Department of Analytical Chemistry and Physical Chemistry, School of Pharmacy and Biochemistry, University of Buenos Aires , Buenos Aires , Argentina.
Institute of Biochemistry and Molecular Medicine (IBIMOL UBA-CONICET) , Buenos Aires , Argentina.
Free Radic Res. 2019 Oct;53(9-10):993-1004. doi: 10.1080/10715762.2019.1661404. Epub 2019 Sep 12.
Sildenafil is a phosphodiesterase type 5 inhibitor which confers cardioprotection against myocardial ischaemia/reperfusion (I/R) injury. The aim of this study was to determine if Trx1 participates in cardioprotection exerted by sildenafil in an acute model of I/R, and to evaluate mitochondrial bioenergetics and cellular redox status. Langendorff-perfused hearts from wild type (WT) mice and a dominant negative (DN-Trx1) mutant of Trx1 were assigned to placebo or sildenafil (0.7 mg/kg i.p.) and subjected to 30 min of ischaemia followed by 120 min of reperfusion. WT + S showed a significant reduction of infarct size (51.2 ± 3.0% vs. 30 ± 3.0%, < .001), an effect not observed in DN-Trx. After I/R, sildenafil preserved state 3 oxygen consumption from WT, but had a milder effect in DN-Trx1 only partially protecting state 3 values. Treatment restored respiratory control (RC) after I/R, which resulted 8% (WT) and 24% (DN-Trx1) lower than in basal conditions. After I/R, a significant increase in HO production was observed both for WT and DN-Trx (WT: 1.17 ± 0.13 nmol/mg protein and DN-Trx: 1.38 ± 0.12 nmol/min mg protein). With sildenafil, values were 21% lower only in WT I/R. Treatment decreased GSSG levels both in WT and DN-Trx1. In addition, GSSG/GSH ratio was partially restored by sildenafil. Also, an increase in p-eNOS/eNOS even before the myocardial ischaemia was observed with sildenafil, both in WT (14%, > .05) and in DN-Trx (35%, < .05). Active Trx1 is required for the onset of the cardioprotective effects of sildenafil on I/R injury, together with the preservation of cellular redox balance and mitochondrial function.
西地那非是一种磷酸二酯酶 5 抑制剂,可对抗心肌缺血/再灌注(I/R)损伤提供心脏保护。本研究的目的是确定 Trx1 是否参与了西地那非在急性 I/R 模型中的心脏保护作用,并评估线粒体生物能学和细胞氧化还原状态。从野生型(WT)小鼠和 Trx1 的显性负(DN-Trx1)突变体的 Langendorff 灌注心脏中,将安慰剂或西地那非(0.7mg/kg i.p.)分配给 WT 或 WT+S,并进行 30min 的缺血,然后进行 120min 的再灌注。WT+S 显著减少了梗死面积(51.2±3.0% vs. 30±3.0%, <.001),而在 DN-Trx1 中则没有观察到这种作用。I/R 后,西地那非维持了 WT 的状态 3 氧消耗,但在 DN-Trx1 中作用较弱,仅部分保护了状态 3 值。治疗后 I/R 后恢复了呼吸控制(RC),RC 分别比基础值低 8%(WT)和 24%(DN-Trx1)。I/R 后,WT 和 DN-Trx 的 HO 产量均显著增加(WT:1.17±0.13 nmol/mg 蛋白和 DN-Trx:1.38±0.12 nmol/min mg 蛋白)。西地那非治疗后,WT I/R 组的数值降低了 21%。治疗后,WT 和 DN-Trx1 中的 GSSG 水平均降低。此外,西地那非部分恢复了 GSSG/GSH 比值。此外,在 I/R 之前,WT(14%, >.05)和 DN-Trx(35%, <.05)中均观察到 p-eNOS/eNOS 的增加。活性 Trx1 是西地那非对 I/R 损伤产生心脏保护作用所必需的,同时还维持了细胞氧化还原平衡和线粒体功能。
