Crovetti G, Carabelli A, Berti E, Guizzardi M, Fossati S, De Filippo C, Bertani E
Photopheresis Department, St. A. Abate Hospital, Gallarate, Italy.
Int J Artif Organs. 2000 Jan;23(1):55-62.
Cutaneous T-cell lymphoma (CTCL) includes several lymphoproliferative disorders involving mature T-lymphocyte proliferation initially confined to the cutis. These affections, after variable periods, may progress to the blood, limph nodes and visceral organs. Mycosis fungoides (MF) is the most frequent form of CTCL and has an indolent clinical course. The therapy of CTCL depends on the stage of the disease and the patient's general conditions. For advanced cases it includes chemotherapy, retinoids, and interferon-alpha. Since 1987 extracorporeal photochemotherapy (ECP), a novel immunomodulatory approach based on apheresis and photoirradiation of leukocytes, has been successfully introduced for the treatment of advanced CTCL. It can prolong survival of patients with erythrodermic CTCL without significant side effects.
To review our five-year experience with ECP in CTCL.
Since June 1994, 33 CTCL patients have been recruited for ECP, using two different regimens: two procedures on two consecutive days at four-week intervals for six months, or at two-week intervals for three months with progressive tapering in the second three-month period for the more severe forms. Six patients received ECP with IFN-alpha. ECP was done using the photopheresis UVAR system and UVAR XTS (Therakos, West Chester, Pa) and always with 8-MOP liquid formulation injected directly into the buffy coat bag. Lymphocytes in peripheral blood were immunophenotypically characterized for each patient and every ECP session.
All patients tolerated ECP well, without significant side effects. Thirty patients are clinically evaluable (at least three ECP cycles). A favourable clinical response was obtained in 80.9% (16/21) of MF patients (complete response 33%, partial response 47.6%) and in 66% (6/9) of patients in the Sézary's syndrome phase (complete response 33.3%, partial response 33.3%). Five of the six patients given IFN-alpha as adjunctive therapy had a PR and one a CR. Four patients are in CR without therapy at follow-ups of 46, 20, 10 and 8 months. There have been no changes in the peripheral lymphocyte immunophenotype during the follow-up. In 19/30 patients the CD95 antigen, correlated with cellular apoptosis, was expressed and was frequently associated with a good clinical response.
In our experience ECP achieved favourable clinical responses in 73% of patients, in monotherapy or in combination with IFN-alpha, without significant side effects.
皮肤T细胞淋巴瘤(CTCL)包括几种淋巴增殖性疾病,涉及最初局限于皮肤的成熟T淋巴细胞增殖。这些病变在不同时期后可能进展至血液、淋巴结和内脏器官。蕈样肉芽肿(MF)是CTCL最常见的形式,临床病程进展缓慢。CTCL的治疗取决于疾病分期和患者的一般状况。对于晚期病例,治疗包括化疗、维甲酸和α干扰素。自1987年以来,体外光化学疗法(ECP)作为一种基于白细胞单采和光照射的新型免疫调节方法,已成功应用于晚期CTCL的治疗。它可以延长红皮病型CTCL患者的生存期,且无明显副作用。
回顾我们在CTCL中应用ECP的五年经验。
自1994年6月起,33例CTCL患者接受了ECP治疗,采用两种不同方案:连续两天进行两次治疗,每四周一次,共六个月;或每两周一次,共三个月,对于病情较重的患者,在后三个月逐渐减量。6例患者在接受ECP治疗时联合使用了α干扰素。使用光分离置换UVAR系统和UVAR XTS(Therakos公司,宾夕法尼亚州韦斯特切斯特)进行ECP治疗,始终将8-甲氧补骨脂素液体制剂直接注入血沉棕黄层袋中。对每位患者的每次ECP治疗,对外周血淋巴细胞进行免疫表型分析。
所有患者对ECP耐受性良好,无明显副作用。30例患者可进行临床评估(至少接受三个ECP周期治疗)。MF患者中有80.9%(16/21)获得了良好的临床反应(完全缓解率33%,部分缓解率47.6%),Sezary综合征期患者中有66%(6/9)获得了良好的临床反应(完全缓解率33.3%,部分缓解率33.3%)。6例联合使用α干扰素作为辅助治疗的患者中有5例部分缓解,1例完全缓解。4例患者在随访46、20、10和8个月时未经治疗处于完全缓解状态。随访期间外周淋巴细胞免疫表型无变化。19/30例患者表达了与细胞凋亡相关的CD95抗原,且常与良好的临床反应相关。
根据我们的经验,ECP在单药治疗或联合α干扰素治疗时,使73%的患者获得了良好的临床反应,且无明显副作用。
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