Department of Genetic Research, Institute for Research and Medical Consultation, Imam Abdulrahman Bin Faisal University, Dammam 31441, Saudi Arabia.
Department of Clinical Pharmacy Research, Institute for Research and Medical Consultation, Imam Abdulrahman Bin Faisal University, Dammam 31441, Saudi Arabia.
Mol Med Rep. 2018 Jan;17(1):1879-1884. doi: 10.3892/mmr.2017.8033. Epub 2017 Nov 13.
The regions of Al‑Qatif and Al‑Ahssa in the Eastern Province of Saudi Arabia are known for their high prevalence of hemoglobinopathies, including β‑thalassemia and sickle cell anemia. Previously, the α‑gene deletion has been demonstrated as highly prevalent among populations residing in these two regions. The present study was conducted in order to investigate the implications of the α‑globin gene deletion on fetal hemoglobin (HbF) and hemoglobin α2 (HbA2) concentrations in patients with transfusion‑dependent β‑thalassemia. A total of 166 Saudi patients with transfusion‑dependent β‑thalassemia and 337 healthy Saudi patients were included in the study. The ‑α3.7, ‑α4.2, -‑FIL, -‑SEA, -‑MED and -‑(20.5) gene deletions were identified using multiplex α‑globin deletion polymerase chain reaction. The present study revealed that the ‑α3.7 gene deletion is the most prevalent (43.5%) in the Saudi populations that were analyzed and is characterized by the deletion of 3,804 base pairs. Numerous genotypes, namely ‑3.7α2/α1α2, ‑3.7α2/α1α12, ‑3.7α2/‑3.7α2, ‑3.7α2HphI/α1α2HphI, ‑3.7α2/α1‑4.2, ‑3.7α2/α1polyA‑1α2, ‑3.7α12/α1α12, ‑‑FIL/‑3.7α2 and ‑3.7α2/‑3.7α2Hb Villiers le Bel were also identified in the investigated population. Furthermore, a gradual increase in the concentration of HbF and HbA2 in patients with β‑thalassemia and the number of α‑gene deletions was demonstrated; whereas in healthy patients the level of HbA2 was demonstrated to decrease as the number of α‑gene deletions increased. Therefore, it can be concluded that the high HbF concentration in the present study is predominantly associated with other mutations associated with β‑thalassemia rather than α‑globin deletions. Furthermore, the results of the present study also revealed novel α‑gene deletion genotypes prevalent in the population studied, namely α1α2/α1α2HphI, α1α2HphI/α1α2HphI, α1α2/α1α2Hb Handsworth, ‑3.7α2HphI/α1α2HphI, ‑3.7α2/‑3.7α2Hb Villiers le Bel and ‑-MED/α1α2HphI.
沙特阿拉伯东部省的盖提夫和阿赫萨地区以高发的血红蛋白病而闻名,包括β-地中海贫血和镰状细胞贫血。此前,研究已经证明α-基因缺失在居住在这两个地区的人群中非常普遍。本研究旨在探讨α-珠蛋白基因缺失对依赖输血的β-地中海贫血患者胎儿血红蛋白(HbF)和血红蛋白α2(HbA2)浓度的影响。研究共纳入 166 例依赖输血的β-地中海贫血沙特患者和 337 例健康沙特患者。采用多重α-珠蛋白缺失聚合酶链反应鉴定-α3.7、-α4.2、-FIL、-SEA、-MED 和-(20.5)基因缺失。本研究显示,-α3.7 基因缺失是分析的沙特人群中最常见的(43.5%),其特征是缺失 3804 个碱基对。许多基因型,如-α3.7α2/α1α2、-α3.7α2/α1α12、-α3.7α2/ -α3.7α2、-α3.7α2HphI/α1α2HphI、-α3.7α2/α1-4.2、-α3.7α2/α1polyA-1α2、-α3.7α12/α1α12、-FIL/ -α3.7α2 和 -α3.7α2/ -α3.7α2Hb Villiers le Bel 也在研究人群中被鉴定出来。此外,还证明了β-地中海贫血患者的 HbF 和 HbA2 浓度以及α-基因缺失数量的逐渐增加;而在健康患者中,随着α-基因缺失数量的增加,HbA2 水平降低。因此,可以得出结论,本研究中高 HbF 浓度主要与β-地中海贫血相关的其他突变有关,而不是与α-珠蛋白缺失有关。此外,本研究的结果还揭示了在研究人群中流行的新型α-基因缺失基因型,即α1α2/α1α2HphI、α1α2HphI/α1α2HphI、α1α2/α1α2Hb Handsworth、-α3.7α2HphI/α1α2HphI、-α3.7α2/ -α3.7α2Hb Villiers le Bel 和 -MED/α1α2HphI。
