Vizzi Esmeralda, Bastidas Gilberto, Hidalgo Mariana, Colman Laura, Pérez Hilda A
Laboratorio de Biología de Virus, Centro de Microbiología y Biología Celular, Instituto Venezolano de Investigaciones Científicas, Apdo 21827, Caracas, 1020-A, Venezuela.
Laboratorio de Inmunoparasitología, Centro de Microbiología y Biología Celular, Instituto Venezolano de Investigaciones Científicas, Apdo 21827, Caracas, 1020-A, Venezuela.
Malar J. 2016 Jan 11;15:19. doi: 10.1186/s12936-015-1069-5.
Glucose-6-phosphate dehydrogenase (G6PD) deficiency causes acute haemolytic anaemia triggered by oxidative drugs such as primaquine (PQ), used for Plasmodium vivax malaria radical cure. However, in many endemic areas of vivax malaria, patients are treated with PQ without any evaluation of their G6PD status.
G6PD deficiency and its genetic heterogeneity were evaluated in northeastern and southeastern areas from Venezuela, Cajigal (Sucre state) and Sifontes (Bolívar state) municipalities, respectively. Blood samples from 664 randomly recruited unrelated individuals were screened for G6PD activity by a quantitative method. Mutation analysis for exons 4-8 of G6PD gen was performed on DNA isolated from G6PD-deficient (G6PDd) subjects through PCR-RFLP and direct DNA sequencing.
Quantitative biochemical characterization revealed that overall 24 (3.6%) subjects were G6PDd (average G6PD enzyme activity 4.5 ± 1.2 U/g Hb, moderately deficient, class III), while DNA analysis showed one or two mutated alleles in 19 of them (79.2%). The G6PD A-(202A/376G) variant was the only detected in 17 (70.8%) individuals, 13 of them hemizygous males and four heterozygous females. Two males carried only the 376A → G mutation. No other mutation was found in the analysed exons.
The G6PDd prevalence was as low as that one shown by nearby countries. This study contributes to the knowledge of the genetic background of Venezuelan population, especially of those living in malaria-endemic areas. Despite the high degree of genetic mixing described for Venezuelan population, a net predominance of the mild African G6PD A-(202A/376G) variant was observed among G6PDd subjects, suggesting a significant flow of G6PD genes from Africa to Americas, almost certainly introduced through African and/or Spanish immigrants during and after the colonization. The data suggest that 1:27 individuals of the studied population could be G6PDd and therefore at risk of haemolysis under precipitating factors. Information about PQ effect on G6PDd individuals carrying mild variant is limited, but since the regimen of 45 mg weekly dose for prevention of malaria relapse does not seem to be causing clinically significant haemolysis in people having the G6PD A-variant, a reasoned weighing of risk-benefit for its use in Venezuela should be done, when implementing public health strategies of control and elimination.
葡萄糖-6-磷酸脱氢酶(G6PD)缺乏症会导致急性溶血性贫血,由氧化药物如伯氨喹(PQ)引发,伯氨喹用于间日疟原虫疟疾的根治。然而,在许多间日疟流行地区,患者在未对其G6PD状态进行任何评估的情况下就接受了PQ治疗。
分别在委内瑞拉的东北部和东南部地区,即苏克雷州的卡希加尔市和玻利瓦尔州的西丰特斯市,评估G6PD缺乏症及其遗传异质性。通过定量方法对随机招募的664名无亲缘关系个体的血样进行G6PD活性筛查。对从G6PD缺乏(G6PDd)受试者分离的DNA通过聚合酶链反应-限制性片段长度多态性(PCR-RFLP)和直接DNA测序进行G6PD基因第4至8外显子的突变分析。
定量生化特征显示,总体上24名(3.6%)受试者为G6PDd(平均G6PD酶活性4.5±1.2 U/g Hb,中度缺乏,III类),而DNA分析显示其中19名(79.2%)有一个或两个突变等位基因。G6PD A-(202A/376G)变体是仅在17名(70.8%)个体中检测到的唯一变体,其中13名是半合子男性,4名是杂合子女性。两名男性仅携带376A→G突变。在所分析的外显子中未发现其他突变。
G6PDd患病率与附近国家所示的患病率一样低。本研究有助于了解委内瑞拉人群的遗传背景,特别是生活在疟疾流行地区的人群。尽管委内瑞拉人群存在高度的基因混合,但在G6PDd受试者中观察到轻度非洲G6PD A-(202A/376G)变体的净优势,这表明G6PD基因从非洲大量流入美洲,几乎可以肯定是在殖民期间和之后通过非洲和/或西班牙移民引入的。数据表明,所研究人群中每27人中有1人可能是G6PDd,因此在诱发因素下有溶血风险。关于PQ对携带轻度变体的G6PDd个体的影响的信息有限,但由于每周45毫克剂量预防疟疾复发的方案似乎不会在具有G6PD A变体的人群中引起临床上显著的溶血,在实施控制和消除的公共卫生策略时,应合理权衡其在委内瑞拉使用的风险效益。
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