Farashi Samaneh, Vakili Shadi, Garous Negin F, Ashki Mehri, Imanian Hashem, Azarkeivan Azita, Najmabadi Hossein
a Genetics Research Centre, University of Social Welfare & Rehabilitation Sciences , Tehran , Iran .
b Kariminejad-Najmabadi Pathology & Genetics Centre , Tehran , Iran.
Hemoglobin. 2015;39(6):398-402. doi: 10.3109/03630269.2015.1075890. Epub 2015 Sep 2.
In the present study, a total of 11 individuals with hypochromic microcytic anemia who did not reveal the most common α-thalassemia (α-thal) deletions or mutations, were subjected to more investigations by DNA sequencing of the α-globin genes. Seven novel nondeletional α-thal mutations localized on the α2-globin gene in the heterozygous state were identified. These mutations either corrupted regulatory splice sites and consequently affected RNA processing or created unstable hemoglobin (Hb) variants. The mutations described here produced globin gene variants that lead to amino acid changes in critical regions of the globin chain. The clinical presentation of most patients was a persistent mild microcytic anemia similar to an α(+)-thal. In the last decade, numerous α-globin mutations have been observed leading to an α-thal phenotype and these studies have been considered to be important as discussed here.
在本研究中,对11例未发现最常见的α地中海贫血(α-地贫)缺失或突变的低色素小细胞性贫血患者,通过α珠蛋白基因的DNA测序进行了更多研究。鉴定出7种以杂合状态定位于α2珠蛋白基因上的新型非缺失性α-地贫突变。这些突变要么破坏调控剪接位点,从而影响RNA加工,要么产生不稳定的血红蛋白(Hb)变体。此处描述的突变产生了导致珠蛋白链关键区域氨基酸变化的珠蛋白基因变体。大多数患者的临床表现为持续性轻度小细胞性贫血,类似于α(+)-地贫。在过去十年中,已观察到许多导致α-地贫表型的α珠蛋白突变,如本文所讨论的,这些研究被认为很重要。
