Liu Xin, Xiong Ling, Xu Rui, Cao Xicai
Department of Radiology, Tianjin Medical University General Hospital, Tianjin 300052, China.
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Zhonghua Zhong Liu Za Zhi. 2015 Feb;37(2):91-4.
To explore the advantages, feasibility and limitations of hepatic arterial infusion under temporary hepatic circulation occlusion.
Twelve rabbits were randomly divided into two groups: hepatic artery infusion group (HAI group) and hepatic artery infusion under temporary hepatic circulation occlusion group (HAI-THCO). Microcatheters were separately inserted into the proper hepatic artery and right hepatic vein. For the HAI group, 5-Fu (10 mg/ml and 100 mg/kg) was infused into the common hepatic artery with a high pressure injector for 10 minutes. For the HAI-THCO group, the common hepatic artery and hepatic portal vein were temporarily occluded for 15 minutes using artery clamp when 5-Fu was being infused. For the two groups, at 2, 5, 10, 15, 20 and 30 min after the start of infusion, blood samples of the hepatic flow were collected from the right hepatic vein and of the systemic blood flow from the inferior vena cava, 1 ml at each time point. The blood drug concentration of these blood samples was determined by high performance liquid chromatography (HPLC).
Except that at 20 and 30 min after infusion, in the HAI group, the blood drug concentration of hepatic circulation was significantly higher than that of systemic circulation (P < 0.05). But in the HAI-THCO group, the blood drug concentration of hepatic circulation was significantly higher than that of systemic circulation at all the time points (P < 0.05). The hepatic circulation blood drug level of the HAI-THCO group was always significantly higher than that of the HAI group (P < 0.05), but the systemic circulation blood drug concentration of the HAI-THCO group was always lower (P < 0.05). The hepatic circulation maximum concentration (Cmax) of blood drug concentration of the HAI-THCO and HAI groups was (23.057±3.270) µg/ml and (4.408±1.092) µg/ml, respectively, and the Cmax of HAI-THCO group was significantly higher (P < 0.001), being 5.23 times of that of HAI group. The systemic circulation Cmax of the two groups was (1.456±0.217) µg/ml and (2.335±0.669) µg/ml, respectively, and the Cmax of HAI group was 1.60 times higher than that of the HAI-THCO group (P = 0.022). The hepatic circulation AUC of HAI-THCO and HAI groups was (368.927±52.416) µg·min·ml(-1) and (65.630±14.928) µg·min·ml(-1), respectively. The AUC of HAI-THCO group was 5.62 times higher than that of the HAI group (P < 0.001). The systemic circulation AUC of the two groups was (27.193±3.948) µg·min·ml(-1) and (45.301±12.275) µg·min·ml(-1), respectively. The AUC of HAI group was 1.67 times higher than that of the HAI-THCO group (P = 0.014).
HAI-THCO is a simple and effective regional hepatic infusion chemotherapy technique. It can be performed through occluding the common hepatic artery and the hepatic portal vein by balloon catheter. HAI-THCO can not only increase the blood drug concentration in the hepatic circulation, but also decrease the blood drug concentration in the systemic circulation, therefore, distinctly lowering the systemic toxicity.
探讨暂时性肝循环阻断下肝动脉灌注的优势、可行性及局限性。
将12只家兔随机分为两组:肝动脉灌注组(HAI组)和暂时性肝循环阻断下肝动脉灌注组(HAI-THCO组)。将微导管分别插入肝固有动脉和右肝静脉。HAI组用高压注射器将5-氟尿嘧啶(10mg/ml,100mg/kg)注入肝总动脉10分钟。HAI-THCO组在注入5-氟尿嘧啶时用动脉夹暂时阻断肝总动脉和肝门静脉15分钟。两组在开始灌注后2、5、10、15、20和30分钟,从右肝静脉采集肝血流血样,从下腔静脉采集体循环血样,每个时间点采集1ml。采用高效液相色谱法(HPLC)测定这些血样的血药浓度。
除灌注后20和30分钟外,HAI组肝循环血药浓度显著高于体循环(P<0.05)。但HAI-THCO组在所有时间点肝循环血药浓度均显著高于体循环(P<0.05)。HAI-THCO组肝循环血药水平始终显著高于HAI组(P<0.05),但HAI-THCO组体循环血药浓度始终较低(P<0.05)。HAI-THCO组和HAI组血药浓度的肝循环最大浓度(Cmax)分别为(23.057±3.270)μg/ml和(4.408±1.092)μg/ml,HAI-THCO组Cmax显著更高(P<0.001),是HAI组的5.23倍。两组体循环Cmax分别为(1.456±0.217)μg/ml和(2.335±0.669)μg/ml,HAI组Cmax比HAI-THCO组高1.60倍(P=0.022)。HAI-THCO组和HAI组肝循环曲线下面积(AUC)分别为(368.927±52.416)μg·min·ml⁻¹和(65.630±14.928)μg·min·ml⁻¹。HAI-THCO组AUC比HAI组高5.62倍(P<0.001)。两组体循环AUC分别为(27.193±3.948)μg·min·ml⁻¹和(45.301±12.275)μg·min·ml⁻¹。HAI组AUC比HAI-THCO组高1.67倍(P=0.014)。
HAI-THCO是一种简单有效的区域性肝灌注化疗技术。可通过球囊导管阻断肝总动脉和肝门静脉来实施。HAI-THCO不仅能提高肝循环中的血药浓度,还能降低体循环中的血药浓度,从而明显降低全身毒性。
