2 型糖尿病合并射血分数保留型心力衰竭患者的代谢生物标志物

IF 0.7 Q4 ENDOCRINOLOGY & METABOLISM Diabetes Mellitus Pub Date : 2024-03-18 DOI:10.14341/dm13028
T. Sveklina, S. B. Shustov, S. N. Kolyubayeva, A. N. Kuchmin, V. A. Kozlov, E. V. Smirnova, A. V. Zharkov
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Finding differences between CSN-SFV and CSN-nFV biomarkers is a pressing scientific problem.AIM: To study the metabolic disorders biomarkers intergenic relationships, myocardial damage, and to evaluate their role in the CHF development in patients with DM2.MATERIALS AND METHODS: We studied the lipid and carbohydrate metabolism disorder genes polymorphisms frequencies in patients with CHF-CFV and DM2 (48 patients), CHF-NFV and DM2 (46) and patients with metabolic syndrome (MS) without CHF (68), mean age of patients was 69,7±5,3 yo. DNA was isolated from venous blood according to the manufacturer’s methodology. Gene polymorphisms were determined by real time PCR. 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引用次数: 0

摘要

背景:半数慢性心力衰竭(CHF)患者的射血分数(CHF-nEF)保持不变。使用药物治疗射血分数降低的慢性心力衰竭(CHF-nFV)可降低住院率,但不会影响 CHF-nFV 患者的心血管疾病发病率或总死亡率。目的:研究代谢紊乱生物标志物的基因间关系、心肌损伤,并评估它们在DM2患者CHF发病中的作用。材料与方法:我们研究了CHF-CFV和DM2患者(48例)、CHF-NFV和DM2患者(46例)以及无CHF的代谢综合征(MS)患者(68例)的脂质和碳水化合物代谢紊乱基因多态性频率,患者平均年龄为69,7±5,3岁。根据制造商提供的方法从静脉血中分离 DNA。基因多态性通过实时 PCR 检测。所研究的多态性与临床和实验室数据的相关性以及临床和实验室检测之间的关联通过回归分析确定。结果在对照组中,PPARG、APOC3 C3238G rs5128、LIPC -250 G>A rs2070895、APOA1 G-75A rs670、FABP2 Ala54Thr G>A rs1799883、ADRB2 5318 C>G rs1042714 基因存在多态性、这些基因多态性与共同依赖的 ADRB3、FTO、FABP2 基因多态性一起,构成了一个调节血浆中低密度脂蛋白、尿酸和 CAD 浓度的基因网络。研究发现,基因多态性与 CHF-CFV 患者的临床和/或实验室指标相关:PPARGC1AGly482Ser G>A rs8192678 与 CAD 相关;PPARGT-2821C rs12497191 与糖化血红蛋白水平相关;FTO A>T rs9939609(α-酮戊二酸依赖性二氧酶基因)与腰围相关;LEPR A>G rs1137101(瘦素受体基因)与 MAP 相关。在CHF-nFV患者中发现以下多态性与腰围相关:LIPC-250 G>A rs2070895(肝脏甘油三酯脂肪酶基因)与腰围相关;PPARGC1A Gly482Ser G>A rs8192678与腰围相关;FTO A>T rs9939609与腰围相关:从研究结果中可以看出,患有不同PV的CHF的DM2患者之间因存在易发生网络交互作用的多态性基因而存在显著差异。在CHF-sFV组中观察到的这种相互作用的数量最多,这决定了这种变异型CHF的病程比CHF-nFV患者的病程更复杂。
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Metabolic biomarkers in patients with type 2 diabetes mellitus and heart failure with preserved ejection fraction
BACKGROUND: Half of all patients with chronic heart failure (CHF) have preserved ejection fraction (CHF-nEF). The drug’s use effective for treatment of CHF with reduced ejection fraction (CHF-nFV) reduces the hospitalization incidence but does not affect the cardiovascular incidence or overall mortality in patients with CHF-nFV. Finding differences between CSN-SFV and CSN-nFV biomarkers is a pressing scientific problem.AIM: To study the metabolic disorders biomarkers intergenic relationships, myocardial damage, and to evaluate their role in the CHF development in patients with DM2.MATERIALS AND METHODS: We studied the lipid and carbohydrate metabolism disorder genes polymorphisms frequencies in patients with CHF-CFV and DM2 (48 patients), CHF-NFV and DM2 (46) and patients with metabolic syndrome (MS) without CHF (68), mean age of patients was 69,7±5,3 yo. DNA was isolated from venous blood according to the manufacturer’s methodology. Gene polymorphisms were determined by real time PCR. The studied polymorphisms correlations with clinical and laboratory data and associations between clinical and laboratory tests were identified by regression analysis.RESULTS: In the control group, PPARG, APOC3 C3238G rs5128, LIPC -250 G>A rs2070895, APOA1 G-75A rs670, FABP2 Ala54Thr G>A rs1799883, ADRB2 5318 C>G rs1042714 genes polymorphisms, along with co-dependent ADRB3, FTO, FABP2 genes polymorphic form a gene network regulating plasma concentrations of LDL, uric acid and CAD. Gene polymorphisms have been found to be associated with clinical and/or laboratory parameters in patients with CHF-CFV: PPARGC1AGly482Ser G>A rs8192678 with CAD; PPARGT-2821C rs12497191 with glycated hemoglobin level; FTO A>T rs9939609 (α-ketoglutarate dependent dioxygenase gene) with waist circumference; LEPR A>G rs1137101 (leptin receptor gene) with MAP. The following polymorphisms were found to be associated in patients with CHF-nFV: LIPC-250 G>A rs2070895 (liver triglyceride lipase gene) with MAP; PPARGC1A Gly482Ser G>A rs8192678 with MAP; FTO A>T rs9939609 with waist volume.CONCLUSIONS: From the study results, it is evident that patients with DM2 having CHF with different PV differ significantly among themselves by the presence of polymorphic genes prone to network interactions. The greatest number of such interactions is observed in the group of CHF-sFV, which determines a more complex course of this variant of CHF than in patients with CHF-nFV.
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来源期刊
Diabetes Mellitus
Diabetes Mellitus ENDOCRINOLOGY & METABOLISM-
CiteScore
1.90
自引率
40.00%
发文量
61
审稿时长
7 weeks
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