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Increased expression of phosphorylated forms of RNA-dependent protein kinase and eukaryotic initiation factor 2α may signal skeletal muscle atrophy in weight-losing cancer patients

机译:磷酸化形式的RNA依赖性蛋白激酶和真核起始因子2α的表达增加可能预示着体重减轻的癌症患者的骨骼肌萎缩

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摘要

Previous studies suggest that the activation (autophosphorylation) of dsRNA-dependent protein kinase (PKR) can stimulate protein degradation, and depress protein synthesis in skeletal muscle through phosphorylation of the translation initiation factor 2 (eIF2) on the α-subunit. To understand whether these mediators are important in muscle wasting in cancer patients, levels of the phospho forms of PKR and eIF2α have been determined in rectus abdominus muscle of weight losing patients with oesophago-gastric cancer, in comparison with healthy controls. Levels of both phospho PKR and phospho eIF2α were significantly enhanced in muscle of cancer patients with weight loss irrespective of the amount and there was a linear relationship between phosphorylation of PKR and phosphorylation of eIF2α (correlation coefficient 0.76, P=0.005). This suggests that phosphorylation of PKR led to phosphorylation of eIF2α. Myosin levels decreased as the weight loss increased, and there was a linear relationship between myosin expression and the extent of phosphorylation of eIF2α (correlation coefficient 0.77, P=0.004). These results suggest that phosphorylation of PKR may be an important initiator of muscle wasting in cancer patients.
机译:先前的研究表明,dsRNA依赖性蛋白激酶(PKR)的激活(自磷酸化)可以刺激蛋白降解,并通过α亚基上翻译起始因子2(eIF2)的磷酸化抑制骨骼肌中的蛋白合成。为了了解这些介质在癌症患者的肌肉消瘦中是否重要,与健康对照组相比,已确定体重减轻的食管胃癌患者的腹直肌中PKR和eIF2α的磷酸化水平。体重减轻的癌症患者的肌肉中,磷酸PKR和eIF2α的水平均显着升高,并且PKR磷酸化与eIF2α的磷酸化之间存在线性关系(相关系数0.76,P = 0.005)。这表明PKR的磷酸化导致eIF2α的磷酸化。随着体重增加,肌球蛋白水平降低,肌球蛋白表达与eIF2α磷酸化程度之间存在线性关系(相关系数0.77,P = 0.004)。这些结果表明,PKR的磷酸化可能是癌症患者肌肉消瘦的重要诱因。

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