2 型糖尿病伴射血分数保留心力衰竭患者的炎症生物标志物。
Inflammatory Biomarkers in Patients With Type 2 Diabetes Mellitus and Heart Failure With Preserved Ejection Faction.
机构信息
Kirov Military Medical Academy, St. Petersburg.
Iljya Uljyanov Chuvash State University, Cheboksary.
出版信息
Kardiologiia. 2024 Jul 31;64(7):40-47. doi: 10.18087/cardio.2024.7.n2562.
AIM
To verify the relationship between gene polymorphisms of tumor necrosis factor alpha (TNF-α) and interleukin-6 (IL-6) with inflammation markers and codependent metabolic variables in patients with type 2 diabetes mellitus and chronic heart failure (CHF).
MATERIAL AND METHODS
This study included 154 patients (mean age, 69.1±3.2 years). The control group consisted of 47 patients with metabolic syndrome (MS) without CHF; the 2nd group included 56 patients with CHF with preserved ejection fraction (CHFpEF); and the 3rd group consisted of 51 patients with CHF with reduced ejection fraction (CHFrEF). The rs1800629 polymorphism of the TNF-α gene (TNF-α: G308A) was studied in real time by the polymerase chain reaction (PCR) method and the rs1800795 polymorphism of the IL-6 gene (IL-6: 174 G>C) was studied by PCR with the electrophoretic detection. The frequencies of polymorphic alleles were compared with the clinical blood test results, plasma concentrations of C-reactive protein (CRP), TNF-α, leptin, and fibrinogen. Differences between the groups were determined using the F test. Relationships between individual studied parameters were identified using the regression analysis.
RESULTS
In most patients, the occurrence of gene polymorphisms was eident as increased plasma concentrations of biomarkers. An association was found between the TNF-α gene polymorphism (G308A) and an increase in plasma TNF-α and between the IL-6 gene polymorphism (174 C>G) and an increase in plasma CRP. In the CHFpEF group, the rs1800629 gene polymorphism was observed in 55% of patients, among whom 93% had increased TNF-α. The rs1800795 gene polymorphism was observed in 82% of CHFpEF patients, among whom 21% had increased CRP. In the CHFrEF group, the G308A transition in the TNF-α gene was observed in 53% of patients; an increase in the respective cytokine was noted in 67% of patients; the IL-6 gene polymorphism 174 C>G was found in 78%, however, only 14% of patients with this polymorphism had also increased CRP. In the control group, the TNF-α G308A gene polymorphism was found in 30% of patients, while an increase in free TNF-α was associated with this polymorphism in 50% of patients; the IL-6 174 C>G gene polymorphism was detected in 78%, while no increase in the CRP level was observed in this group. This demonstrates a high probability of the TNF-α G308A gene polymorphism occurrence in patients with CHF.
CONCLUSION
Inflammatory markers are important predictors of CHF. The most significant predictor was the TNF-α G308A gene polymorphism, which was observed in more than 50% of patients, the majority of whom had an increase in plasma TNF-α.
目的
验证肿瘤坏死因子-α(TNF-α)和白细胞介素-6(IL-6)基因多态性与 2 型糖尿病伴慢性心力衰竭(CHF)患者炎症标志物和依存代谢变量之间的关系。
材料与方法
本研究纳入 154 例患者(平均年龄 69.1±3.2 岁)。对照组由 47 例无 CHF 的代谢综合征(MS)患者组成;第 2 组包括 56 例射血分数保留的 CHF(CHFpEF)患者;第 3 组包括 51 例射血分数降低的 CHF(CHFrEF)患者。采用实时聚合酶链反应(PCR)法检测 TNF-α 基因 rs1800629 多态性(TNF-α:G308A),采用 PCR 电泳检测 IL-6 基因 rs1800795 多态性(IL-6:174 G>C)。将多态性等位基因频率与临床血液检查结果、血浆 C 反应蛋白(CRP)、TNF-α、瘦素和纤维蛋白原浓度进行比较。采用 F 检验比较组间差异。采用回归分析确定各研究参数之间的关系。
结果
在大多数患者中,基因多态性的发生与生物标志物血浆浓度的升高有关。TNF-α 基因多态性(G308A)与 TNF-α 血浆浓度升高有关,IL-6 基因多态性(174 C>G)与 CRP 血浆浓度升高有关。在 CHFpEF 组中,rs1800629 基因多态性在 55%的患者中观察到,其中 93%的患者 TNF-α 升高。rs1800795 基因多态性在 82%的 CHFpEF 患者中观察到,其中 21%的患者 CRP 升高。在 CHFrEF 组中,TNF-α 基因 G308A 转换在 53%的患者中观察到;在 67%的患者中观察到相应细胞因子升高;IL-6 基因多态性 174 C>G 在 78%的患者中发现,但只有 14%的具有该多态性的患者 CRP 也升高。在对照组中,TNF-α G308A 基因多态性在 30%的患者中观察到,而在这组患者中,50%的患者与该多态性相关的游离 TNF-α升高;IL-6 174 C>G 基因多态性在 78%的患者中检测到,但该组患者 CRP 水平无升高。这表明 TNF-α G308A 基因多态性在 CHF 患者中发生的可能性较高。
结论
炎症标志物是 CHF 的重要预测指标。最显著的预测因子是 TNF-α G308A 基因多态性,该多态性在超过 50%的患者中观察到,其中大多数患者的 TNF-α 血浆浓度升高。
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