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重组人干扰素γ治疗系统性硬化症患者的多中心试验:对皮肤纤维化和白细胞介素2受体水平的影响。

A multicenter trial of recombinant human interferon gamma in patients with systemic sclerosis: effects on cutaneous fibrosis and interleukin 2 receptor levels.

作者信息

Polisson R P, Gilkeson G S, Pyun E H, Pisetsky D S, Smith E A, Simon L S

机构信息

Arthritis Unit, Massachusetts General Hospital, Harvard Medical School, Boston 02114, USA.

出版信息

J Rheumatol. 1996 Apr;23(4):654-8.

PMID:8730122
Abstract

OBJECTIVE

To evaluate the acute toxicity, potential efficacy, and effects on the soluble interleukin 2 receptor (sIL-2R) of recombinant human interferon gamma (rIFN-gamma) in patients with systemic sclerosis (SSc).

METHODS

A multicentered, pilot clinical trial of rIFN-gamma was performed on 20 patients (15 women, 5 men, mean age 45 years) with active cutaneous SSc (mean disease duration 36 months) to evaluate it potential as a novel therapy for this untreatable disorder. After one week of rIFN-gamma 0.01 mg/m2/day, subjects self-administered rIFN-gamma 0.1 mg/m2/day intramuscularly for a total of 18 weeks. The major outcome variable was a modified skin score (0 = normal skin, 3 = hidebound skin) measured and summed from 15 anatomic areas of the body. sIL-2R levels were measured by ELISA at entry and exit from the study.

RESULTS

The clinical results were modest at best. Nine of 20 patients achieved at least a 20% reduction in skin score, with one patient showing almost total remission of all skin abnormalities. The mean skin score at entry for all subjects was 22.8 +/- 8.9 and over the course of the trial improved marginally compared to baseline (mean change -4.72 +/- 6.62; p = 0.008). However, 8 subjects did not change appreciably while in the trial. Antibodies to Scl-70 were observed in only 5 patients (all with diffuse scleroderma) and were not associated with either response to or complications from therapy. The adverse reactions were frequent and occasionally severe. Ten subjects were withdrawn because of exacerbation of Raynaud's symptoms (n = 5), constitutional symptoms (n = 2), development of renal crises (n = 2), and mild pancytopenia (n = 1). Minor laboratory abnormalities were common and included elevation of cholesterol, triglycerides, hepatic transaminases, and reduction in white blood cell count. Compared to controls, mean sIL-2R was markedly elevated at entry (1309 +/- 495 U/ml; p = 0.0001) and did not change appreciably at exit. Spearman correlation analysis showed a trend but no statistically significant association of skin score with sIL-2R (R = 0.408; p = 0.074). However, sIL-2R was significantly correlated with erythrocyte sedimentation rate (R = 0.542; p = 0.0165). A subset analysis revealed that skin score (p = 0.0001) and sIL-2R (p = 0.00170) were significantly higher at baseline for patients with diffuse scleroderma compared to patients with limited disease.

CONCLUSION

rIFN-gamma may be beneficial for some patients with SSc, but the benefit appears marginal for most individuals and the side effects frequent. Although sIL-2R was elevated in many of the patients with SSc, it did not appear to be correlated with activity of cutaneous disease or response to therapy.

摘要

目的

评估重组人干扰素γ(rIFN-γ)对系统性硬化症(SSc)患者的急性毒性、潜在疗效以及对可溶性白细胞介素2受体(sIL-2R)的影响。

方法

对20例(15例女性,5例男性,平均年龄45岁)活动性皮肤型SSc(平均病程36个月)患者进行了一项rIFN-γ的多中心、试点临床试验,以评估其作为这种无法治愈疾病的新型治疗方法的潜力。在给予0.01mg/m²/天的rIFN-γ一周后,受试者自行肌肉注射0.1mg/m²/天的rIFN-γ,共18周。主要结局变量是改良皮肤评分(0 = 正常皮肤,3 = 硬皮样皮肤),该评分是对身体15个解剖区域进行测量并求和得到的。在研究入组时和结束时通过酶联免疫吸附测定(ELISA)测量sIL-2R水平。

结果

临床结果充其量只能说是一般。20例患者中有9例皮肤评分至少降低了20%,其中1例患者几乎所有皮肤异常都完全缓解。所有受试者入组时的平均皮肤评分为22.8±8.9,在试验过程中与基线相比仅有轻微改善(平均变化-4.72±6.62;p = 0.008)。然而,8例受试者在试验期间没有明显变化。仅在5例患者(均为弥漫性硬皮病)中观察到抗Scl-70抗体,且与治疗反应或并发症均无关。不良反应频繁,偶尔较为严重。10例受试者因雷诺症状加重(n = 5)、全身症状(n = 2)、出现肾危象(n = 2)和轻度全血细胞减少(n = 1)而退出。轻微的实验室异常很常见,包括胆固醇、甘油三酯、肝转氨酶升高以及白细胞计数降低。与对照组相比,入组时平均sIL-2R显著升高(1309±495 U/ml;p = 0.0001),结束时没有明显变化。Spearman相关性分析显示有趋势但皮肤评分与sIL-2R无统计学显著关联(R = 0.408;p = 0.074)。然而,sIL-与红细胞沉降率显著相关(R = 0.542;p = 0.0165)。亚组分析显示,与局限性疾病患者相比,弥漫性硬皮病患者基线时的皮肤评分(p = 0.0001)和sIL-2R(p = 0.00170)显著更高。

结论

rIFN-γ可能对某些SSc患者有益,但对大多数个体而言益处似乎不大,且副作用频繁。尽管许多SSc患者体内sIL-2R升高,但它似乎与皮肤疾病活动度或治疗反应无关。

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