Mast cells promote the progression of experimental tumors and might be a valuable therapeutic target. However, the relevant clinical evidence is still controversial. This study analyzed the relationship between the distribution of mast cells and the survival of patients with colon cancer to study whether mast cells contribute to tumor progression. Materials and methods Ninety-three cases of pathologically confirmed primary cancer tissues matched with adjacent normal mucosa, metastases of regional-draining lymph nodes and regional-draining lymph nodes without metastases were collected from stage IIIB colon carcinoma patients between January 1997 and July 2004 at the Cancer Center of Sun Yat-Sen University. Tryptase-positive mast cells were counted. The relationships of the distribution of mast cells with clinicopathologic parameters and 5-year survival were analyzed. Results Although the mast cell count in the mucosa adjacent to the primary colon cancer was significantly higher than that in the stroma of the primary colon cancer, no difference in mast cell counts was observed between the stroma in lymph node metastasis and the lymph tissue adjacent to the metastasis. Additionally, the mast cell count in the regional-draining lymph node without the invasion of cancer cells was significantly higher than that in the stroma of lymph node metastasis and adjacent lymph tissue. However, none of those mast cell counts was related to 5-year survival. Conclusion Although mast cell count varied with location, none of the mast cell counts was related to 5-year survival, suggesting that mast cells do not contribute to the progression of stage IIIB colon cancer.
Xiaet al.Journal of Translational Medicine2011,9:88 http://www.translationalmedicine.com/content/9/1/88
R E S E A R C HOpen Access No relationship between the distribution of mast cells and the survival of stage IIIB colon cancer patients 1,2 1,31,2,5 1,41,4 1,3 Qing Xia, XiaoJun Wu, Qiang Zhou, JingZeng, JingHui Hou, ZhiZhong Panand 1,2* XiaoShi Zhang
Abstract Background:Mast cells promote the progression of experimental tumors and might be a valuable therapeutic target. However, the relevant clinical evidence is still controversial. This study analyzed the relationship between the distribution of mast cells and the survival of patients with colon cancer to study whether mast cells contribute to tumor progression. Materials and methods:Ninetythree cases of pathologically confirmed primary cancer tissues matched with adjacent normal mucosa, metastases of regionaldraining lymph nodes and regionaldraining lymph nodes without metastases were collected from stage IIIB colon carcinoma patients between January 1997 and July 2004 at the Cancer Center of Sun YatSen University. Tryptasepositive mast cells were counted. The relationships of the distribution of mast cells with clinicopathologic parameters and 5year survival were analyzed. Results:Although the mast cell count in the mucosa adjacent to the primary colon cancer was significantly higher than that in the stroma of the primary colon cancer, no difference in mast cell counts was observed between the stroma in lymph node metastasis and the lymph tissue adjacent to the metastasis. Additionally, the mast cell count in the regionaldraining lymph node without the invasion of cancer cells was significantly higher than that in the stroma of lymph node metastasis and adjacent lymph tissue. However, none of those mast cell counts was related to 5year survival. Conclusion:Although mast cell count varied with location, none of the mast cell counts was related to 5year survival, suggesting that mast cells do not contribute to the progression of stage IIIB colon cancer. Keywords:Mast cells, Colon cancer, Survival, Progression
Background In addition to the genetic alterations of cancer cells, it is believed that the infiltration of immune cells, such as dendritic cells, T cells, macrophages, and mast cells, are involved in the progression of colon cancer [1-6]. For example, mast cells might impact tumor progres-sion by induction of angiogenesis, tissue remodeling, immune cell recruitment and direct cytotoxicity against cancer cells [7-9]. Because c-kit inhibitors such as imatinib and sunitinib have been approved in
* Correspondence: zxs617@hotmail.com 1 State Key Laboratory of Oncology in South China, Sun Yatsen University Cancer Center, Guangzhou 510060, China Full list of author information is available at the end of the article
clinical practice and mast cells depend on c-kit, mast cells might be a new target for cancer therapy [10]. In animal models, polyps are infiltrated by pro-inflamma-tory mast cells and their precursors. Depletion of mast cells, either pharmacologically or through the genera-tion of chimeric mice with genetic lesions in mast cell development, leads to a profound remission of existing polyps [11]. The interaction between mast cells and Treg cells shifts the local balance of immune surveil-lance in favor of tumor progression [12]. However, the relevant clinical evidence is controversial. For example, although Yodavudh and Nielsen reported that mast cell count was an independent prognostic factor for