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结直肠癌患者中白细胞介素-2激活的杀伤细胞活性:胸腺素α1对其体外作用的评估

Interleukin-2-activated killer cell activity in colorectal tumor patients: evaluation of in vitro effects by prothymosin alpha1.

作者信息

Eckert K, Grünberg E, Immenschuh P, Garbin F, Kreuser E D, Maurer H R

机构信息

Institut für Pharmazie der Freien Universität Berlin, Germany.

出版信息

J Cancer Res Clin Oncol. 1997;123(8):420-8. doi: 10.1007/BF01372545.

Abstract

The effects of prothymosin alpha1 (Pro alpha1) in combination with interleukin-2 (IL-2) on peripheral blood lymphocytes from 50 colorectal tumor patients at different stages were studied with respect to immunocytotoxicity, adhesion to cultured SW620 colon carcinoma cells, secretion of cytokines and expression of adhesion and surface marker molecules. On average, the patients showed lower natural killer (NK) cell activity than healthy donors, which was associated with a lower adhesion capacity to the tumor target cells. The NK cell activity of the patients was inversely related to the tumor stage. The generation of lymphokine(IL-2)-activated killer (LAK) cell activity was found to be comparable on lymphocytes from healthy individuals and patients and was not correlated to tumor stage. Pro alpha1 stimulated patients' LAK cell activity only, primarily at the early stage (Dukes A/B). The Pro alpha1 effect was associated with an increased adhesion of lymphocytes to tumor target cells and an increased secretion of the deficient IL-2-induced IFN gamma secretion. No significant effects on the low level of TNF alpha secretion was noted. By flow cytometry, Pro alpha1 in combination with IL-2 augmented the expression of the NK cell markers CD56, CD16/56, the subset CD3/16/56 and CD25 on lymphocytes of the patients. In contrast, Pro alpha1 was equally effective by increasing the expression of CD18 and CD11a on lymphocytes from the patients and from normal controls. In conclusion, Pro alpha1, in combination with IL-2, can partially normalize lymphocyte deficiencies of colon cancer patients in vitro. This potential might provide an experimental basis for applying Pro alpha1 or related thymic peptides in selected immunotherapies against colorectal tumors.

摘要

研究了胸腺素α1(Pro α1)与白细胞介素-2(IL-2)联合应用对50例不同分期结直肠癌患者外周血淋巴细胞免疫细胞毒性、与培养的SW620结肠癌细胞的黏附、细胞因子分泌以及黏附分子和表面标志物分子表达的影响。平均而言,患者的自然杀伤(NK)细胞活性低于健康供体,这与对肿瘤靶细胞的较低黏附能力相关。患者的NK细胞活性与肿瘤分期呈负相关。发现健康个体和患者淋巴细胞上淋巴因子(IL-2)激活的杀伤(LAK)细胞活性的产生相当,且与肿瘤分期无关。Pro α1仅刺激患者的LAK细胞活性,主要在早期(杜克A/B期)。Pro α1的作用与淋巴细胞对肿瘤靶细胞黏附增加以及IL-2诱导的干扰素γ分泌不足的分泌增加有关。未观察到对低水平肿瘤坏死因子α分泌的显著影响。通过流式细胞术,Pro α1与IL-2联合增强了患者淋巴细胞上NK细胞标志物CD56、CD16/56、亚群CD3/16/56和CD25的表达。相反,Pro α1通过增加患者和正常对照淋巴细胞上CD18和CD11a的表达同样有效。总之,Pro α1与IL-2联合应用可在体外部分使结肠癌患者的淋巴细胞缺陷正常化。这种潜力可能为在针对结直肠癌的选定免疫治疗中应用Pro α1或相关胸腺肽提供实验依据。

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