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ATP8A1 activity and phosphatidylserine transbilayer movement

机译:ATP8A1活性和磷脂酰丝氨酸跨双层运动

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Abstract: The asymmetric distribution of the amino-containing phospholipids, phosphatidyl-serine (PS) and phosphatidyl-ethanolamine (PE), across the two leaflets of red blood cell (RBC) membrane is essential to the function and survival of the cell. PS and PE are sequestered in the inner leaflet by an ATP-dependent transport activity of a membrane protein known as the RBC flippase that specifically moves amino-phospholipids from the outer to the inner leaflet. The enucleated RBC lacks the means to replace damaged enzymes and inactivation of the flippase can lead to the unwarranted exposure of PS on the cell surface. Loss in the ability to maintain phospholipid asymmetry is exacerbated in RBC disorders and PS-exposing RBCs present in the circulation play a significant role in the pathology of hemoglobinopathies. We identified the Atp8a1 protein, a member of the family of the P4-type ATPases, as a RBC flippase candidate. Atp8a1 is expressed in RBC precursors and is present in the membrane of mature red cells. The flippase activity of the protein was established in purified secretory vesicles of Saccharomyces cerevisiae. ATPase activity was stimulated by PS and PE. In addition, Atp8a1 can move PS molecules across the leaflets of the vesicle membrane in presence of ATP.
机译:摘要:含氨基的磷脂,磷脂酰丝氨酸(PS)和磷脂酰乙醇胺(PE)在红细胞(RBC)膜的两张小叶上的不对称分布对于细胞的功能和存活至关重要。 PS和PE通过称为RBC脂肪酶的膜蛋白的ATP依赖性转运活性而被螯合在内部小叶中,该膜蛋白特异性地将氨基磷脂从外部小叶移动到内部小叶。去核的红细胞缺乏替换受损酶的手段,而活菌的失活会导致PS不必要地暴露在细胞表面。在RBC疾病中,维持磷脂不对称性的能力加剧,循环中存在的PS暴露RBC在血红蛋白病的病理学中起重要作用。我们确定Atp8a1蛋白,P4型ATPases家族的成员,作为RBC flippase候选。 Atp8a1在RBC前体中表达,并存在于成熟红细胞的膜中。该蛋白质的flippase活性在酿酒酵母的纯化分泌小泡中建立。 PS和PE刺激ATPase活性。此外,Atp8a1可以在ATP存在的情况下使PS分子穿过囊泡小叶移动。

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