| Literature DB >> 19583834 |
Chun-Yan Li1, Bao-Xiu Li, Yi Liang, Rui-Qing Peng, Ya Ding, Da-Zhi Xu, Xin Zhang, Zhi-Zhong Pan, De-Sen Wan, Yi-Xin Zeng, Xiao-Feng Zhu, Xiao-Shi Zhang.
Abstract
BACKGROUND: Cancer stem cell model suggested that tumor progression is driven by the overpopulation of cancer stem cells and eradicating or inhibiting the symmetric division of cancer stem cells would become the most important therapeutic strategy. However, clinical evidence for this hypothesis is still scarce. To evaluate the overpopulation hypothesis of cancer stem cells the association of percentage of CD133+ tumor cells with clinicopathological parameters in colon cancer was investigated since CD133 is a putative cancer stem cell marker shared by multiple solid tumors. PATIENTS AND METHODS: Tumor tissues matched with adjacent normal tissues were collected from 104 stage IIIB colon cancer patients who were subject to radical resection between January, 1999 to July, 2003 in this center. The CD133 expression was examined with immunohistochemical staining. The correlation of the percentage of CD133+ cell with clinicopathological parameters and patients' 5-year survival was analyzed.Entities:
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Year: 2009 PMID: 19583834 PMCID: PMC2715381 DOI: 10.1186/1479-5876-7-56
Source DB: PubMed Journal: J Transl Med ISSN: 1479-5876 Impact factor: 5.531
Figure 1The expression of CD133 in colon cancer patients with stage IIIB (10 × 20~10 × 100). The expression of CD133 was examined with immunohistochemical assay. (A): <5% CD133+ cells in the cancer nest; (B): ≥5% CD133+ cells in the cancer nest; (C) and (D): the staining of CD133 on the luminal surface and the basal surface of cancer cells; (E): the staining of CD133 on budding cancer nest; (F): the staining of CD133 on poor-differentiated cancer nests with ductal structures.
Correlations of CD133 expression with clinicopathological parameters in the Stage IIIB colon carcinomas
| Variables | gender | age | Invasive depth | Sites of primary mass | Grades | Pathological classifications | The percentage of CD133+ cells | |
|---|---|---|---|---|---|---|---|---|
| gender | P | . | .242 | .541 | .792 | .129 | .129 | .785 |
| age | P | .242 | . | .312 | .075 | .455 | .869 | .249 |
| Invasive depth | P | .541 | .312 | . | .895 | .272 | .426 | .499 |
| Sites of primary mass | P | .792 | .075 | .895 | . | .936 | .022* | .786 |
| Grades | P | .129 | .455 | .272 | .936 | . | .000** | .536 |
| Pathological classifications | P | .129 | .869 | .426 | .022* | .000** | . | .333 |
| The percentage of CD133+ cells | P | .785 | .249 | .499 | .786 | .536 | .333 | . |
*: P < 0.05; **: P < 0.001
Assessment of overall survival for stage IIIB colon carcinoma patients by clinicopathological parameters with univariate and multivariate analysis
| Clinicopaothological characteristics | N | 5-year survival | Kaplan-Meier analysis | Cox regression model analysis |
|---|---|---|---|---|
| 64.4% | ||||
| Gender | 0.461 | 0.479 | ||
| male | 65 | 61.5% | ||
| female | 39 | 69.2% | ||
| 64.4% | ||||
| Age | 0.148 | 0.211 | ||
| ≥ 60 year old | 57 | 57.9% | ||
| <60 year old | 47 | 72.3% | ||
| 64.4% | ||||
| Sites of primary mass | 0.291 | 0.381 | ||
| Left hemicolon | 60 | 68.3% | ||
| Right hemicolon | 44 | 59.1% | ||
| 64.4% | ||||
| Pathological classifications | 0.423 | 0.139 | ||
| papillary + tubular | 82 | 65.9% | ||
| mucoid + signet ring | 22 | 59.1% | ||
| 64.4% | ||||
| Grades | 0.154 | 0.114 | ||
| G1 | 5 | 60% | ||
| G2 | 80 | 68.8% | ||
| G3 | 19 | 47.4% | ||
| 64. 4% | ||||
| Invasive depth | 0.001 | 0.002 | ||
| T3 | 92 | 69.6% | ||
| T4 | 12 | 25.0% | ||
| 64.4% | ||||
| The percentage of CD133+ cells | 0.001 | 0.004 | ||
| ≥5% CD133 positive | 42 | 45.2% | ||
| <5%CD133 positive | 62 | 77.4% |
Figure 2The association of overall survival with the percentage of CD133+ cells in colon carcinoma patients with Stage IIIB. The patients with a lower percentage of CD133+ cells (<5%) in the cancer nests were strongly associated with longer 5-year survival than those with a higher percentage of CD133+ cells (≥5%).