Red blood cell membrane defects.

Achille Iolascon, Silverio Perrotta, Gordon W Stewart
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Abstract

We present an overview of the currently known molecular basis of red cell membrane disorders. A detailed discussion of the structure of the red cell membrane and the pathophysiology and clinical aspects of its disorders is reported. Generally speaking, hereditary spherocytosis (HS) results from a loss of erythrocyte surface area. The mutations of most cases of HS are located in the following genes: ANK1, SPTB, SLC4A1, EPB42 and SPTA1, which encode for ankyrin, spectrin beta-chain, the anion exchanger 1 (band 3), protein 4.2 and spectrin alpha-chain, respectively. Hereditary elliptocytosis (HE) reflects a diminished elasticity of the skeleton. Its aggravated form, hereditary pyropoikilocytosis (HPP), implies that the skeleton undergoes further destabilization. The mutations responsible for HE and HPP, lie in the SPTA1 and SPTB gene, and in the EPB41 gene encoding protein 4.1. Allele alpha LELY is a common polymorphic allele, which plays the role of an aggravating factor when it occurs in trans of an elliptocytogenic allele of the SPTA1 gene. Southeast Asian ovalocytosis derives from a change in band 3. The genetic disorders of membrane permeability to monovalent cations required a positional cloning approach. In this respect, channelopathies represent a new frontier in the field. Dehydrated hereditary stomatocytosis (DHS) was shown to belong to a pleiotropic syndrome: DHS + fetal edema + pseudohyperkalemia, which maps 16q23-24. Splenectomy is strictly contraindicated in DHS and another disease of the same class, overhydrated hereditary stomatocytosis, because it increases the risk of thromboembolic accidents.

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红细胞膜缺损。
我们提出了一个概述,目前已知的红细胞膜疾病的分子基础。详细讨论了红细胞膜的结构和病理生理和临床方面的疾病的报道。一般来说,遗传性球形红细胞增多症(HS)是由红细胞表面积的减少引起的。大多数HS病例的突变位于以下基因:ANK1、SPTB、SLC4A1、EPB42和SPTA1,它们分别编码锚蛋白、spectrin β链、阴离子交换器1(带3)、蛋白4.2和spectrin α链。遗传性椭圆细胞病(HE)反映了骨骼弹性的降低。其加重形式,遗传性焦嗜细胞增多症(HPP),意味着骨骼进一步不稳定。负责HE和HPP的突变位于SPTA1和SPTB基因,以及编码蛋白4.1的EPB41基因。等位基因α - LELY是一种常见的多态性等位基因,当它出现在SPTA1基因的椭圆型等位基因的反式中时,它起着加重因子的作用。东南亚卵母细胞增多症源于第3带的改变。膜对一价阳离子渗透性的遗传障碍需要定位克隆方法。在这方面,渠道病代表了该领域的一个新前沿。脱水遗传性口细胞增多症(DHS)属于一种多征综合征:DHS +胎儿水肿+假性高钾血症,定位于16q23-24。脾切除术是DHS和另一种同类疾病,过度水合遗传性口细胞增多症的严格禁忌症,因为它增加了血栓栓塞事故的风险。
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