Abstract
One of the main aims of the follow-up after curative resection of colorectal cancer is the early detection and treatment of tumor recurrence. We previously demonstrated decreased preoperative soluble CD26 (sCD26) levels in serum from colorectal cancer patients. We extended now the study to investigate if sCD26 levels in postoperative serum serve as marker of recurrence of the disease during surveillance. Soluble sCD26 was measured in pre- and postoperative serum samples of 43 patients with primary colorectal cancer. Carcinoembryonic antigen, carbohydrate antigen 19.9 and 72.4 levels were also measured during surveillance. The average follow-up period was 41.8±20.8 months. sCD26 levels during follow-up showed well-defined patterns in patients without disease (n = 28), and in patients with tumor persistence (n = 2), local recurrence (n = 3) or distant metastasis (n = 10). Disease-free patients showed stable levels between 460–850 ng/mL during follow-up, while high (over 850 ng/mL) and unstable sCD26 levels were found before recurrence was diagnosed. The mean maximum/minimum sCD26 ratios during surveillance were 1.52, 2.12 and 2.63 for patients with no recurrence, local recurrence and metastasis, respectively (p = 0.005). From the cut-off obtained from a receiver operator characteristics (ROC) curve built with the maximum/minimum sCD26 ratios and the upper and lower cut-offs of sCD26, we were able to discriminate patients with and without recurrent disease. We propose that the measurement of serum sCD26 during the follow-up of patients diagnosed of colorectal cancer could be valuable for the early detection of local and distant recurrence. A large, randomized, prospective trial should be performed to confirm our findings.
Highlights
At the time of diagnosis, about 75% of colorectal cancer (CRC) patients have the tumor confined to a portion of the bowel or to regional lymph nodes, and can be referred for curative resection
Regarding patients treated with curative resection, after the follow-up period 28 were disease-free (68.3%; mean follow-up: 44.9619.5 months; range: 17.3–81.4 months), while local recurrences were documented in 3 cases (7.3%; mean follow-up: 25.763.1 months; range: 22.4–28.6 months)
Chemotherapy was given to 29 patients: 17 free of disease, 2 with local recurrence and 10 with metastases
Summary
At the time of diagnosis, about 75% of colorectal cancer (CRC) patients have the tumor confined to a portion of the bowel or to regional lymph nodes, and can be referred for curative resection. One of the aims of the follow-up after curative resection in CRC patients is to improve the outcome by early detection and treatment of recurrence. Postoperative surveillance must identify asymptomatic recurrences for the early detection of locally persistent tumors or metastases, so that further curative treatment can be initiated and the survival rates improved. Surveillance strategies require effective means for identifying residual or recurrent disease. Meta-analyses and reviews agree that a more intensive follow-up contributes to an overall survival benefit [1,2,3,4,5,6,7,8]
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