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趋化因子CCL21在人类结肠腺癌中的表达降低。

Decreased expression of the chemokine CCL21 in human colorectal adenocarcinomas.

作者信息

Mumtaz Melad, Wågsäter Dick, Löfgren Sture, Hugander Anders, Zar Niklas, Dimberg Jan

机构信息

Biotechnology, Al-Nahrain University, Baghdad, Iraq.

出版信息

Oncol Rep. 2009 Jan;21(1):153-8.

PMID:19082456
Abstract

Recent studies have revealed participation of chemokines in cancer by regulating leukocyte movement to modify local immunoresponse. The chemokine CCL21 has been identified to play a pivotal role in homing and localization of immune cells to lymphoid tissue and into organ of non-lymphoid origin. In the cancer biology CCL21 seems to have multifaceted roles. CCL21 attracts CCR7 bearing cells especially T and dendritic cells but also various cancer cells. Besides the antitumour role as leukocyte recruiting, CCL21 has been shown to facilitate dendritic cell functions and to exert an angiostatic effect. To gain insight into the possible influence of CCL21 on colorectal cancer (CRC) we determined whether the CCL21 is altered in CRC tissue. Collectively, by using ELISA we noted a significant lower CCL21 level in cancer tissue compared with paired normal tissue. Patients with a tumour localized in the rectum revealed significantly lower level of CCL21 than patients with a tumour localized in the colon both compared with paired normal tissue. We used immunohistochemistry and found heterogeneous immunoreactivity predominantly within areas of stromal cells mainly in macrophages. We also used a TaqMan system to investigate two single-nucleotide polymorphisms rs 11574915 and rs 2812377 with supposed effect on CRC. No significant difference was observed between CRC and control subjects regarding genotype and allelic distributions or associations to clinical characteristics or CCL21 tissue levels. Our study implied that lower level of CCL21 in CRC tissue supports the idea that cancer is related to immunodeficiency probably depending on regulatory factors produced by tumour cells and that the different levels of CCL21 in rectum and colon may reflect divergent mechanisms in colorectal carcinogenesis. Further studies are needed to clarify whether the CCL21 level has an impact on CRC progression and survival rate.

摘要

最近的研究表明,趋化因子通过调节白细胞运动来改变局部免疫反应,从而参与癌症进程。趋化因子CCL21已被确定在免疫细胞归巢和定位于淋巴组织以及非淋巴源性器官中起关键作用。在癌症生物学中,CCL21似乎具有多方面的作用。CCL21吸引携带CCR7的细胞,尤其是T细胞和树突状细胞,也吸引各种癌细胞。除了作为白细胞募集的抗肿瘤作用外,CCL21还被证明可促进树突状细胞功能并发挥血管生成抑制作用。为了深入了解CCL21对结直肠癌(CRC)的可能影响,我们确定了CRC组织中CCL21是否发生改变。总体而言,通过酶联免疫吸附测定(ELISA),我们发现癌组织中的CCL21水平明显低于配对的正常组织。与配对的正常组织相比,肿瘤位于直肠的患者的CCL21水平明显低于肿瘤位于结肠的患者。我们使用免疫组织化学方法,发现主要在巨噬细胞等基质细胞区域内存在异质性免疫反应。我们还使用TaqMan系统研究了两个单核苷酸多态性rs 11574915和rs 2812

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