高剂量白细胞介素-2单独或联合淋巴因子激活的杀伤细胞治疗晚期癌症患者的前瞻性随机试验。

Prospective randomized trial of high-dose interleukin-2 alone or in conjunction with lymphokine-activated killer cells for the treatment of patients with advanced cancer.

作者信息

Rosenberg S A, Lotze M T, Yang J C, Topalian S L, Chang A E, Schwartzentruber D J, Aebersold P, Leitman S, Linehan W M, Seipp C A

机构信息

Division of Cancer Treatment, National Cancer Institute, Bethesda, Md 20892.

出版信息

J Natl Cancer Inst. 1993 Apr 21;85(8):622-32. doi: 10.1093/jnci/85.8.622.

DOI:10.1093/jnci/85.8.622

PMID:8468720

Abstract

BACKGROUND

Treatment using interleukin-2 (IL-2) alone or in conjunction with lymphokine-activated killer (LAK) cells has been shown to mediate disease regression in selected patients with advanced cancer.

PURPOSE

This prospective randomized trial was designed to determine whether the administration of LAK cells in conjunction with high-dose IL-2 alters response and survival rates, compared with those for IL-2 alone, in patients with advanced cancer.

METHODS

The 181 patients who had metastatic cancer that had failed to respond to standard therapy or who had disease for which no effective therapy existed received treatment with high-dose IL-2 alone or with LAK cells plus IL-2. Both treatment groups were to receive the same dose of IL-2 administered according to the same schedule. IL-2 doses were omitted depending on the tolerance of the patient. Of the 181 patients, 97 had renal cell cancer and 54 had melanoma.

RESULTS

Median potential follow-up was 63.2 months. There were 10 complete responses among the 85 assessable patients who received IL-2 plus LAK cells, compared with four among the 79 who received IL-2 alone. There were 14 and 12 partial responses, respectively. Complete response continues in seven patients at 50-66 months. The 36-month actuarial survival with IL-2 plus LAK cells was 31%, compared with 17% with IL-2 alone (two-sided P value [P2] = .089). A trend toward improved survival was seen for patients with melanoma who received IL-2 plus LAK cells, compared with those who received IL-2 alone (24-month survival: 32% versus 15%; 48-month survival: 18% versus 4%; P2 = .064 [corrected]). None of 26 patients with melanoma who received IL-2 alone are alive; five of 28 who received IL-2 plus LAK cells are alive, and three continue in complete response. No difference in survival was seen in patients with renal cell cancer in the two treatment groups. There were six treatment-related deaths (3.3%); three were due to myocardial infarction. Other toxic effects resolved by discontinuation of IL-2. Many toxic effects were related to increased vascular permeability induced by IL-2.

CONCLUSIONS

Some patients with metastatic cancer have prolonged remission when they are treated with high-dose IL-2 alone or in conjunction with LAK cells. Our results suggest a trend toward increased survival when IL-2 is given with LAK cells in patients with melanoma, but no trend was observed for patients with renal cell cancer.

IMPLICATIONS

As these studies continue, efforts are underway to develop improved immunotherapies using tumor-infiltrating lymphocytes (TIL) and gene-modified TIL.

摘要

背景

已证明单独使用白细胞介素-2（IL-2）或与淋巴因子激活的杀伤细胞（LAK）联合使用可使部分晚期癌症患者的病情得到缓解。

目的

本前瞻性随机试验旨在确定与单独使用IL-2相比，晚期癌症患者使用LAK细胞联合高剂量IL-2治疗是否能改变缓解率和生存率。

方法

181例转移性癌症患者，对标准治疗无反应或无有效治疗方案，接受单独高剂量IL-2治疗或LAK细胞加IL-2治疗。两个治疗组均按照相同方案接受相同剂量的IL-2治疗。根据患者耐受性调整IL-2剂量。181例患者中，97例为肾细胞癌，54例为黑色素瘤。

结果

中位潜在随访时间为63.2个月。在85例接受IL-2加LAK细胞治疗的可评估患者中，有10例完全缓解，而在79例单独接受IL-2治疗的患者中，有4例完全缓解。分别有14例和12例部分缓解。7例患者在50 - 66个月时仍持续完全缓解。IL-2加LAK细胞治疗的36个月精算生存率为31%，单独使用IL-2治疗的为17%（双侧P值[P2]=0.089）。与单独接受IL-2治疗的黑色素瘤患者相比，接受IL-2加LAK细胞治疗的患者有生存改善趋势（24个月生存率：32%对15%；48个月生存率：18%对4%；P2 = 0.064[校正后]）。单独接受IL-2治疗的26例黑色素瘤患者均无存活；接受IL-2加LAK细胞治疗的28例中有5例存活，3例仍持续完全缓解。两个治疗组的肾细胞癌患者生存率无差异。有6例治疗相关死亡（3.3%）；3例死于心肌梗死。其他毒性作用通过停用IL-2得以缓解。许多毒性作用与IL-2诱导的血管通透性增加有关。