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首页> 外文期刊>Frontiers in Physiology >Membrane Rearrangements in the Maturation of Circulating Human Reticulocytes
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Membrane Rearrangements in the Maturation of Circulating Human Reticulocytes

机译:循环人网状细胞的成熟中的膜重排

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Red blood cells (RBCs) begin their circulatory life as reticulocytes (Retics) after their egress from the bone marrow where, as R1 Retics, they undergo significant rearrangements in their membrane and intracellular components, via autophagic, proteolytic, and vesicle-based mechanisms. Circulating, R2 Retics must complete this maturational process, which involves additional loss of significant amounts of membrane and selected membrane proteins. Little is known about the mechanism(s) at the basis of this terminal differentiation in the circulation, which culminates with the production of a stable biconcave discocyte. The membrane of R1 Retics undergoes a selective remodeling through the release of exosomes that are enriched in transferrin receptor and membrane raft proteins and lipids, but are devoid of Band 3, glycophorin A, and membrane skeletal proteins. We wondered whether a similar selective remodeling occurred also in the maturation of R2 Retics. Peripheral blood R2 Retics, isolated by an immunomagnetic method, were compared with mature circulating RBCs from the same donor and their membrane protein and lipid content was analyzed. Results show that both Band 3 and spectrin decrease from R2 Retics to RBCs on a “per cell” basis. Looking at membrane proteins that are considered as markers of membrane rafts, flotillin-2 appears to decrease in a disproportionate manner with respect to Band 3. Stomatin also decreases but in a more proportionate manner with respect to Band 3, hinting at a heterogeneous nature of membrane rafts. High resolution lipidomics analysis, on the contrary, revealed that those lipids that are typically representative of the membrane raft phase, sphingomyelin and cholesterol, are enriched in mature RBCs with respct to Retics, relative to total cell lipids, strongly arguing in favor of the selective retention of at least certain subclasses of membrane rafts in RBCs as they mature from Retics. Our hypothesis that rafts serve as additional anchoring sites for the lipid bilayer to the underlying membrane-skeleton is corroborated by the present results. It is becoming ever more clear that a proper lipid composition of the reticulocyte is necessary for the production of a normal mature RBC.
机译:红细胞(RBCS)在从骨髓出口后开始其循环寿命作为网状细胞(视网膜),在骨髓中作为R1检测器,它们通过自噬,蛋白水解和基于囊泡的机制在其膜和细胞内部件中进行显着重排。循环,R2 reciCs必须完成这种成熟过程,这涉及额外的大量膜和所选膜蛋白的额外损失。在循环中的这种末端分化的基础上,对该机制众所周知,其促使稳定的双凸晶状体的产生。 R1 retics的膜通过释放在转铁蛋白受体和膜筏蛋白和脂质中的外来释放的选择性重塑,但是缺乏带3,糖蛋白A和膜骨架蛋白。我们想知道是否也发生了类似的选择性重塑在R2的成熟中。通过免疫磁性方法分离的外周血R2 reciCs与来自相同供体的成熟循环RBC和它们的膜蛋白和脂质含量进行比较。结果表明,频段3和光谱从R2检素到RBC的基础上的RBC依据。看着被认为是膜筏的标记的膜蛋白质,Flotillin-2似乎以不成比例的方式减少,相对于带3.穴位也降低但以更比例的方式相对于带3,暗示在异质性质上暗示膜筏。相反,高分辨率脂多元族分析显示,这些脂质通常代表膜筏相,鞘氨酰胺和胆固醇,富含成熟的RBC,相对于总细胞脂质,强烈争论有利于选择性在RBCS中保留至少某些膜筏的亚类,因为它们从重视中成熟。我们假设筏作为脂质双层的额外锚定部位,通过本结果得到证实。众所周知,括号的适当脂质组合物是生产正常成熟RBC的必要条件。

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