TCF7L2多态性与心肌梗死后一氧化氮释放低、内皮功能障碍和炎症反应增强有关

Riobaldo Cintra , Filipe A. Moura , Luiz S.F. Carvalho , Mauricio Daher , Simone N. Santos , Ana P.R. Costa , Valeria N. Figueiredo , Joalbo M. Andrade , Francisco A.R. Neves , Jose C. Quinaglia e Silva , Andrei C. Sposito , on behalf of the Brasília Heart Study Group
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引用次数: 2

摘要

由于外源性胰岛素给药的机制研究和临床试验之间的分歧,胰岛素在心肌梗死(MI)期间的有利作用尚不清楚。转录因子7-样2 (TCF7L2)基因rs7903146多态性与胰岛素分泌减少有关。方法在非糖尿病st段抬高型心肌梗死(STEMI)患者中,采用基因决定的内源性胰岛素分泌下调模型,研究入院(D1)至心肌梗死后第5天(D5)血浆胰岛素、c肽、白细胞介素-2 (IL-2)、c反应蛋白(CRP)和一氧化氮(NOx)水平的变化。入院时和心肌梗死后30天分别进行冠状动脉造影和血流介导扩张(FMD)。稳态模型评估评估胰岛素分泌(HOMA2%β)和胰岛素敏感性(HOMA2%S)。结果携带t等位基因的患者在D1和D5的血糖水平均有较低的homa2 - β和较高的homa2 - s。与非携带者相比,t等位基因携带者在D5时血浆IL-2和CRP较高,冠状动脉内血栓分级较高,D1和D5间FMD和NOx变化较低,30天死亡率较高。结论在非糖尿病STEMI患者中,rs7903146 TCF7L2基因多态性与胰岛素分泌降低、内皮功能恶化、冠状动脉血栓负担加重和短期死亡率升高有关。一般意义在心肌梗死急性期,胰岛素分泌能力降低可能影响临床结果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

TCF7L2 polymorphism is associated with low nitric oxide release, endothelial dysfunction and enhanced inflammatory response after myocardial infarction

TCF7L2 polymorphism is associated with low nitric oxide release, endothelial dysfunction and enhanced inflammatory response after myocardial infarction

TCF7L2 polymorphism is associated with low nitric oxide release, endothelial dysfunction and enhanced inflammatory response after myocardial infarction

Backgound

The favorable effects of insulin during myocardial infarction (MI) remain unclear due to the divergence between mechanistic studies and clinical trials of exogenous insulin administration. The rs7903146 polymorphism of the transcription factor 7-like 2 (TCF7L2) gene is associated with attenuated insulin secretion.

Methods

In non-diabetic patients with ST-elevation MI (STEMI), using such a model of genetically determined down-regulation of endogenous insulin secretion we investigated the change in plasma insulin, C-peptide, interleukin-2 (IL-2), C-reactive protein (CRP), and nitric oxide (NOx) levels between admission (D1) and the fifth day after MI (D5). Coronary angiography and flow-mediated dilation (FMD) were performed at admission and 30 days after MI, respectively. Homeostasis Model Assessment estimated insulin secretion (HOMA2%β) and insulin sensitivity (HOMA2%S).

Results

Although glycemia did not differ between genotypes, carriers of the T-allele had lower HOMA2%β and higher HOMA2%S at both D1 and D5. As compared with non-carriers, T-allele carriers had higher plasma IL-2 and CRP at D5, higher intracoronary thrombus grade, lower FMD and NOx change between D1 and D5 and higher 30-day mortality.

Conclusion

In non-diabetic STEMI patients, the rs7903146 TCF7L2 gene polymorphism is associated with lower insulin secretion, worse endothelial function, higher coronary thrombotic burden, and higher short-term mortality.

General significance

During the acute phase of MI, a lower capacity of insulin secretion may influence clinical outcome.

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