HLA与恶性黑色素瘤抗肿瘤反应的关系。

F M Marincola, P Shamamian, L Rivoltini, M Salgaller, J Cormier, N P Restifo, T B Simonis, D Venzon, D E White, D R Parkinson
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引用次数: 63

摘要

在这项研究中,我们分析了北美高加索人转移性黑色素瘤患者的人类白细胞抗原(HLA)模式,并与北美高加索人(NAC)人群进行了比较。我们还研究了HLA类型是否影响黑色素瘤患者对基于白细胞介素-2 (IL-2)的治疗的耐受性和反应。从1989年2月到1993年12月,通过对患者外周血淋巴细胞进行分型收集了来自国家癌症研究所和国家卫生研究院的412例高加索黑色素瘤患者的血清学表型。此外,通过高分辨率序列特异性引物聚合酶链反应对74例黑色素瘤患者进行HLAⅱ型分型。将接受基于il -2治疗的患者(N = 272)的缓解率和治疗相关毒性与HLA血清学类型进行比较。与NAC人群相比,四种HLA-B等位基因的频率在黑色素瘤中有显著差异:其中HLA-B5、-B8和-B15的频率介于NAC和北欧人群之间。黑色素瘤患者和NAC人群在其他HLA位点上没有其他显著差异。HLA-DR3和-DR4等位基因与IL-2耐受性降低之间存在相关性,而HLA-DR的纯合性降低了反应的机会。HLA类型与应答无显著相关性。一些HLA-B等位基因与黑色素瘤之间的关联不太可能对该疾病的病因有显著影响。美国黑色素瘤患者和NAC人群之间的差异可能最好用地理血统来解释。本研究中提到的HLA-DR与IL-2治疗耐受性之间的关系可能有助于理解IL-2全身给药后一系列事件的调节机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
HLA associations in the antitumor response against malignant melanoma.

In this study we analyzed the human leukocyte antigen (HLA) pattern of North American Caucasian patients with metastatic melanoma as compared with the North American Caucasian (NAC) population. We also investigated whether the HLA type of melanoma patients had an effect on their tolerance and response to interleukin-2 (IL-2)-based therapy. Four hundred twelve serologic phenotypes of Caucasian melanoma patients referred to the National Cancer Institute, National Institutes of Health, from February 1989 through December 1993 were collected by typing the patient's peripheral blood lymphocytes. Furthermore, 74 melanoma patients were typed for HLA class II by high-resolution sequence specific primer-polymerase chain reaction. Response rate and treatment-related toxicity in those patients receiving IL-2-based treatment (N = 272) were compared with HLA serologic types. The frequency of four HLA-B alleles was significantly different in the melanoma compared with the NAC population: of these, HLA-B5, -B8, and -B15 had a frequency falling between the NAC and the Northern European population. No other significant differences between melanoma patients and NAC population were noted for other HLA loci. A correlation was noted between HLA-DR3 and -DR4 alleles and decreased tolerance to IL-2, whereas homozygosity for HLA-DR decreased the chance of response. There were no significant associations between HLA type and response. It is unlikely that the associations noted between some HLA-B alleles and melanoma bear significantly on the etiology of the disease. The differences seen between American melanoma patients and the NAC population are probably best explained by geographical ancestry. The association between HLA-DR and tolerance to IL-2 therapy noted in this study may offer insight toward the understanding of mechanisms regulating the cascade of events after the systemic administration of IL-2.

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