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在猪身上进行的单独肝灌注实验,使用了肿瘤坏死因子-α(TNF-α),分别在有和没有美法仑的情况下。

Isolated hepatic perfusion in the pig with TNF-alpha with and without melphalan.

作者信息

Borel Rinkes I H, de Vries M R, Jonker A M, Swaak T J, Hack C E, Nooyen P T, Wiggers T, Eggermont A M

机构信息

Department of Surgical Oncology, Rotterdam Cancer Institute/University Hospital Rotterdam, The Netherlands.

出版信息

Br J Cancer. 1997;75(10):1447-53. doi: 10.1038/bjc.1997.248.

Abstract

Isolated limb perfusion with tumour necrosis factor alpha (TNF-alpha) and melphalan is well tolerated and highly effective in irresectable sarcoma and melanoma. No data are available on isolated hepatic perfusion (IHP) with these drugs for irresectable hepatic malignancies. This study was undertaken to assess the feasibility of such an approach by analysing hepatic and systemic toxicity of IHP with TNF-alpha with and without melphalan in pigs. Ten healthy pigs underwent IHP. After vascular isolation of the liver, inflow catheters were placed in the hepatic artery and portal vein, and an outflow catheter was placed in the inferior vena cava (IVC). An extracorporeal veno-venous bypass was used to shunt blood from the lower body and intestines to the heart. The liver was perfused for 60 min with (1) 50 microg kg(-1) TNF-alpha (n = 5), (2) 50 microg kg(-1) TNF-alpha plus 1 mg kg(-1) melphalan (n = 3) or (3) no drugs (n = 2). The liver was washed with macrodex before restoring vascular continuity. All but one pigs tolerated the procedure well. Stable perfusion was achieved in all animals with median perfusate TNF-alpha levels of 5.1 +/- 0.78 x 10(6) pg ml(-1) (+/- s.e.m). Systemic leakage of TNF-alpha from the perfusate was consistently < 0.02%. Following IHP, a transient elevation of systemic TNF-alpha levels was observed in groups 1 and 2 with a median peak level of 23 +/- 3 x 10(3) pg ml(-1) at 10 min after washout, which normalized within 6 h. No significant systemic toxicity was observed. Mild transient hepatotoxicity was seen to a similar extent in all animals, including controls. IHP with TNF-alpha with(out) melphalan in pigs is technically feasible, results in minimal systemic drug exposure and causes minor transient disturbances of liver biochemistry and histology.

摘要

用肿瘤坏死因子α(TNF-α)和美法仑进行孤立肢体灌注对不可切除的肉瘤和黑色素瘤耐受性良好且疗效显著。目前尚无关于用这些药物对不可切除的肝脏恶性肿瘤进行孤立肝灌注(IHP)的数据。本研究旨在通过分析在猪身上进行含或不含美法仑的TNF-α肝灌注的肝脏和全身毒性,评估这种方法的可行性。十只健康猪接受了IHP。在肝脏血管隔离后,将流入导管置于肝动脉和门静脉中,并将流出导管置于下腔静脉(IVC)中。使用体外静脉-静脉旁路将下半身和肠道的血液分流至心脏。肝脏用以下溶液灌注60分钟:(1)50微克/千克(-1)TNF-α(n = 5),(2)50微克/千克(-1)TNF-α加1毫克/千克(-1)美法仑(n = 3)或(3)无药物(n = 2)。在恢复血管连续性之前,用大分子右旋糖酐冲洗肝脏。除一只猪外,所有猪对该手术耐受性良好。所有动物均实现了稳定灌注,灌注液中TNF-α的中位数水平为5.1±0.78×10(6)皮克/毫升(±标准误)。灌注液中TNF-α的全身泄漏始终<0.02%。IHP后,第1组和第2组观察到全身TNF-α水平短暂升高,冲洗后10分钟时的中位数峰值水平为23±3×10(3)皮克/毫升,6小时内恢复正常。未观察到明显的全身毒性。在所有动物(包括对照组)中均观察到程度相似的轻度短暂肝毒性。在猪身上用含(或不含)美法仑的TNF-α进行IHP在技术上是可行的,全身药物暴露最小,并导致肝脏生化和组织学的轻微短暂干扰。

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