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转移性人类黑色素瘤中树突状细胞密度及肿瘤浸润淋巴细胞的活化状态:对前哨淋巴结转移的潜在影响

Dendritic cell density and activation status of tumour-infiltrating lymphocytes in metastatic human melanoma: possible implications for sentinel node metastases.

作者信息

Barbour Angela H, Coventry Brendon J

机构信息

Department of Pathology, University of Adelaide, Adelaide, South Australia, 5005, Australia.

出版信息

Melanoma Res. 2003 Jun;13(3):263-9. doi: 10.1097/00008390-200306000-00007.

DOI:10.1097/00008390-200306000-00007
PMID:12777981
Abstract

Nodal deposits of melanoma may present many years after resection of the primary tumour, implying initial suppression of tumour growth with subsequent immune escape. Using immunocytochemical techniques on frozen sections, the cellular types and activation status of infiltrating cells within a series of 19 clinically apparent nodal metastases of melanoma were studied. Infiltrating cells were assessed using a semiquantitative grading system. Macrophages (CD68+) and T-lymphocytes (CD3+) (including both CD8+ and probably also CD4+ T-cells) were the predominant cells infiltrating the tumours. B-lymphocytes (CD20+) were generally present in low numbers. CD1a+ putative dendritic cell density and expression of the early lymphocyte activation markers interleukin-2 receptor alpha (IL2Ralpha) and CD69 was low. However, greater evidence of intermediate lymphocyte activation (CD38) was identified. Expression of interleukin-2 (IL2) by tumour-infiltrating cells was not detected. The paucity of staining for IL2 and IL2Ralpha, with greater expression of CD38 by infiltrating cells, suggests that the usual pathways of lymphocyte activation via IL2 were bypassed or impaired within the lymph node metastases. Low numbers of CD1a+ putative dendritic cells may result in reduced effector cell activation. These findings provide evidence to support the hypothesis that antitumour immune responses within clinically involved lymph nodes are reduced in metastatic melanoma. This also has possible implications for micrometastases to the sentinel lymph node.

摘要

黑色素瘤的淋巴结转移灶可能在原发肿瘤切除多年后才出现,这意味着肿瘤生长最初受到抑制,随后出现免疫逃逸。利用免疫细胞化学技术对冰冻切片进行研究,分析了19例临床可见的黑色素瘤淋巴结转移灶中浸润细胞的细胞类型和激活状态。采用半定量分级系统对浸润细胞进行评估。巨噬细胞(CD68+)和T淋巴细胞(CD3+)(包括CD8+和可能的CD4+ T细胞)是浸润肿瘤的主要细胞。B淋巴细胞(CD20+)数量通常较少。CD1a+假定树突状细胞密度以及早期淋巴细胞激活标志物白细胞介素-2受体α(IL2Rα)和CD69的表达较低。然而,发现了更多中间淋巴细胞激活(CD38)的证据。未检测到肿瘤浸润细胞表达白细胞介素-2(IL2)。IL2和IL2Rα染色较少,而浸润细胞CD38表达较高,这表明在淋巴结转移灶中,通过IL2激活淋巴细胞的通常途径被绕过或受损。CD1a+假定树突状细胞数量较少可能导致效应细胞激活减少。这些发现为支持以下假设提供了证据:在临床受累的淋巴结中,转移性黑色素瘤的抗肿瘤免疫反应降低。这对前哨淋巴结微转移也可能有影响。

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