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84%肝切除术后犬的病理生理学,重点关注前列腺素代谢产物以及血栓素A2合成抑制剂和前列腺素I2类似物的作用。

Pathophysiology of dogs after 84% hepatectomy with emphasis on prostaglandin metabolites and the effect of a thromboxane A2 synthesis inhibitor and a prostaglandin I2 analog.

作者信息

Iwata M

机构信息

First Department of Surgery, Mie University School of Medicine, Japan.

出版信息

Surg Today. 1994;24(12):1056-67. doi: 10.1007/BF01367456.

Abstract

The pathophysiological conditions following 84% hepatectomy were examined in terms of the changes in thromboxane A2 (TxA2) and prostaglandin I2 (PGI2) in a canine model. OKY-046, a TxA2 inhibitor, and OP-2507, a PGI2 analog, were administered to evaluate the possibility of extending hepatic resection. The 2-week survival rate following 84% hepatectomy significantly improved after the administration of OKY-046 and OP-2507, from 12.5% to 58.3% and 75.0%, respectively. Furthermore, OP-2507 significantly improved impaired hepatocyte and sinusoidal endothelial cell function after 84% hepatectomy, resulting in a satisfactory recovery to the preoperative levels. Within 24 h after 84% hepatectomy, the plasma levels of thromboxane B2 (TxB2) increased significantly, and the 6-keto-prostaglandin F1 alpha (6-KF) levels became slightly elevated. OKY-046 and OP-2507 decreased TxB2 and increased 6-KF in the plasma, resulting in the maintenance of sufficient blood flow in the portal vein and hepatic tissue and the mitigation of microcirculatory disorders. Moreover, the cytoprotective effects of the two drugs inhibited functional impairment of the residual liver. In conclusion, abnormal prostaglandin metabolites were produced after 84% hepatectomy, being involved in residual liver disorders. However, the administration of either an inhibitor of TxA2 synthesis or a PGI2 analog ameliorated the functional impairment of the residual liver, which suggests their potential value for extending the resectability of the liver from what is presently feasible.

摘要

在犬类模型中,根据血栓素A2(TxA2)和前列腺素I2(PGI2)的变化,对84%肝切除术后的病理生理状况进行了研究。给予TxA2抑制剂OKY-046和PGI2类似物OP-2507,以评估扩大肝切除术的可能性。在给予OKY-046和OP-2507后,84%肝切除术后的2周生存率显著提高,分别从12.5%提高到58.3%和75.0%。此外,OP-2507显著改善了84%肝切除术后受损的肝细胞和肝窦内皮细胞功能,使其恢复到术前水平且效果良好。84%肝切除术后24小时内,血浆血栓素B2(TxB2)水平显著升高,6-酮-前列腺素F1α(6-KF)水平略有升高。OKY-046和OP-2507降低了血浆中的TxB2并提高了6-KF水平,从而维持了门静脉和肝组织的充足血流,并减轻了微循环障碍。此外,这两种药物的细胞保护作用抑制了残余肝脏的功能损害。总之,84%肝切除术后产生了异常的前列腺素代谢产物,参与了残余肝脏疾病的发生。然而,给予TxA2合成抑制剂或PGI2类似物可改善残余肝脏的功能损害,这表明它们在扩大目前可行的肝脏可切除性方面具有潜在价值。

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