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The effects of a thromboxane A2 synthesis inhibitor and a prostaglandin I2 analogue on experimental acute necrotizing pancreatitis in rats.

机译:血栓烷A2合成抑制剂和前列腺素I2类似物对大鼠实验性急性坏死性胰腺炎的作用。

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To elucidate the role of thromboxane A2 (TxA2) and prostaglandin I2 (PGI2) in acute necrotizing pancreatitis (ANP) in rats and to determine the effect of the TxA2 synthesis inhibitor OKY-046 and the PGI2 analogue OP-2507, the levels of two prostanoids (TxB2, 6-keto PGF1alpha) and two types of phospholipase A2 (PLA2) activity (cytosolic and secretory) were measured in plasma and three tissues (pancreas, lung, and kidney) after injection of a mixed solution of 5% sodium taurocholate and 0.1% trypsin into the pancreatic duct to induce ANP. The survival rate 24 h after inducing ANP was 33.3% in the nontreated group, versus 83.3 and 58.3% in the groups treated with OKY-046 and OP-2507, respectively. Only the group treated with OKY-046 showed significant improvement compared with the nontreated group. The plasma, pancreatic, and pulmonary TxB2 levels decreased significantly in the group treated with OKY-046, and the histopathological changes were not as severe. The levels of pancreatic and pulmonary cytosolic PLA2 activities decreased, and plasma and pancreatic secretory PLA2 activities also decreased. In conclusion, the levels of both types of PLA2 activity and TxA2 production decreased, and the survival rate improved as a result in the group treated with OKY-046, but OP-2507 had no effect on ANP. TxA2 and two types of PLA2 activity play an important role in the process of aggravation of acute pancreatitis.
机译:为了阐明血栓烷A2(TxA2)和前列腺素I2(PGI2)在大鼠急性坏死性胰腺炎(ANP)中的作用,并确定TxA2合成抑制剂OKY-046和PGI2类似物OP-2507的作用,两种在注射5%牛磺胆酸钠溶液后,在血浆和三个组织(胰腺,肺和肾脏)中分别测定了类前列腺素(TxB2、6-酮PGF1alpha)和两种磷脂酶A2(PLA2)的活性(胞浆和分泌液) 0.1%胰蛋白酶进入胰管以诱导ANP。在未经治疗的组中,诱导ANP后24小时的存活率为33.3%,而用OKY-046和OP-2507治疗的组分别为83.3和58.3%。与未治疗组相比,只有用OKY-046治疗的组显示出明显的改善。 OKY-046治疗组的血浆,胰腺和肺TxB2水平显着降低,并且组织病理学变化不那么严重。胰腺和肺胞质PLA2活性降低,血浆和胰腺分泌PLA2活性也降低。总之,OKY-046处理组的PLA2活性和TxA2产生水平均降低,存活率提高,而OP-2507对ANP无影响。 TxA2和两种PLA2活性在急性胰腺炎加重过程中起重要作用。

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