首页> 外文期刊>Journal of enzyme inhibition and medicinal chemistry. >Potentiation of the reductase activity of protein disulphide isomerase (PDI) by 19-nortestosterone, bacitracin, fluoxetine, and ammonium sulphate
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Potentiation of the reductase activity of protein disulphide isomerase (PDI) by 19-nortestosterone, bacitracin, fluoxetine, and ammonium sulphate

机译:19-去甲睾丸激素,杆菌肽,氟西汀和硫酸铵可增强蛋白质二硫键异构酶(PDI)的还原酶活性

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Protein disulphide isomerase (PDI) in the endoplasmic reticulum catalyzes the rearrangement of disulphide bridges during folding of secreted proteins. It binds various molecules that inhibit its activity. But here, we looked for molecules that would potentiate its activity. PDI reductase activity was measured in vitro using di-eosin-oxidized glutathione as substrate. Its classical inhibitor bacitracin was found to exert a biphasic effect: stimulatory at low concentrations (10?6 M) and inhibitory only at higher concentrations (10?4–10?3 M). The weak oestrogenic molecule bisphenol A was found to exert a weak inhibitory effect on PDI reductase activity relative to the strong oestrogens, ethynylestradiol, and diethylstilbestrol. Like 19-nortestosterone, fluoxetine was found to exert a potentiating effect on PDI reductase activity and their potentiating effects could be reversed by increasing concentrations of oestrogens. In conclusion, this paper provides the first identification of potentiators of PDI activity that are potential pharmaceuticals against pathologies affecting protein folding such as Alzheimer’s disease.
机译:内质网中的蛋白质二硫键异构酶(PDI)在分泌的蛋白质折叠过程中催化二硫键的重排。它结合各种抑制其活性的分子。但是在这里,我们寻找了能够增强其活性的分子。使用二曙红氧化的谷胱甘肽作为底物在体外测量PDI还原酶活性。发现其经典抑制剂杆菌肽具有双相作用:低浓度(10 ?6 M)具有刺激性,而高浓度(10 ? 4 < / sup> –10 ?3 M)。相对于强雌激素,乙炔雌二醇和己烯雌酚,发现弱雌激素分子双酚A对PDI还原酶活性的抑制作用较弱。像19-去甲睾丸激素一样,氟西汀被发现对PDI还原酶活性具有增强作用,而其增强作用可通过增加雌激素的浓度来逆转。总之,本文首次鉴定了PDI活性增效剂,这些增效剂是潜在的药物,可抗击影响蛋白质折叠的疾病,例如阿尔茨海默氏病。

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