首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >An extracellular region of the erythropoietin receptor of the subterranean blind mole rat Spalax enhances receptor maturation
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An extracellular region of the erythropoietin receptor of the subterranean blind mole rat Spalax enhances receptor maturation

机译:地下黑痣大鼠Spalax促红细胞生成素受体的胞外区域增强受体成熟

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Erythropoietic functions of erythropoietin (EPO) are mediated by its receptor (EPO-R), which is present on the cell surface of ery-throid progenitors and induced by hypoxia. We focused on EPO-R from Spalax galili (sEPO-R), one of the four Israeli species of the subterranean blind mole rat, Spalax ehrenbergi superspecies, as a special natural animal model of high tolerance to hypoxia. Led by the intriguing observation that most of the mouse EPO-R (mEPO-R) is retained in the endoplasmic reticulum (ER), we hypothesized that sEPO-R is expressed at higher levels on the cell surface, thus maximizing the response to elevated EPO, which has been reported in this species. Indeed, we found increased cell-surface levels of sEPO-R as compared with mEPO-R by using flow cytom-etry analysis of BOSC cells transiently expressing HA-tagged EPO-Rs (full length or truncated). We then postulated that unique extracellular sEPO-R sequence features contribute to its processing and cell-surface expression. To map these domains of the sEPO-R that augment receptor maturation, we generated EPO-R derivatives in which parts of the extracellular region of mEPO-R were replaced with the corresponding fragments of sEPO-R. We found that an extracellular portion of sEPO-R, harboring the N-glycosylation site, conferred enhanced maturation and increased transport to the cell surface of the respective chimeric receptor. Taken together, we demonstrate higher surface expression of sEPO-R, attributed at least in part to increased ER exit, mediated by an extracellular region of this receptor. We speculate that these sEPO-R sequence features play a role in the adaptation of Spalax to extreme hypoxia.
机译:促红细胞生成素(EPO)的促红细胞功能由其受体(EPO-R)介导,该受体存在于红系祖细胞的细胞表面并由缺氧诱导。我们重点研究了Spalax galili(sEPO-R)的EPO-R,它是地下盲mole鼠的四个以色列物种之一,Spalax ehrenbergi超级物种,是对缺氧具有高度耐受性的特殊天然动物模型。有趣的观察是,大多数小鼠EPO-R(mEPO-R)保留在内质网(ER)中,我们假设sEPO-R在细胞表面以较高水平表达,从而最大化了对EPO-R的反应。 EPO,已在该物种中报道。确实,我们通过对瞬时表达HA标签的EPO-R(全长或截短)的BOSC细胞进行流式细胞术分析,发现与mEPO-R相比,sEPO-R的细胞表面水平增加。然后,我们推测独特的细胞外sEPO-R序列特征有助于其加工和细胞表面表达。为了绘制增强受体成熟的sEPO-R的这些结构域,我们生成了ePO-R衍生物,其中mEPO-R的胞外区部分被sEPO-R的相应片段取代。我们发现,sEPO-R的一个胞外部分,具有N-糖基化位点,具有增强的成熟度,并增加了向各个嵌合受体细胞表面的转运。两者合计,我们证明更高的表面表达的sEPO-R,至少部分归因于该受体的胞外区域介导的ER出口增加。我们推测这些sEPO-R序列特征在Spalax对极端缺氧的适应中起作用。

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