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Serum macrophage migration‐inhibitory factor as a diagnostic and prognostic biomarker for gastric cancer
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AbstractBACKGROUND:This study aimed to determine the potential diagnostic value of migration‐inhibitory factor (MIF) for gastric cancer in patients presenting with dyspepsia and its prognostic value for gastric cancer.METHODS:A cohort of 97 patients with histologically confirmed gastric adenocarcinoma and 222 patients with dyspepsia were recruited. Enzyme‐linked immunosorbent assay was used to measure serum MIF and carcinoembryonic antigen (CEA).RESULTS:The serum MIF concentrations were 6554.0 ± 204.1 pg/mL and 1453.7 ± 79.9 pg/mL, respectively, in gastric cancer patients and dyspeptic patients (P < .001). Serum MIF levels increased with the advancing gastric pathologies (P < .001). With the cutoff value of 3230 pg/mL, serum MIF had sensitivity, specificity, and accuracy of 83.5%, 92.3%, and 89.7%, respectively, in diagnosing gastric cancer, whereas the rates were 60.8%, 83.3%, and 76.5%, respectively, for serum CEA. Gastric cancer patients with serum MIF levels above 6600 pg/mL had a lower 5‐year survival rate than those with serum MIF level below that level (P = .012). Higher serum CEA levels were also associated with poor survival. The prediction for 5‐year survival was even better (P = .0001), using a combination of serum MIF and CEA.CONCLUSIONS:Serum MIF level, which correlates with gastric MIF expression, is a better molecular marker than CEA in diagnosing gastric cancer in patients presenting with dyspepsia. A combination of serum MIF and CEA predicts 5‐year survival better than the individual test. Cancer 2009. © 2009 American Cancer Society.
Title: Serum macrophage migration‐inhibitory factor as a diagnostic and prognostic biomarker for gastric cancer
Description:
AbstractBACKGROUND:This study aimed to determine the potential diagnostic value of migration‐inhibitory factor (MIF) for gastric cancer in patients presenting with dyspepsia and its prognostic value for gastric cancer.
METHODS:A cohort of 97 patients with histologically confirmed gastric adenocarcinoma and 222 patients with dyspepsia were recruited.
Enzyme‐linked immunosorbent assay was used to measure serum MIF and carcinoembryonic antigen (CEA).
RESULTS:The serum MIF concentrations were 6554.
0 ± 204.
1 pg/mL and 1453.
7 ± 79.
9 pg/mL, respectively, in gastric cancer patients and dyspeptic patients (P < .
001).
Serum MIF levels increased with the advancing gastric pathologies (P < .
001).
With the cutoff value of 3230 pg/mL, serum MIF had sensitivity, specificity, and accuracy of 83.
5%, 92.
3%, and 89.
7%, respectively, in diagnosing gastric cancer, whereas the rates were 60.
8%, 83.
3%, and 76.
5%, respectively, for serum CEA.
Gastric cancer patients with serum MIF levels above 6600 pg/mL had a lower 5‐year survival rate than those with serum MIF level below that level (P = .
012).
Higher serum CEA levels were also associated with poor survival.
The prediction for 5‐year survival was even better (P = .
0001), using a combination of serum MIF and CEA.
CONCLUSIONS:Serum MIF level, which correlates with gastric MIF expression, is a better molecular marker than CEA in diagnosing gastric cancer in patients presenting with dyspepsia.
A combination of serum MIF and CEA predicts 5‐year survival better than the individual test.
Cancer 2009.
© 2009 American Cancer Society.
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