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氯胺酮、硫喷妥钠和氟烷对自然杀伤细胞活性的抑制及对肿瘤转移的促进作用,而丙泊酚无此作用:介导机制及预防措施

Suppression of natural killer cell activity and promotion of tumor metastasis by ketamine, thiopental, and halothane, but not by propofol: mediating mechanisms and prophylactic measures.

作者信息

Melamed Rivka, Bar-Yosef Shahar, Shakhar Guy, Shakhar Keren, Ben-Eliyahu Shamgar

机构信息

*Neuroimmunology Research Unit, Department of Psychology, Tel Aviv University, Tel Aviv, Israel; and †Department of Anesthesiology, Rabin Medical Center-Beilinson Campus, Petach Tikva, affiliated with the Sackler School of Medicine, Tel Aviv University, Tel Aviv, Israel.

出版信息

Anesth Analg. 2003 Nov;97(5):1331-1339. doi: 10.1213/01.ANE.0000082995.44040.07.

Abstract

UNLABELLED

Postoperative immunosuppression is partly ascribed to anesthesia and has been suggested to compromise patients' resistance to infection and tumor metastasis. We compared the effects of various anesthetics on natural killer (NK) cell activity and on resistance to experimental metastasis, and studied mediating mechanisms and prophylactic measures. Fischer 344 rats served as controls or were anesthetized for 1 h with ketamine, thiopental, halothane, or propofol. Anesthetized rats were either maintained in normothermia or left to spontaneously reach 33 degrees C-35 degrees C. Rats were then injected IV with MADB106 tumor cells, and 24 h later lung tumor retention was assessed, or 3 wk later, lung metastases were counted. Additionally, the number and activity of circulating NK cells were assessed after anesthesia. All anesthetics, except propofol, significantly reduced NK activity and increased MADB106 lung tumor retention or lung metastases. Hypothermia had no significant effects. Ketamine increased metastasis most potently, and this effect was markedly reduced in rats pretreated with a beta-adrenergic antagonist (nadolol) or with chronic small doses of an immunostimulator (polyriboinosinic:polyribocytidylic acid). Overall, the marked variation in the NK-suppressive effects of anesthetics seems to underlie their differential promotion of MADB106 metastasis. Prophylactic measures may include perioperative immunostimulation and the use of beta-blockers.

IMPLICATIONS

This study in a rat model of pulmonary metastasis demonstrates that some anesthetics, but not others, increase susceptibility to tumor metastasis, apparently by suppressing natural killer cell activity. Ketamine was most deleterious, and its effects were prevented by peripheral blockade of beta-adrenoceptors combined with low levels of immunostimulation.

摘要

未标记

术后免疫抑制部分归因于麻醉,并且有人认为这会削弱患者对感染和肿瘤转移的抵抗力。我们比较了各种麻醉剂对自然杀伤(NK)细胞活性和对实验性转移抵抗力的影响,并研究了介导机制和预防措施。将Fischer 344大鼠作为对照,或用氯胺酮、硫喷妥钠、氟烷或丙泊酚麻醉1小时。麻醉后的大鼠要么维持正常体温,要么任其自发达到33℃-35℃。然后给大鼠静脉注射MADB106肿瘤细胞,24小时后评估肺部肿瘤滞留情况,或3周后计数肺转移灶数量。此外,在麻醉后评估循环NK细胞的数量和活性。除丙泊酚外,所有麻醉剂均显著降低NK活性,并增加MADB106肺部肿瘤滞留或肺转移。体温过低没有显著影响。氯胺酮最显著地增加转移,在用β-肾上腺素能拮抗剂(纳多洛尔)或慢性小剂量免疫刺激剂(聚肌苷酸:聚胞苷酸)预处理的大鼠中,这种作用明显减弱。总体而言,麻醉剂对NK的抑制作用存在显著差异似乎是其对MADB106转移促进作用不同的基础。预防措施可能包括围手术期免疫刺激和使用β受体阻滞剂。

启示

这项在大鼠肺转移模型中的研究表明,一些麻醉剂而非其他麻醉剂会增加对肿瘤转移的易感性,显然是通过抑制自然杀伤细胞活性。氯胺酮的危害最大,通过外周β-肾上腺素能受体阻滞联合低水平免疫刺激可预防其作用。

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