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Sevoflurane modulates the activity of glyceraldehyde 3-phosphate dehydrogenase.

机译:七氟醚调节3-磷酸甘油醛脱氢酶的活性。

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The mechanism of inhalation anesthesia remains to be fully elucidated. While certain neuronal membrane proteins are considered sites of action, cytosolic proteins may also be targets. We hypothesize that inhaled anesthetics may act via glyceraldehyde 3-phosphate dehydrogenase (GAPDH), which has recently been shown to participate in neuronal inhibition. We examined the effects of sevoflurane, a halogenated ether anesthetic, on the catalytic and fluorescence properties of GAPDH. Initial rates of oxidoreductase activity decreased approximately 30% at saturating levels of sevoflurane. NADH-stimulated oxidoreductase activity (25 microM NADH; 0.8mM NAD+) increased with sevoflurane. Sevoflurane quenched tryptophan fluorescence emission and increased polarization. Additionally, sevoflurane increased the susceptibility of GAPDH to thermal denaturation suggesting an effect on conformation. Our findings warrant further research on sevoflurane's effect on GAPDH and indicate that this approach may lead to delineation of a novel contribution to the mechanism of anesthesia.
机译:吸入麻醉的机制仍有待充分阐明。虽然某些神经元膜蛋白被认为是作用部位,但胞质蛋白也可能是靶标。我们假设吸入麻醉药可能通过3-磷酸甘油醛脱氢酶(GAPDH)起作用,最近该研究表明它可以参与神经元抑制作用。我们研究了七氟醚(一种卤代醚麻醉剂)对GAPDH催化和荧光性质的影响。在七氟醚饱和水平下,氧化还原酶活性的初始速率降低了约30%。随着七氟醚的增加,NADH刺激的氧化还原酶活性(25 microM NADH; 0.8mM NAD +)增加。七氟醚淬灭了色氨酸的荧光发射并增强了极化。另外,七氟醚增加了GAPDH对热变性的敏感性,表明对构象有影响。我们的发现值得对七氟醚对GAPDH的作用进行进一步研究,并表明这种方法可能导致描述对麻醉机制的新贡献。

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