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Dynamics of tissue ubiquitin pools and ubiquitin-proteasome pathway component activities during the systemic response to traumatic shock

机译:创伤性休克全身反应过程中组织遍在蛋白池和遍在蛋白-蛋白酶体途径组分活动的动态

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摘要

Based on the biological significance of the ubiquitin-proteasome pathway (UPP) and its potential role during sepsis, burns and ischemia-reperfusion injury, we hypothesized that the systemic response to traumatic shock (TS) is accompanied by tissue-specific UPP alterations. Therefore, we studied tissue ubiquitin pools, chymotryptic- and trypticlike proteasome peptidase activities and ubiquitin-protein ligation (UbPL) rates in skeletal muscle, heart, lung, liver, spleen and kidney using a clinically relevant porcine model (bilateral femur fracture/hemorrhage followed by fluid resuscitation). TS induced a systemic reduction of tissue-specific high molecular mass ubiquitin-protein conjugates (> 50 kDa). Free ubiquitin was unaffected. The dynamic organ patterns of ubiquitin pools paralleled the typical physiological response to TS and resuscitation. Reduction of ubiquitin-protein conjugates was most pronounced in heart and lung (p < 0.05 vs. control) and accompanied by significant increases in proteasome peptidase and UbPL activities in these organs. Unlike all other tissues, spleen proteasome peptidase and UbPL activities were significantly reduced 10 h after TS. These findings support the concept that the UPP could play an important role in regulation of cell functions during the early whole-body response to TS. The UPP might be a therapeutic target to improve the metabolic care after TS, particularly in the heart, lung, and spleen.
机译:基于泛素-蛋白酶体途径(UPP)的生物学意义及其在败血症,烧伤和局部缺血-再灌注损伤中的潜在作用,我们假设对创伤性休克(TS)的全身反应伴随组织特异性UPP改变。因此,我们使用临床相关的猪模型研究了骨骼肌,心脏,肺,肝,脾和肾中组织泛素库,胰凝乳蛋白酶和胰蛋白酶样蛋白酶体肽酶活性以及泛素蛋白结扎(UbPL)率(双侧股骨骨折/出血通过液体复苏)。 TS诱导组织特异性高分子量泛素-蛋白质偶联物(> 50 kDa)的全身性降低。游离泛素不受影响。遍在蛋白池的动态器官模式与对TS和复苏的典型生理反应平行。心脏和肺中泛素蛋白偶联物的减少最为明显(与对照组相比,p <0.05),并伴随着这些器官中蛋白酶体肽酶和UbPL活性的显着增加。与所有其他组织不同,TS后10 h脾蛋白酶体肽酶和UbPL活性显着降低。这些发现支持了这样的观念:UPP可以在全身对TS的早期反应期间在调节细胞功能中发挥重要作用。 UPP可能是改善TS后代谢护理的治疗目标,尤其是在心脏,肺和脾脏中。

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