肿瘤内治疗I:免疫治疗与转移性癌症永久长期治愈的关系

Max H. Cohen, A. Ketcham, R. Herberman
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引用次数: 0

摘要

我们在一项随机前瞻性研究中证明了肿瘤内(病灶内)二硝基氯苯(DNCB)与肿瘤内(病灶内)卡介苗(BCG)在治疗进展性转移性黑色素瘤方面的优势。转移性黑色素瘤以卫星状和/或途中转移的形式存在。我们现在证明了局灶内DNCB能够永久治愈一组具有相同临床标准的患者,并描述了他们的临床特征和治疗方案。所描述的治愈患者在其剩余的生命中被跟踪,长达30年,在免疫治疗后没有转移性癌症。她们都是女性,肿瘤内治疗开始时年龄在51到56岁之间。治疗是针对两例腿部进展性皮肤和皮下转移性疾病,另一例是针对迅速扩散的头皮和前额转移性疾病。在每个病例中,这种疾病都不是手术可以控制的。治疗持续6 ~ 26个月。随后,患者在无肿瘤的情况下存活了18年,在83岁时死亡;或者活了24年,89岁去世;或者30年,97岁去世。近年来,人们对晚期癌症的免疫治疗产生了极大的兴趣。本文报道的治愈患者无全身性毒性,这为考虑将肿瘤内治疗与目前有效但全身性毒性更大的免疫治疗方法结合起来治疗某些转移性癌症提供了基础。瘤内治疗可能特别适用于具有皮肤转移的不可控黑色素瘤,如当前报告中所述,没有远处扩散的证据。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Intratumoral Therapy I: Association of Immunotherapy with Permanent Long Term Cure of Metastatic Cancer
We have demonstrated in a randomized prospective study the superiority of intratumoral (intralesional) dinitrochlorobenzene (DNCB) compared to intratumoral (intralesional) bacillus Calmette-Guerin (BCG) in the treatment of progressive metastatic melanoma. The metastatic melanoma was in the form of satellitosis and/or in-transit metastases. We now demonstrate the ability of intralesional DNCB to permanently cure a selected group of patients with the same clinical criteria, and describe their clinical characteristics and treatment regimens. The described cured patients were followed for their remaining lifetimes, for up to 30 years, after being immunotherapeutically rendered free of metastatic cancer. They were each female, between the ages of 51 and 56 when intratumoral treatments were begun. Treatment was for progressive cutaneous and subcutaneous metastatic disease in the leg in two cases and for rapidly spreading scalp and forehead metastases in another. In each case the disease was not surgically controllable. Treatments were continued for 6 to 26 months. Subsequently the patients survived tumor free for either 18 years, dying at age 83; or for 24 years, dying at age 89; or for 30 years, dying at age 97. There has been a significant interest in recent years in immunotherapy for advanced cancer. The absence of systemic toxicity in the cured patients reported herein provides a basis for consideration of combining intratumoral treatments with current effective but systemically more toxic immunotherapeutic approaches to some metastatic cancers. Intratumoral treatments may be particularly applicable in cases of uncontrollable melanoma with cutaneous metastases, without evidence of distant spread, as in the current report.
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