶的颗粒靶向。

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摘要

Targeting mechanisms of neutrophil elastase (NE) and other luminal proteins stored in myeloperoxidase (MPO)-positive secretory lysosomes/primary granules of neutrophils are unknown. These granules contain an integral membrane protein, CD63, with an adaptor protein-3-dependent granule delivery system. Therefore, we hypothesized that CD63 cooperates in granule delivery of the precursor of NE (proNE). Supporting this hypothesis, an association was demonstrated between CD63 and proNE upon coexpression in COS cells. This also involved augmented cellular retention of proNE requiring intact large extracellular loop of CD63. Furthermore, depletion of CD63 in promyelocytic HL-60 cells with RNA interference or a CD63 mutant caused reduction of cellular NE. However, the proNE steady-state level was similar to wild type in CD63-depleted clones, making it feasible to examine possible effects of CD63 on NE trafficking. Thus, depletion of CD63 led to reduced processing of proNE into mature NE and reduced constitutivesecretion. Furthermore, CD63-depleted cells showed a lack of morphologically normal granules, but contained MPO-positive cytoplasmic vacuoles with a lack of proNE and NE. Collectively, our data suggest that granule proteins may cooperate in targeting; CD63 can be involved in ER or Golgi export, cellular retention, and granule targeting of proNE before storage as mature NE.
机译:嗜中性粒细胞弹性蛋白酶(NE)和其他管腔蛋白存储在髓过氧化物酶(MPO)阳性分泌性溶酶体/嗜中性粒细胞初级颗粒中的靶向机制尚不清楚。这些颗粒包含完整的膜蛋白CD63,以及依赖于衔接蛋白3的颗粒递送系统。因此,我们假设CD63协同NE前体(proNE)的颗粒输送。支持该假设的事实证明,在COS细胞中共表达时,CD63和proNE之间存在关联。这还涉及需要完整的CD63大细胞外环的proNE的增强的细胞保留。此外,在具有RNA干扰的早幼粒细胞HL-60细胞中CD63的消耗或CD63突变体引起细胞NE的减少。但是,proNE稳态水平与CD63缺失克隆中的野生型相似,这使得检查CD63对NE转运的可能影响变得可行。因此,CD63的消耗导致proNE加工成成熟NE的过程减少,并且组成性分泌减少。此外,CD63耗尽的细胞显示缺乏形态正常的颗粒,但含有MPO阳性的细胞质液泡,而proNE和NE则缺乏。总的来说,我们的数据表明颗粒蛋白可能在靶向中协同作用。在存储为成熟NE之前,CD63可能参与ER或高尔基体的输出,细胞滞留以及proNE的颗粒靶向。

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