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一项I期临床研究中接受静脉注射苔藓抑素1的患者的免疫调节:与苔藓抑素1对体外淋巴细胞功能的影响比较

Immunomodulation in patients receiving intravenous Bryostatin 1 in a phase I clinical study: comparison with effects of Bryostatin 1 on lymphocyte function in vitro.

作者信息

Scheid C, Prendiville J, Jayson G, Crowther D, Fox B, Pettit G R, Stern P L

机构信息

Cancer Research Campaign Department of Immunology, Christie Hospital, Paterson Institute for Cancer Research, Manchester, UK.

出版信息

Cancer Immunol Immunother. 1994 Oct;39(4):223-30. doi: 10.1007/BF01525985.

Abstract

Bryostatin 1 is a protein kinase C activator that inhibits growth of tumour cells and activates lymphocytes in vitro, properties that have encouraged its use in phase 1 clinical studies as an anticancer agent. We investigated interleukin-2(IL-2)-induced proliferation and lymphokine-activated killer (LAK) cell activity in peripheral blood mononuclear cells (PBMC) from cancer patients receiving Bryostatin intravenously. After Bryostatin administration both LAK generation and proliferation were enhanced when patients' PBMC were stimulated with IL-2 in vitro. However, when normal donors' PBMC were cultured in vitro in the presence Bryostatin and IL-2, LAK induction was inhibited while IL-2-driven proliferation was increased. These effects were also seen following only 2 h exposure to Bryostatin and could be elicited by conditioned medium from Bryostatin-pretreated cells. Neither IL-4 nor interferon gamma was detected in the conditioned medium. Bryostatin in vitro was found to increase expression of IL-2 receptors on CD4+, CD8+ and CD56+ cells and augment the proportion of CD8+ cells in conjunction with IL-2. We conclude that Bryostatin in combination with IL-2 in vitro enhances proliferation and IL-2 receptor expression on lymphocytes, favouring CD8+ cells while suppressing the generation of LAK activity. Intravenous administration of Bryostatin increases the potential of IL-2 to induce proliferation and LAK activity in lymphocytes which, taken together with its putative direct antitumour effect, makes Bryostatin an interesting candidate for clinical trials in combination with IL-2.

摘要

苔藓抑素1是一种蛋白激酶C激活剂,在体外可抑制肿瘤细胞生长并激活淋巴细胞,这些特性促使其作为抗癌药物用于1期临床研究。我们研究了静脉注射苔藓抑素的癌症患者外周血单核细胞(PBMC)中白细胞介素-2(IL-2)诱导的增殖和淋巴因子激活的杀伤(LAK)细胞活性。给予苔藓抑素后,当患者的PBMC在体外受到IL-2刺激时,LAK细胞的生成和增殖均增强。然而,当正常供体的PBMC在苔藓抑素和IL-2存在的情况下进行体外培养时,LAK细胞的诱导受到抑制,而IL-2驱动的增殖增加。仅暴露于苔藓抑素2小时后也观察到了这些效应,并且可以由苔藓抑素预处理细胞的条件培养基引发。在条件培养基中未检测到IL-4和干扰素γ。发现体外苔藓抑素可增加CD4 +、CD8 +和CD56 +细胞上IL-2受体的表达,并与IL-2一起增加CD8 +细胞的比例。我们得出结论,体外苔藓抑素与IL-2联合可增强淋巴细胞的增殖和IL-2受体表达,有利于CD8 +细胞,同时抑制LAK细胞活性的产生。静脉注射苔藓抑素可增加IL-2诱导淋巴细胞增殖和LAK细胞活性的潜力,再加上其假定的直接抗肿瘤作用,使得苔藓抑素成为与IL-2联合进行临床试验的一个有吸引力的候选药物。

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