A gene signature, first identified in mouse colon cancer cells, may help identify patients at risk of colon cancer recurrence, has been suggested by researchers.
The study by Vanderbilt-Ingram Cancer Center researchers has been published in the March issue of Gastroenterology.
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In its early stages, colorectal cancer is treated with surgery only. However, between 20 percent and 25 percent of patients with Stage II disease (when the tumor has penetrated the muscular wall of the colon) will experience metastatic recurrence after surgical resection alone.
For stage III, when the cancer has spread to the lymph nodes, surgery is generally followed by chemotherapy - despite research showing that about 40 percent of stage III patients treated by surgery alone do not have a recurrence of disease in five years.
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Using a mouse colon cancer cell line, R. Daniel Beauchamp, M.D., the John Clinton Foshee Distinguished Professor of Surgery and chair of the Section of Surgical Sciences, and colleagues identified 300 genes that showed distinct patterns of expression related to their ability to invade into a gel-like matrix, a test that reflects the aggressiveness of cancer cells.
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The researchers then examined whether this 34-gene signature could predict recurrence and death in a larger patient population.
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Among patients with stage II disease, those with the "poor prognosis" signature had a five-year mortality rate of 31 percent. However, no stage II patients with a "low recurrence" (or "good prognosis") signature died within the five-year period.
In patients with stage III disease, 38 percent of those with a "poor" signature died of their disease within five years, whereas only 10.7 percent of those with a "good" prognosis signature died within that time period.
"Across all stages, if patients had a 'poor' prognosis signature, then they would be five times more likely to have a recurrence of cancer than those with a 'good' prognosis signature," said Beauchamp.
But the most interesting finding, Beauchamp says, is the ability of this gene signature to identify the patients most likely to benefit from chemotherapy.
Among stage III patients with a "poor" prognosis signature, those who had received chemotherapy had a 36 percent cancer-related death rate. Those who did not receive chemotherapy had an 86 percent death rate.
"That tells us that patients with the ('poor' prognosis signature) probably benefited from chemotherapy," Beauchamp said.
"And (patients with a 'good' prognosis signature) appeared to get no benefit from chemotherapy."
Source-ANI
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