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高剂量皮质类固醇对蛋白水解级联系统的调节作用。

Modulation of the proteolytic cascade systems by high dose corticosteroids.

作者信息

Aasen A O, Ruud T E, Pillgram-Larsen J, Röise O, Stadaas J

出版信息

Acta Chir Scand Suppl. 1985;526:56-65.

PMID:3911708
Abstract

The effects of high-dose corticosteroids (HDC) on activities within the proteolytic cascade systems were studied in vitro and in vivo using chromogenic peptide substrate assays. In in vitro experiments 20 mg methylprednisolone sodium succinate (Solu-Medrol) per ml plasma significantly inhibited activation of plasma prekallikrein, prothrombin and plasminogen and reduced functional plasma kallikrein inhibition, antithrombin and antiplasmin activities. The effects of HDC on activities within these proteolytic cascade systems were further evaluated in experimental acute pancreatitis in pigs. Acute pancreatitis was induced by injection of Na-taurocholate into the pancreatic duct. Seven test animals received methylprednisolone sodium succinate 30 mg per kg intravenously for 30 minutes before the induction of pancreatitis as pretreatment. Eight animals remained untreated. Trypsin (TRY), plasma prekallikrein (PKK), plasma kallikrein (KK) and functional plasma kallikrein inhibition capacity (KKI) were studied in the peritoneal exudate. Cardiac output (CO) and mean arterial pressure (MAP) were monitored regularly before and during a 6 hour observation period. During untreated pancreatitis a reduction of PKK levels of about 40% were found, paralleled by an increased KK activity and a reduction of KKI capacity. Several of the animals experienced high TRY activities. The mortality rate was 63% (5 out of 8 animals). In the pretreated groups, all animals survived the observation period. CO and MAP were significantly less reduced than the untreated group at 6 hours. HDC was also found to reduce significantly plasma kallikrein activities in the peritoneal exudate compared with untreated animals. No changes in TRY activities were found in pretreated animals. Furthermore, plasma prekallikrein and functional plasma kallikrein inhibition values in the exudate were elevated significantly in HDC treated animals compared with untreated animals.

摘要

使用发色肽底物分析法在体外和体内研究了高剂量皮质类固醇(HDC)对蛋白水解级联系统内活性的影响。在体外实验中,每毫升血浆中20毫克甲泼尼龙琥珀酸钠(甲强龙)显著抑制血浆前激肽释放酶、凝血酶原和纤溶酶原的激活,并降低血浆激肽释放酶功能抑制、抗凝血酶和抗纤溶酶活性。在猪的实验性急性胰腺炎中进一步评估了HDC对这些蛋白水解级联系统内活性的影响。通过将牛磺胆酸钠注入胰管诱导急性胰腺炎。7只试验动物在诱导胰腺炎前30分钟静脉注射每千克30毫克甲泼尼龙琥珀酸钠作为预处理。8只动物未接受治疗。研究了腹腔渗出液中的胰蛋白酶(TRY)、血浆前激肽释放酶(PKK)、血浆激肽释放酶(KK)和血浆激肽释放酶功能抑制能力(KKI)。在6小时观察期之前和期间定期监测心输出量(CO)和平均动脉压(MAP)。在未治疗的胰腺炎期间,发现PKK水平降低约40%,同时KK活性增加,KKI能力降低。几只动物出现高TRY活性。死亡率为63%(8只动物中的5只)。在预处理组中,所有动物在观察期内存活。在6小时时,CO和MAP的降低明显低于未治疗组。与未治疗的动物相比,还发现HDC显著降低了腹腔渗出液中的血浆激肽释放酶活性。在预处理的动物中未发现TRY活性有变化。此外,与未治疗的动物相比,HDC治疗的动物渗出液中的血浆前激肽释放酶和血浆激肽释放酶功能抑制值显著升高。

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