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首页> 美国卫生研究院文献>International Journal of Clinical and Experimental Pathology >Delayed cardioprotection by sevoflurane preconditioning: a novel mechanism via inhibiting Beclin 1-mediated autophagic cell death in cardiac myocytes exposed to hypoxia/reoxygenation injury
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Delayed cardioprotection by sevoflurane preconditioning: a novel mechanism via inhibiting Beclin 1-mediated autophagic cell death in cardiac myocytes exposed to hypoxia/reoxygenation injury

机译:七氟醚预处理对心脏的保护作用延迟:一种通过抑制Beclin 1介导的缺氧/复氧损伤心肌细胞自噬细胞死亡的新机制

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Sevoflurane preconditioning has shown to exert delayed caridioprotection against subsequent ischemia and reperfusion injury, but the mechanisms underlying is unclear. Inhibition of autophagy by 3-methyladenine (3-MA) or knockdown of Beclin 1 leads to enhanced cardiac myocyte survival. Our study aimed to test whether sevoflurane preconditioning provides a second window of anesthetic preconditioning (SWOP) via inhibit Beclin 1-mediated autophagic cell death. H9c2 rat cardiomyocytes were randomly divided into five groups: Control (CON) group; hypoxia/reoxygenation (H/R) group, rat cardiomyocytes was exposed in the airtight container for 2 h followed by 1 h of reoxgenation; SWOP group, rat cardiomyocytes was exposed to 1 h of 2.5% sevoflurane 24 h before H/R; Autophagic inhibitors, 3-methyladenine (3-MA, 10 mM) was added to culture medium 15 min before sevoflurane exposure (3-MA+SWOP group) or cells were treated by 3-MA alone (3-MA group). The cell proliferation was significantly increased in SWOP group (79.49 ± 1.37%, P < 0.05) when compared to H/R group (62.2 ± 6.49%, P < 0.05). 3-MA administered before SWOP significantly attenuated the H/R induced autophagy and cell death. H/R injury up-regulated the expression of LC3-II and Beclin 1 proteins (342 ± 66% and 163 ± 18%, respectively, P < 0.05) compared to the CON group (100%), which were increased in SWOP group (202 ± 77% and 128 ± 8%, respectively, P < 0.05). The expression of LC3-II and Beclin 1 proteins was decreased in 3-MA group (110 ± 28% and 97 ± 6%, respectively) and 3-MA+SWOP group (93 ± 7% and 98 ± 6%, respectively) compared with H/R group, but Bcl-2 was upregulated in 3-MA group (158 ± 4%) and 3-MA+SWOP group (156 ± 5%) compared to H/R group (103 ± 7%). In conclusion, sevoflurane preconditioning confers delayed cardioprotection via inhibition Beclin 1-mediated autophagic cell death in cardiac myocytes 24 h before exposed to H/R injury.
机译:七氟醚预处理已显示出对随后的局部缺血和再灌注损伤的延迟心血管保护作用,但其潜在机制尚不清楚。 3-甲基腺嘌呤(3-MA)抑制自噬或Beclin 1的敲低导致心肌细胞存活增加。我们的研究旨在测试七氟醚预处理是否通过抑制Beclin 1介导的自噬细胞死亡提供了麻醉剂预处理(SWOP)的第二窗口。 H9c2大鼠心肌细胞随机分为5组:对照组(CON)组; H9c2大鼠心肌细胞。低氧/复氧(H / R)组,将大鼠心肌细胞在密闭容器中暴露2 h,然后再进行1 h复氧。 SWOP组,大鼠心肌细胞在H / R前24小时暴露于2.5%七氟醚中1小时。将自噬抑制剂3-甲基腺嘌呤(3-MA,10 mM)加入七氟醚暴露15分钟前(3-MA + SWOP组)或仅通过3-MA处理细胞(3-MA组)15分钟。与H / R组(62.2±6.49%,P <0.05)相比,SWOP组的细胞增殖显着增加(79.49±1.37%,P <0.05)。在SWOP之前使用3-MA可以显着减轻H / R诱导的自噬和细胞死亡。与CON组(100%)相比,H / R损伤上调LC3-II和Beclin 1蛋白的表达(分别为342±66%和163±18%,P <0.05),而SWOP组有所增加(分别为202±77%和128±8%,P <0.05)。 3-MA组(分别为110±28%和97±6%)和3-MA + SWOP组(分别为93±7%和98±6%)的LC3-II和Beclin 1蛋白的表达降低。与H / R组相比,Bcl-2在3-MA组(158±4%)和3-MA + SWOP组(156±5%)高于H / R组(103±7%)。总之,在暴露于H / R损伤前24小时,七氟醚预处理通过抑制Beclin 1介导的自噬细胞在心肌细胞中的死亡而赋予了延迟的心脏保护作用。

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