c.202G > A/c.376A > G G6PD 多态性增加急性髓性白血病患者真菌感染的风险

Noeme Henriques Freitas, Cinthia Cristina Matheus Xerez Albuquerque, Mariana Pereira Lima, N. A. Fraiji, Marilda de Souza Gonçalves, J. P. M. Moura Neto
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引用次数: 0

摘要

简介急性髓性白血病(AML)患者感染多种类型感染的风险较高,其中真菌感染(FI)是发病和死亡的主要原因之一。葡萄糖-6-磷酸脱氢酶(G6PD)是一种存在于所有细胞中的酶,是白细胞产生碱性和酸性蛋白酶所必需的,这些蛋白酶用于消灭入侵的微生物。本研究的目的是评估 G6PD 基因多态性与 FI 是否同时与巴西玛瑙斯亚马孙州血液中心(HEMOAM)随访的确诊急性髓细胞白血病患者的临床事件和发病率有关:研究对象为被诊断为急性髓性白血病并在亚马孙州血液中心(HEMOAM)接受治疗的成人和儿童,性别不限,年龄不限。使用实时 PCR(qPCR)进行分子基因分型,随后进行 Sanger 测序以确认 c.202G > A/c.376A > G 多态性:研究共涉及 157 名患者(男性 91 人(58%),女性 66 人(42%))。研究组中最常见的急性髓细胞性白血病亚型是M3型,有63名患者(40.12%),其次是M5型,有33名患者(21.02%),M2型有21名患者(13.37%),M4型有15名患者(9.55%),男女发病率相似。真菌感染的男女发病率相同;但女性出现瘀斑(p = 0.004)、呕吐(p = 0.016)和心脏改变(p < 0.001)的比例较高,而男性出现持续咳嗽(p = 0.049)和腹泻(p < 0.001)的比例较高。共有18名患者出现G6PD多态性,其中8人(5.1%)为c.202GA/AA,18人(11.5%)为c.376AG/GG,4人(2.5%)同时出现两种多态性(c.202AA/c.376GG)。然而,具有这些多态性的 FI 患者的死亡发生率要高得多(p < 0.001):我们相信,G6PD 多态性的确定将有助于制定监测策略,并有助于急性髓细胞性白血病的早期诊断和有针对性的适当治疗。此外,评估 G6PD 多态性的活性还有助于识别 FI 风险较高的急性髓细胞性白血病患者,从而制定更深入的治疗和监测策略。
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c.202G > A/c.376A > G G6PD Polymorphisms Increase the Risk of Fungal Infections in Acute Myeloid Leukemia Patients
Introduction: Patients with acute myeloid leukemia (AML) show a higher risk for several types of infections, including fungal infections (FI), which are one of the main causes of morbidity and mortality. Glucose-6-phosphate dehydrogenase (G6PD) is an enzyme located in all cells that is very necessary in leukocytes for the production of basic and acid proteases that are used to destroy invading microorganisms. Our objective in this study was to evaluate whether polymorphisms in the G6PD gene concomitantly with FI are associated with clinical events and morbidity in patients diagnosed with AML and followed up at the Amazonas State Blood Center (HEMOAM), Manaus, Brazil. Materials and Methods: The study population was randomly constituted of adults and children, of either sex, and any age, with a diagnosis of acute myeloid leukemia, all of whom were undergoing treatment at the HEMOAM. Molecular genotyping was performed using real-time PCR (qPCR) and subsequent Sanger sequencing to confirm the c.202G > A/c.376A > G polymorphisms. Results: A total of 157 patients (91 (58%) males and 66 (42%) females) were involved in the study. The most prevalent AML subtype in the studied group was M3 in 63 patients (40.12%), followed by M5 in 33 patients (21.02%), M2 in 21 patients (13.37%) and M4 in 15 patients (9.55%), with a similar prevalence between genders. The prevalence of fungal infections was identical between genders; however, bruising (p = 0.004), vomiting (p = 0.016) and cardiac alterations (p < 0.001) were higher in females, while persistent cough (p = 0.049) and diarrhea (p < 0.001) were higher in males. A total of eighteen patients presents G6PD polymorphisms, with 8 (5.1%) of these for c.202GA/AA, 18 (11.5%) for c.376AG/GG and 4 (2.5%) for both polymorphisms concomitantly (c.202AA/c.376GG). However, the prevalence of death in patients affected with FI was much higher in those that have these polymorphisms (p < 0.001). Conclusion: We believe that the determination of G6PD polymorphisms will allow the development of monitoring strategies, and aid in early diagnosis and the appropriate and targeted treatment for AML. In addition, evaluating their activity may help to identify AML patients at a higher risk of FI, thus allowing the design of more intensive therapeutic and surveillance strategies.
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