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一项关于α血红蛋白稳定蛋白(AHSP)表达变异性的双胞胎遗传力研究。

A twins heritability study on alpha hemoglobin stabilizing protein (AHSP) expression variability.

作者信息

Lai Mei I, Garner Chad, Jiang Jie, Silver Nicholas, Best Steve, Menzel Stephan, Thein Swee L

机构信息

Department of Pathology, Universiti Putra Malaysia, Malaysia.

出版信息

Twin Res Hum Genet. 2010 Dec;13(6):567-72. doi: 10.1375/twin.13.6.567.

Abstract

Cytotoxic precipitation of free α-globin monomers and its production of reactive oxygen species cause red cell membrane damage that leads to anemia and eventually ineffective erythropoiesis in β-thalassemia. Alpha hemoglobin stabilizing protein (AHSP) was found to bind only to free α-globin monomers creating a stable and inert complex which remains soluble in the cytoplasm thus preventing harmful precipitations. Alpha hemoglobin stabilizing protein was shown to bind nascent α-globin monomers with transient strength before transferring α-globin to β-globin to form hemoglobin tetramer. A classical twin study would be beneficial to investigate the role of genetics and environment in the variation of alpha hemoglobin stabilizing protein expression as this knowledge will enable us to determine further investigations with regards to therapeutic interventions if alpha hemoglobin stabilizing protein is to be a therapeutic agent for β-thalassemia. This study investigates the heritability influence of alpha hemoglobin stabilizing protein expression and factors that may contribute to this. Results indicated that a major proportion of alpha hemoglobin stabilizing protein expression was influenced by genetic heritability (46%) with cis-acting factors accounting for 19% and trans-acting factors at 27%.

摘要

游离α-珠蛋白单体的细胞毒性沉淀及其产生活性氧会导致红细胞膜损伤,进而引发贫血,并最终导致β地中海贫血中的无效红细胞生成。人们发现α血红蛋白稳定蛋白(AHSP)仅与游离的α-珠蛋白单体结合,形成一种稳定且无活性的复合物,该复合物仍可溶于细胞质中,从而防止有害沉淀的形成。研究表明,α血红蛋白稳定蛋白在将α-珠蛋白转移至β-珠蛋白以形成血红蛋白四聚体之前,会以短暂的强度结合新生的α-珠蛋白单体。一项经典的双胞胎研究将有助于调查遗传和环境在α血红蛋白稳定蛋白表达变异中的作用,因为如果α血红蛋白稳定蛋白要成为β地中海贫血的治疗药物,这些知识将使我们能够确定关于治疗干预的进一步研究方向。本研究调查了α血红蛋白稳定蛋白表达的遗传力影响以及可能导致这种情况的因素。结果表明,α血红蛋白稳定蛋白表达的很大一部分受遗传遗传力影响(46%),其中顺式作用因子占19%,反式作用因子占27%。

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