Highly selective sodium glucose cotransporter type 2 inhibitor empagliflozin neuroprotective potential in chronic brain dyscirculation

О. S. Fuks, A. Simanenkova, N. Timkina, Polina A. Tikhomirova, Aleksandr Z. Gagiev, T. Karonova
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Abstract

Background. Chronic brain dyscirculation occurs in type 2 diabetes mellitus (DM2) with a high frequency and leads to patients disability. The early diagnosis of this disorder is difficult. Sodium-glucose cotransporter type 2 inhibitors are among the priority antidiabetic drugs due to their pronounced cardioprotective effect, but their effect on the central nervous system has not been studied enough. Aim. To study empagliflozin effect on clinical and laboratory parameters of brain damage in patients with DM2. Materials and methods. The study included patients with DM2 on metformin therapy (n=52). Patients with target glycated hemoglobin level formed the MET group (n=18), in those with non-target glycated hemoglobin level empagliflozin was added for 6 months (group MET+EMPA; n=19). A healthy control group was also created (n=15). The cognitive status and concentration of neurofilament light chains were studied. Results. In patients of the MET group, despite the target level of glycated hemoglobin, there was a cognitive deficit, according to the Montreal Cognitive Assessment: 25.0 (21.0; 27.0) points with a norm of 26 points or more. Therapy with empagliflozin led to the normalization of cognitive status after 6 months: 26.5 (24.0; 27.0) points. Initially, all patients had an increased neurofilament light chains level: 4.50 (3.31; 5.56) ng/ml in the MET group, 5.25 (3.75; 6.25) ng/ml in the MET+EMPA comparing with 3.50 (2.25; 3.50) ng/ml in the Control group. Empagliflozin therapy led to a decrease in this parameter after 3 months: 3.80 (3.25; 3.87) ng/ml and maintenance of this level after 6 months. Conclusion. DM2 is accompanied by pathological changes in the central nervous system even under satisfactory glycemic control. Empagliflozin therapy causes an improvement in cognitive status and a decrease in the level of neurofilament light chains.
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高选择性葡萄糖共转运蛋白2型抑制剂恩格列净在慢性脑循环障碍中的神经保护潜力
背景。慢性脑循环障碍发生于2型糖尿病(DM2),发病率高,可导致患者残疾。这种疾病的早期诊断是困难的。钠-葡萄糖共转运蛋白2型抑制剂因其明显的心脏保护作用而成为首选的降糖药物之一,但其对中枢神经系统的作用尚未得到足够的研究。的目标。探讨恩格列净对DM2患者脑损伤临床及实验室指标的影响。材料和方法。该研究包括二甲双胍治疗的DM2患者(n=52)。达到目标糖化血红蛋白水平的患者组成MET组(n=18),未达到目标糖化血红蛋白水平的患者加用恩格列净治疗6个月(MET+EMPA组;n = 19)。另设健康对照组(n=15)。对认知状态和神经丝轻链浓度进行了研究。结果。在MET组患者中,尽管糖化血红蛋白达到了目标水平,但仍存在认知缺陷,根据蒙特利尔认知评估:25.0 (21.0;27.0分),标准为26分或以上。恩格列净治疗导致6个月后认知状态正常化:26.5 (24.0;27.0)点。最初,所有患者的神经丝轻链水平均升高:4.50 (3.31;MET组为5.56)ng/ml, MET组为5.25 (3.75;MET+EMPA为6.25)ng/ml,而MET+EMPA为3.50 (2.25;对照组为3.50)ng/ml。依帕列净治疗导致3个月后该参数下降:3.80 (3.25;3.87) ng/ml, 6个月后维持该水平。结论。即使在血糖控制满意的情况下,DM2也伴有中枢神经系统的病理改变。恩帕列净治疗导致认知状态的改善和神经丝轻链水平的降低。
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