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用血栓素合酶抑制剂预防实验性肝转移

Prevention of experimental hepatic metastasis with thromboxane synthase inhibitor.

作者信息

Yokoyama I, Hayashi S, Kobayashi T, Negita M, Yasutomi M, Uchida K, Takagi H

机构信息

Department of Surgery II, School of Medicine, Nagoya University, Japan.

出版信息

Res Exp Med (Berl). 1995;195(4):209-15. doi: 10.1007/BF02576790.

DOI:10.1007/BF02576790
PMID:8525071
Abstract

To investigate the effectiveness of thromboxane (Tx) synthase inhibitor in the prevention of experimental hepatic metastasis, an in vivo study was designed. Hepatic metastasis was brought about by injection of 1 x 10(5) cells of colon 38 tumor into the portal vein of C57 B1/65 mice. Seven groups (n = 16 in each group) received different treatments: with TxA2 synthase inhibitor (sodium ozagrel), 5, 10 or 15 mg/kg BW before tumor inoculation, and daily for the following 3 days, (groups A, B and C, respectively); with acetyl salicylic acid (aspirin), 1.0, 1.5 or 2.0 mg/kg BW (groups C, D, and E, respectively); a control group, inoculated with vehicle only. Serum TxB2, a stable metabolite of TxA2, and prostaglandin F1 alpha were measured. Labeling index for tumor proliferation by bromodeoxy-uridine radioimmuno-assay was also studied. Incidence of metastasis in groups A (60.5%), B (49.5%), C (43.0%), D (80.5%), E (66.0%) and F (58.4%) was less than that in the control group (100%). Tumor size, number of labeling index did not differ among the groups. Serum TxB2 (pg/ml) levels were significantly lower in all of the groups than in the control. Serum PGF1 alpha levels in the groups with aspirin were lower than those in sodium ozagrel. Tx synthase inhibitor is effective in the prevention of experimental hepatic metastasis when it is given before and immediately after tumor inoculation. As Tx synthase inhibitor leaves metabolic pathway to PGI2 production intact, it is more effective in the prevention of metastasis than aspirin since aspirin inhibits both thromboxane and PGI2.

摘要

为研究血栓素(Tx)合酶抑制剂在预防实验性肝转移中的效果,设计了一项体内研究。通过将1×10⁵个结肠38肿瘤细胞注射到C57 B1/65小鼠的门静脉中来诱导肝转移。七组(每组n = 16)接受不同治疗:在肿瘤接种前给予血栓素A₂合酶抑制剂(奥扎格雷钠),剂量为5、10或15 mg/kg体重,并在随后3天每日给药(分别为A、B和C组);给予乙酰水杨酸(阿司匹林),剂量为1.0、1.5或2.0 mg/kg体重(分别为C、D和E组);一个对照组,仅接种赋形剂。检测血清TxB₂(血栓素A₂的稳定代谢产物)和前列腺素F1α。还通过溴脱氧尿苷放射免疫测定法研究肿瘤增殖的标记指数。A组(60.5%)、B组(49.5%)、C组(43.0%)、D组(80.5%)、E组(66.0%)和F组(58.4%)的转移发生率低于对照组(100%)。各组之间肿瘤大小、标记指数数量无差异。所有组的血清TxB₂(pg/ml)水平均显著低于对照组。使用阿司匹林的组血清PGF1α水平低于使用奥扎格雷钠的组。Tx合酶抑制剂在肿瘤接种前和接种后立即给药时对预防实验性肝转移有效。由于Tx合酶抑制剂使PGI₂产生的代谢途径保持完整,因此它在预防转移方面比阿司匹林更有效,因为阿司匹林同时抑制血栓素和PGI₂。

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