肿瘤内皮在人胰腺癌CD4 + CD25 +调节性T细胞浸润中的作用

Role of tumor endothelium in CD4+ CD25+ regulatory T cell infiltration of human pancreatic carcinoma.

作者信息

Nummer Daniel, Suri-Payer Elisabeth, Schmitz-Winnenthal Hubertus, Bonertz Andreas, Galindo Luis, Antolovich Dalibor, Koch Moritz, Büchler Markus, Weitz Jürgen, Schirrmacher Volker, Beckhove Philipp

机构信息

T cell Tumor Immunity group, The German Cancer Research Center, INF280, 69120 Heidelberg, Germany.

出版信息

J Natl Cancer Inst. 2007 Aug 1;99(15):1188-99. doi: 10.1093/jnci/djm064. Epub 2007 Jul 24.

DOI:10.1093/jnci/djm064

PMID:17652277

Abstract

BACKGROUND

Regulatory T (Treg) cells have been detected in human carcinomas and may play a role in preventing the rejection of malignant cells.

METHODS

We quantified Treg cells and the expression of the addressins and the respective ligands that attract them in blood and in human pancreatic tumors and adjacent nonmalignant tissues from 47 patients. The capacity of Treg cells to adhere to and transmigrate through autologous endothelial cells was tested in vitro using spheroid adhesion assays and in vivo using a xenotransplant NOD/SCID model and in the presence and absence of antibodies to addressins. All statistical tests were two-sided.

RESULTS

More Treg cells infiltrated pancreatic carcinomas than adjacent nonmalignant pancreatic tissues (120 cells per mm2 versus 80 cells per mm2, difference = 40 cells per mm2, 95% confidence interval [CI] = 21.2 cells per mm2 to 52.1 cells per mm2; P<.001). In contrast to conventional CD4+ T cells, more blood-derived Treg cells adhered to (1.0% versus 5.2%, difference = 4.2%, 95% CI = 2.7% to 5.6%; P<.001) and transmigrated through (3332 cells versus 4976 cells, difference = 1644 cells, 95% CI = 708 cells to 2580 cells; P = .008) autologous tumor-derived endothelial cells in vitro and in vivo (458 cells versus 605 cells, difference = 147 cells, 95% CI = 50.8 to 237.2 cells; P = .04). Tumor-derived endothelial cells expressed higher levels of addressins--including mucosal adressin cell adhesion molecule-1 (MAdCAM-1), vascular cell adhesion molecule-1 (VCAM-1), CD62-E, and CD166--than endothelial cells from normal tissue. Experiments using antibodies to addressins showed that transmigration was mediated by interactions of addressins, including MAdCAM-1, VCAM-1, CD62-E, and CD166 with their respective ligands, beta7 integrin, CD62L, and CD166, which were expressed specifically on Treg cells.

CONCLUSIONS

Tumor-induced expression of addressins on the surface of endothelial cells allows a selective transmigration of Treg cells from peripheral blood to tumor tissues.

摘要

背景

已在人类癌症中检测到调节性T（Treg）细胞，其可能在防止恶性细胞被排斥方面发挥作用。

方法

我们对47例患者血液、人胰腺肿瘤及相邻非恶性组织中的Treg细胞、归巢素及其吸引Treg细胞的相应配体的表达进行了定量分析。采用球体黏附试验在体外以及采用异种移植NOD/SCID模型在体内，在有和没有归巢素抗体的情况下，测试Treg细胞黏附于自体内皮细胞并穿过自体内皮细胞迁移的能力。所有统计检验均为双侧检验。

结果

浸润胰腺癌的Treg细胞多于相邻的非恶性胰腺组织（每平方毫米120个细胞对每平方毫米80个细胞，差值为每平方毫米40个细胞，95%置信区间[CI]=每平方毫米21.2个细胞至每平方毫米52.1个细胞；P<0.001）。与传统CD4+T细胞相比，更多源自血液的Treg细胞在体外和体内黏附于（1.0%对5.2%，差值为4.2%，95%CI=2.7%至5.6%；P<0.001）并穿过（3332个细胞对4976个细胞，差值为1644个细胞，95%CI=708个细胞至2580个细胞；P=0.008）自体肿瘤来源的内皮细胞（458个细胞对605个细胞，差值为147个细胞，95%CI=50.8至237.2个细胞；P=0.04）。肿瘤来源的内皮细胞表达的归巢素水平更高，包括黏膜地址素细胞黏附分子-1（MAdCAM-1）、血管细胞黏附分子-1（VCAM-1）、CD62-E和CD166，高于正常组织来源的内皮细胞。使用归巢素抗体的实验表明，迁移是由归巢素（包括MAdCAM-1、VCAM-1、CD62-E和CD166）与其各自配体（β7整合素、CD62L和CD166）的相互作用介导的，这些配体在Treg细胞上特异性表达。