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II型先天性红细胞生成异常性贫血:七个候选基因的排除

Congenital dyserythropoietic anemia type II: exclusion of seven candidate genes.

作者信息

Lanzara Carmela, Ficarella Romina, Totaro Angela, Chen Xin, Roberto Roberta, Perrotta Silverio, Lasalandra Carla, Gasparini Paolo, Iolascon Achille, Carella Massimo

机构信息

TIGEM (Telethon Institute of Genetics and Medicine), 80131 Naples, Italy.

出版信息

Blood Cells Mol Dis. 2003 Jan-Feb;30(1):22-9. doi: 10.1016/s1079-9796(03)00009-3.

Abstract

Congenital dyserythropoietic anemias (CDA) are genetic disorders characterized by anemia and ineffective erythropoiesis. Three main types of CDA have been distinguished: CDA I, CDAII and CDA III, whose loci have been already mapped. After the identification of the locus for CDA II, also known as HEMPAS (hereditary erythroblast multinuclearity with positive acidified serum test), on the long arm of chromosome 20 (20q11.2) we have analyzed by a mutational search seven candidate genes in a large series of CDA II patients. In particular, the following genes have been investigated: integrin beta 4 binding protein, ribophorin II, ubiquitin protein ligase ITCH, mannosil-oligosaccharide alpha-1,2-mannosidase like protein, erythrocyte protein band 4.1 like protein, zinc finger protein PLAGL2, and finally novel zinc finger protein. None of them resulted as the causative gene but several protein variants and DNA polymorphisms have been identified. These data exclude the role of the above mentioned genes in causing CDA II and add further information in the process of cloning the CDA II gene.

摘要

先天性红细胞生成异常性贫血(CDA)是一类以贫血和无效红细胞生成为特征的遗传性疾病。已区分出三种主要类型的CDA:CDA I、CDA II和CDA III,其基因座已被定位。在确定了位于20号染色体长臂(20q11.2)上的CDA II(也称为HEMPAS,即遗传性成红细胞多核症伴酸化血清试验阳性)的基因座后,我们通过突变搜索分析了一大系列CDA II患者中的七个候选基因。具体而言,研究了以下基因:整合素β4结合蛋白、核糖体结合蛋白II、泛素蛋白连接酶ITCH、甘露糖寡糖α-1,2-甘露糖苷酶样蛋白、红细胞蛋白带4.1样蛋白、锌指蛋白PLAGL2,以及最后一个新型锌指蛋白。它们均未被证实为致病基因,但已鉴定出几种蛋白质变体和DNA多态性。这些数据排除了上述基因在导致CDA II中的作用,并为克隆CDA II基因的过程增添了更多信息。

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