Insulin mitigates acute ischemia–induced atrial fibrillation and sinoatrial node dysfunction ex vivo
Huiliang Qiu, … , Michael Rubart, Wuqiang Zhu
Huiliang Qiu, … , Michael Rubart, Wuqiang Zhu
Published November 14, 2024
Citation Information: JCI Insight. 2025;10(1):e185961. https://doi.org/10.1172/jci.insight.185961.
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Research Article Cardiology Therapeutics

Insulin mitigates acute ischemia–induced atrial fibrillation and sinoatrial node dysfunction ex vivo

Abstract

Acute atrial ischemia is a well-known cause of postoperative atrial fibrillation (POAF). However, mechanisms through which ischemia contributes to the development of POAF are not well understood. In this study, ex vivo Langendorff perfusion was used to induce acute ischemia/reperfusion in the heart to mimic POAF. Inducibility of atrial fibrillation (AF) was evaluated using programmed electrical stimulation and verified with open-atrium optical mapping. Compared with the control group without ischemia, 25 minutes of ischemia substantially increased the incidence of AF. The right atrium was more susceptible to AF than the left atrium. Administering insulin for 30 minutes before ischemia and during reperfusion with 25 minutes of ischemia greatly reduced the vulnerability to AF. However, insulin treatment during reperfusion only did not show substantial benefits against AF. Optical mapping studies showed that insulin mitigated ischemia-induced abnormal electrophysiology, including shortened action potential duration and effective refractory period, slowed conduction velocity, increased conduction heterogeneity, and altered calcium transients. In conclusion, insulin reduced the risk of acute ischemia/reperfusion–induced AF via improving the electrophysiology and calcium handling of atrial cardiomyocytes, which provides a potential therapy for POAF.

Authors

Huiliang Qiu, Fan Li, Hannah Prachyl, Alejandra Patino-Guerrero, Michael Rubart, Wuqiang Zhu

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Figure 2

Insulin prevents I/R-induced RAF.

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Insulin prevents I/R-induced RAF. (A) Experimental groups. IS-25, ischem...
(A) Experimental groups. IS-25, ischemia for 25 minutes without insulin; IS-25ins, ischemia for 25 minutes with insulin; 11.3GLU, treatment with high concentration of glucose (11.2 mM) without insulin; PRV, treatment with pyruvate without insulin; PRVins, treatment with pyruvate plus insulin; Insulin-reperfusion, insulin treatment during reperfusion only. (B) Inducibility of RAF. (C) RAF duration. (D) SANRT. (E and F) Effective refractory period (ERP). Horizontal bars represent individual comparisons (P < 0.05). (G) Pacing threshold. Data in all panels except for C were presented as mean ± SEM; n = 6 (biological repeats) per group; statistical analysis was performed by 1-way ANOVA with Tukey’s test. Data in C were presented as median [25 to 75 percentile]. n = 14, 11, 14, 6, 7, and 7 (technical repeats), respectively, in IS-25, IS-25ins, 11.2GLU, PRV, PRVins, and Insulin-reperfusion; statistical analysis was performed by Kruskal-Wallis test with Dunn’s multiple-comparison test.