Elsässer-Beile U, Kölble N, Grussenmeyer T, Wetterauer U, Schultze-Seemann W
Department of Urology, University of Freiburg, Germany.
Anticancer Res. 1998 May-Jun;18(3B):1883-90.
IFN-gamma production in whole blood cell cultures (WBCC), and TNF-receptor p75 (TNF-R-75) plasma levels were measured as two independent immunological parameters in a group of 67 untreated renal cell carcinoma (RCC) patients at different clinical stages, and 40 age matched healthy controls. In the blood cell cultures of the tumor patients the levels of IFN-gamma were significantly lower compared to the controls and the values decreased with increasing tumor mass. In contrast, TNF-R-75 plasma levels were significantly higher in the tumor patients and increased with tumor stage. Additionally serial assessments of these parameters were studied in another group of 15 patients with advanced RCC during treatment with IL-2, IFN-alpha and retinoic acid according to three different protocols in order to search for any correlation between the biological marker values and the clinical response to treatment. During each 5 day cycle of high dose IL-2/IFN-alpha combination therapy (protocol 1) IFN-gamma-levels in the WBCC were markedly decreased, whereas the plasma levels of TNF-R-75 were increased. During low dose, long-term continuous IFN-alpha/IL-2 administration (protocol 2) in two patients a clear increase of the ex vivo leukocyte IFN-gamma production was seen for the first 5 and 6 months of treatment, respectively, which could be correlated to stable disease for this time. When progression was diagnosed, IFN-gamma levels in the WBCC decreased. In the WBCC of the other four patients with progressive IFN-gamma levels were rather low throughout (< 10 ng/ml) and no clear changes were measured. During low does IFN-alpha and 13-cis-retinoic acid therapy in repetitive weekly cycles (protocol 3) two patients had stable disease for 6 and 14 months respectively. In the WBCC cultures of these patients IFN-gamma production was higher during stable than during progressive disease. The other two patients with tumor progression had a very low leukocyte IFN-gamma production and high plasma levels of TNF-R-75. It is concluded that IFN-gamma levels in WBCC and TNF-R-75 plasma levels may be useful parameters for the immunological monitoring of therapies with biological response modifiers. Low IFN-gamma values and high TNF-R-75 levels may be predictive of tumor progression and bad prognosis.
在一组67例处于不同临床阶段的未经治疗的肾细胞癌(RCC)患者以及40例年龄匹配的健康对照中,检测全血细胞培养物(WBCC)中的γ干扰素产生量以及血浆中肿瘤坏死因子受体p75(TNF-R-75)水平,将其作为两个独立的免疫学参数。在肿瘤患者的血细胞培养物中,γ干扰素水平相较于对照组显著降低,且该值随肿瘤肿块增大而下降。相反,肿瘤患者的TNF-R-75血浆水平显著更高,并随肿瘤分期增加。此外,在另一组15例晚期RCC患者中,根据三种不同方案在接受白细胞介素-2、α干扰素和视黄酸治疗期间对这些参数进行了连续评估,以寻找生物学标志物值与临床治疗反应之间的任何相关性。在高剂量白细胞介素-2/α干扰素联合治疗的每个5天周期(方案1)中,WBCC中的γ干扰素水平显著降低,而TNF-R-75的血浆水平升高。在低剂量、长期持续给予α干扰素/白细胞介素-2(方案2)时,两名患者在治疗的前5个月和6个月分别出现离体白细胞γ干扰素产生量明显增加,这可能与该时间段内的疾病稳定相关。当诊断为疾病进展时,WBCC中的γ干扰素水平下降。在另外四名疾病进展的患者中,WBCC中的γ干扰素水平始终相当低(<10 ng/ml),未检测到明显变化。在低剂量α干扰素和13-顺式视黄酸每周重复周期治疗(方案3)期间,两名患者分别有6个月和14个月的疾病稳定期。在这些患者的WBCC培养物中,稳定期的γ干扰素产生量高于疾病进展期。另外两名肿瘤进展患者的白细胞γ干扰素产生量非常低,而TNF-R-75血浆水平很高。结论是,WBCC中的γ干扰素水平和TNF-R-75血浆水平可能是用于生物反应调节剂治疗免疫监测的有用参数。低γ干扰素值和高TNF-R-75水平可能预示肿瘤进展和不良预后。
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