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黑色素瘤的区域性免疫:免疫抑制变化先于淋巴结转移。

Regional immunity in melanoma: immunosuppressive changes precede nodal metastasis.

机构信息

Division of Hematology, Department of Internal Medicine, Mayo Clinic, Rochester,MN 55905, USA.

出版信息

Mod Pathol. 2011 Apr;24(4):487-94. doi: 10.1038/modpathol.2010.227. Epub 2010 Dec 10.

DOI:10.1038/modpathol.2010.227
PMID:21151098
Abstract

In order to characterize the degree of immunosuppression in regional immunity in patients with melanoma, we used immunohistochemistry to analyze markers of T-cell subtype and polarity, costimulation, dendritic cell maturation, monocytes, lymphatic vasculature, and angiogenesis. Specifically, we analyzed expression of CD4, CD8, CD14, CD40, CD86, CD123, HLA-DR, IL-10, LYVE, VEGFR3, and VEGF-C in lymph nodes. We compared sentinel lymph nodes with and without metastasis from patients with melanoma with both infection inflamed (reactive) and dormant human lymph nodes. There were no differences demonstrated between sentinel lymph nodes with or without metastasis from patients with melanoma in any of the markers that were tested. Both groups of sentinel lymph nodes had fewer CD8(+) T cells than either set of control nodes. Whereas the infection inflamed lymph nodes demonstrated Th2 polarity, the dormant lymph nodes demonstrated Th1 polarity. In conclusion, changes in regional immunity appeared to precede metastasis in melanoma. Whether there was tumor present in sentinel lymph nodes or not, these nodes demonstrated a marked decrease in cytotoxic T cells compared with both sets of controls. Furthermore, the control lymph nodes used for comparison can significantly impact interpretation, as the dormant and reactive lymph nodes markedly varied in their immune profiles. These immunologic changes may explain the successful metastasis of melanoma in the midst of the immune environment of the sentinel lymph node, and lend insights into the mechanisms of lymphatic metastases in other solid malignancies.

摘要

为了描述黑色素瘤患者局部免疫抑制的程度,我们使用免疫组织化学分析了 T 细胞亚型和极性、共刺激、树突状细胞成熟、单核细胞、淋巴管和血管生成的标志物。具体来说,我们分析了淋巴结中 CD4、CD8、CD14、CD40、CD86、CD123、HLA-DR、IL-10、LYVE、VEGFR3 和 VEGF-C 的表达。我们比较了黑色素瘤患者伴或不伴转移的前哨淋巴结与具有感染性炎症(反应性)和休眠性的人类淋巴结。在测试的任何标志物中,黑色素瘤患者伴或不伴转移的前哨淋巴结之间均未显示出差异。两组前哨淋巴结中的 CD8(+) T 细胞均少于对照组的任何一组。感染性炎症的淋巴结表现出 Th2 极性,而休眠的淋巴结表现出 Th1 极性。总之,局部免疫的变化似乎先于黑色素瘤的转移。无论前哨淋巴结中是否存在肿瘤,这些淋巴结与两组对照相比,细胞毒性 T 细胞明显减少。此外,用于比较的对照淋巴结会显著影响解释,因为休眠和反应性淋巴结的免疫特征明显不同。这些免疫变化可能解释了黑色素瘤在淋巴结的免疫环境中成功转移,并深入了解了其他实体恶性肿瘤中淋巴转移的机制。

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