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咪喹莫特外用联合白细胞介素-2病灶内注射治疗恶性黑色素瘤可及转移灶的I/II期研究

Phase I/II study of topical imiquimod and intralesional interleukin-2 in the treatment of accessible metastases in malignant melanoma.

作者信息

Green D S, Bodman-Smith M D, Dalgleish A G, Fischer M D

机构信息

Department of Oncology, St George's University of London, Cranmer Terrace, London, UK.

出版信息

Br J Dermatol. 2007 Feb;156(2):337-45. doi: 10.1111/j.1365-2133.2006.07664.x.

Abstract

BACKGROUND

Patients with metastatic skin disease in malignant melanoma can be difficult to treat effectively, often requiring repeated treatments with different modalities in an attempt to control their disease. Treatment of nonsurgically resectable melanoma deposits is unsatisfactory, as they are often multiple and recurring. Anecdotal evidence from individual use of imiquimod in superficial metastases and intralesional interleukin (IL)-2 in subcutaneous deposits suggests that the combination may be more effective in bulky subcutaneous disease.

OBJECTIVES

To investigate the combination of topical imiquimod and, for selected lesions, intralesional IL-2, to treat a small cohort of patients with accessible melanoma metastases resistant to other treatments.

METHODS

Thirteen patients were recruited: all had evidence of multiple cutaneous and/or subcutaneous metastases. Imiquimod was applied to the metastases on a daily basis for 4 weeks, before the introduction of intralesional IL-2. This was injected up to three times a week, into selected lesions, with 0.1 mL injected per lesion at a concentration of 3.6 MIU mL(-1), a total of 1 mL being given at each session. The treated lesions were assessed individually at intervals of 3 months.

RESULTS

Thirteen patients were treated, with 10 being eligible for assessment. In total, 182 lesions were treated: 137 purely cutaneous lesions and 41 subcutaneous lesions. Overall, a clinical response was seen in 92 lesions (50.5%) with 74 (40.7%) of these being a complete response (CR) with 91% of the CRs being in the cutaneous lesions. New lesions did appear during the treatment course; however, patients with cutaneous disease experienced a marked slowing of the appearance of new cutaneous lesions. No cutaneous lesions that responded reappeared on cessation of treatment.

CONCLUSIONS

The combination of imiquimod and IL-2 is effective in controlling this mixed cutaneous and subcutaneous disease, and is well tolerated. Imiquimod alone is often enough to elicit a response in purely cutaneous lesions. The addition of intralesional IL-2 increases the response rates in subcutaneous lesions, and in otherwise refractory cutaneous lesions.

摘要

背景

恶性黑色素瘤伴转移性皮肤疾病的患者可能难以得到有效治疗,往往需要采用不同方式反复治疗以控制病情。对于无法通过手术切除的黑色素瘤病灶,治疗效果并不理想,因为这些病灶常常多发且易复发。个别使用咪喹莫特治疗浅表转移灶以及病灶内注射白细胞介素(IL)-2治疗皮下病灶的案例表明,联合使用这两种方法可能对体积较大的皮下疾病更为有效。

目的

研究外用咪喹莫特联合病灶内注射IL-2(针对部分病灶)治疗一小群对其他治疗方法耐药且有可触及的黑色素瘤转移灶患者的效果。

方法

招募了13名患者,所有患者均有多处皮肤和/或皮下转移的证据。在开始病灶内注射IL-2之前,每天在转移灶上涂抹咪喹莫特,持续4周。每周对选定的病灶注射IL-2多达3次,每个病灶注射0.1 mL,浓度为3.6 MIU/mL(-1),每次注射总量为1 mL。每隔3个月对治疗的病灶进行单独评估。

结果

13名患者接受了治疗,其中10名符合评估条件。总共治疗了182个病灶,其中137个为单纯皮肤病灶,41个为皮下病灶。总体而言,92个病灶(50.5%)出现了临床反应,其中74个(40.7%)为完全缓解(CR),91%的CR出现在皮肤病灶中。在治疗过程中确实出现了新的病灶;然而,患有皮肤疾病的患者新皮肤病灶的出现明显减缓。停止治疗后,有反应的皮肤病灶未再出现。

结论

咪喹莫特和IL-2联合使用可有效控制这种皮肤和皮下混合性疾病,且耐受性良好。单独使用咪喹莫特通常足以使单纯皮肤病灶产生反应。病灶内注射IL-2可提高皮下病灶以及其他难治性皮肤病灶的反应率。

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