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[低度恶性非霍奇金淋巴瘤——治疗现状与趋势]

[Low-grade malignant non-Hodgkin lymphomas--current status and trends in therapy].

作者信息

Hiddemann W

机构信息

Abteilung Hämatologie und Onkologie, Medizinische Universitätsklinik, Georg-August-Universität, Göttingen.

出版信息

Ther Umsch. 1996 Feb;53(2):123-32.

PMID:8629262
Abstract

Low-grade Non-Hodgkin Lymphomas [NHL] comprise a heterogenous group of disorders both in terms of their cellular and histological composition as in terms of their clinical course. The currently mostly applied classification systems, the Working Formulation and the Kiel Classification as well as the recently proposed Revised European American Lymphoma Classification, discriminate between low-, intermediate and high-grade subtypes. Low-grade NHL are characterized by a low to moderate proliferative activity and a long clinical course with median survival times ranging for approximately three years for centrocytic [CC] or mantle cell lymphomas [MCL] to five to eight years for centroblastic centrocytic [CB-CC] or follicular lymphomas [FL]. Recent cytogenetic and molecular biologic analyses indicate that these differences may result from distinct genetic abnormalities such as the translocation t [14; 18] which is frequently observed in FL-NHL and is associated with a bcl 2 overexpression, or the deregulation of the PRAD 1 in MCL-NHL induced by the translocation t [11; 14]. Therapy of low-grade lymphomas depends mainly on the extend of the disease. In the early stages I and II, at which approximately 15-20% of low-grade NHL are diagnosed, an extended field or a total nodal radiotherapy may be applied with curative intention. The treatment of patients with more advanced stages III and IV is controversial. The currently available information justifies a conservative approach by observing the natural course of the disease until therapeutic intervention is required due to the occurrence of B-symptoms, hematopoietic insufficient or lymphoma progression. Intensive chemotherapy seems not to translate into an improved disease-free or overall survival and can, therefore, not be recommended for first-line treatment. The most recent data of the German Low-Grade Lymphoma Study Group indicate, however, that after successful initial cytoreductive therapy maintenance treatment with interferon-alpha prolongs the disease-free interval and possibly also overall survival. New perspectives have arisen from the introduction of novel cytostatic agents such as purine analogues and the development of immunotoxins and antibody conjugated radioisotopes. Most promising at the present time appears the application of myelo-ablative radiochemotherapy followed by autologous peripheral blood stem cell transplantation which may provide a curative approach even for advanced stages of the disease.

摘要

低度非霍奇金淋巴瘤(NHL)在细胞和组织学构成以及临床病程方面均包含一组异质性疾病。当前应用最广泛的分类系统,即工作分类法、基尔分类法以及最近提出的修订欧美淋巴瘤分类法,区分了低、中、高度亚型。低度NHL的特征是增殖活性低至中等,临床病程长,中心细胞性(CC)或套细胞淋巴瘤(MCL)的中位生存时间约为3年,中心母细胞中心细胞性(CB-CC)或滤泡性淋巴瘤(FL)的中位生存时间为5至8年。最近的细胞遗传学和分子生物学分析表明,这些差异可能源于不同的基因异常,例如在FL-NHL中经常观察到的t(14;18)易位,其与bcl 2过表达相关,或者在MCL-NHL中由t(11;14)易位诱导的PRAD 1失调。低度淋巴瘤的治疗主要取决于疾病的范围。在I期和II期早期,约15%-20%的低度NHL在此阶段被诊断出来,可采用扩大野或全淋巴结放疗,目的是治愈。对III期和IV期更晚期患者的治疗存在争议。目前可得的信息支持一种保守方法,即观察疾病的自然病程直到因出现B症状、造血功能不足或淋巴瘤进展而需要进行治疗干预。强化化疗似乎并不能转化为无病生存期或总生存期的改善,因此不推荐用于一线治疗。然而,德国低度淋巴瘤研究组的最新数据表明,在成功进行初始细胞减灭治疗后,用α干扰素进行维持治疗可延长无病间期,也可能延长总生存期。新型细胞毒药物如嘌呤类似物的引入以及免疫毒素和抗体偶联放射性同位素的开发带来了新的前景。目前最有前景的似乎是应用清髓性放化疗,随后进行自体外周血干细胞移植,这甚至可能为疾病晚期提供一种治愈方法。

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