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原发性结直肠癌中单核炎性细胞浸润:一项免疫组织学分析。

Infiltration of mononuclear inflammatory cells into primary colorectal carcinomas: an immunohistological analysis.

作者信息

Håkansson L, Adell G, Boeryd B, Sjögren F, Sjödahl R

机构信息

Department of Oncology, University Hospital of Linköping, Sweden.

出版信息

Br J Cancer. 1997;75(3):374-80. doi: 10.1038/bjc.1997.61.

Abstract

Local immunoregulation mediated by mononuclear tumour-infiltrating cells is considered of importance for tumour progression of colorectal cancer, although the balance between immunosuppressor and cytotoxic activities is unclear. Colorectal cancers from 26 patients were investigated using a panel of monoclonal antibodies in order to identify subsets of mononuclear inflammatory cells and to study their pattern of distribution in relation to tumour stage and cytotoxic immune reactivity against the tumour. In all but five tumours, mononuclear cells, lymphocytes or monocytes were present in fairly large numbers, particularly in the stroma. The infiltration of CD4+ mononuclear cells predominated over the CD8+ subset. Infiltration near the tumour cells was found in four cancers only. Stromal infiltration of CD11c+ macrophages was found in all but eight tumours. Small regressive areas, in which the histological architecture of the tumours was broken down, were found in 17 tumours with intense or moderate infiltration by CD4+ lymphocytes or CD11c+ macrophages. Probably this destruction of tumour tissue was caused by cytotoxic activity of the tumour-infiltrating mononuclear cells. In Dukes' class A and B tumours, CD4+ lymphocytes predominated over CD4+ cells with macrophage morphology, but the latter were increasingly found in Dukes' class C and D disease. The occurrence of MHC II-positive macrophages and lymphocytes in different Dukes' classes was similar to that of CD4+ cells. In contrast to this, CD11c+ and CD11a+ cells were more frequent in Dukes' A and B class tumours compared with Dukes' C and D. Four out of nine tumours of the latter stages showed a poor inflammatory reaction. The interpretation of our results is that the subsets of tumour-infiltrating mononuclear cells change with advancing Dukes' class and that the local immune control is gradually broken down in progressive tumour growth, even if some cytotoxic activity is still present.

摘要

尽管免疫抑制和细胞毒性活性之间的平衡尚不清楚,但单核肿瘤浸润细胞介导的局部免疫调节被认为对结直肠癌的肿瘤进展很重要。使用一组单克隆抗体对26例患者的结直肠癌进行了研究,以识别单核炎性细胞亚群,并研究它们与肿瘤分期及针对肿瘤的细胞毒性免疫反应相关的分布模式。除5个肿瘤外,其他所有肿瘤中均存在大量单核细胞、淋巴细胞或单核细胞,尤其是在基质中。CD4 + 单核细胞的浸润多于CD8 + 亚群。仅在4例癌症中发现肿瘤细胞附近有浸润。除8个肿瘤外,其他所有肿瘤中均发现CD11c + 巨噬细胞的基质浸润。在17例有强烈或中度CD4 + 淋巴细胞或CD11c + 巨噬细胞浸润的肿瘤中发现了小的退行性区域,其中肿瘤的组织结构被破坏。肿瘤组织的这种破坏可能是由肿瘤浸润单核细胞的细胞毒性活性引起的。在Dukes A和B期肿瘤中,CD4 + 淋巴细胞多于具有巨噬细胞形态的CD4 + 细胞,但在Dukes C和D期疾病中后者越来越常见。不同Dukes分期中MHC II阳性巨噬细胞和淋巴细胞的出现情况与CD4 + 细胞相似。与此相反,与Dukes C和D期相比,CD11c + 和CDlla + 细胞在Dukes A和B期肿瘤中更常见。后两个阶段的9个肿瘤中有4个显示出不良的炎症反应。我们的结果表明,肿瘤浸润单核细胞亚群随Dukes分期的进展而变化,并且在进行性肿瘤生长中局部免疫控制逐渐被破坏,即使仍存在一些细胞毒性活性。

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