KiSS-1 expression in human breast cancer

被引:122
作者
Martin, TA [1 ]
Watkins, G [1 ]
Jiang, WG [1 ]
机构
[1] Cardiff Univ, Wales Coll Med, Univ Dept Surg, Metastasis & Angiogenesis Res Grp, Cardiff, Wales
关键词
human breast cancer; KiSS-1; metastasis; prognosis;
D O I
10.1007/s10585-005-4180-0
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
The KiSS-1 gene encodes a 145 amino acid residue peptide that is further processed to a final peptide, metastin, a ligand to a G-coupled orphan receptor (OT7T175/AXOR12). KiSS-1 has been identified as a putative human metastasis suppressor gene in melanomas and in breast cancer cell lines. This study aimed to determine the expression and distribution of KiSS-1 and its receptor in human breast cancer tissues and to identify a possible link between expression levels and patient prognosis. Frozen sections from breast cancer primary tumours (matched tumour 124 and background 33) were immuno-stained with KiSS-1 antibody. RNA was reverse transcribed and analyzed by Q-PCR (standardized using beta-actin, and normalized with cytokeratin-19 levels). Levels of expression of KiSS-1 were higher in tumour compared to background tissues (3124 +/- 1262 vs 2397 +/- 1181) and significantly increased in node positive tumours compared to node negative (3637 +/- 1719 vs 2653 +/- 1994, P = 0.02). KiSS-1 expression was also increased with increasing grade and TNM status. There were no such trends with the KiSS-1 receptor. Expression of KiSS-1 was higher in patients who had died from breast cancer than those who had remained healthy (4631 +/- 3024 vs 2280 +/- 1403) whereas expression of the receptor was reduced (480 +/- 162 vs 195 +/- 134). Immunohistochemical staining showed increased expression of KiSS-1 in tumour sections. Insertion of the KiSS-1 gene into the human breast cancer cell line MDA-MB-231, resulted in cells that were significantly more motile and invasive in behaviour, with reduced adhesion to matrix, using respective assays. In conclusion, KiSS-1 expression is increased in human breast cancer, particularly in patients with aggressive tumours and with mortality. Over-expression of KiSS-1 in breast cancer cells result in more aggressive phenotype. Together, it suggests that KiSS-1 plays a role beyond the initial metastasis repressor in this cancer type.
引用
收藏
页码:503 / 511
页数:9
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