Background & Aims: The gold standard for screening for colorectal carcinoma is colonoscopy. The aim of this study was to compare endoscopic results with those obtained using the noninvasive screening test of K-ras determination in the stool in a large population of patients undergoing colonoscopy. Methods: Two hundred thirty consecutive patients were studied by K-ras amplification on stool-derived DNA using polymerase chain reaction and oligomer-specific hybridization. Results: Wild-type K-ras was amplified in 103 of 230 patients (44.8%), the rate of amplification being directly proportional to the presence of an organic disease of the intestine characterized by hyperproliferating mucosa. In 30 of these 103 patients (29.1%), a K-ras mutation was found. Four of 5 with early colorectal carcinoma, all who had K-ras mutations in the tumor, were identified. In first-degree relatives of patients with colorectal carcinoma, all subjects either carrying adenomas >1 cm in diameter or multiple smaller adenomas were identified. In patients with inflammatory bower disease, the test identified the only patient with neoplastic transformation. Conclusions: The sensitivity and specificity of K-ras determination on stool-derived DNA in patients with colorectal carcinoma, in first-degree relatives of patients with colorectal carcinoma, and in patients with inflammatory bowel disease support the opportunity of a large-scale trial to validate its use as a screening test.

Identification of subjects at risk for colorectal carcinoma through a test based on K-ras determination in the stool / Villa, Erica; A., Dugani; Am, Rebecchi; A., Vignoli; Grottola, Antonella; P., Buttafoco; Losi, Lorena; M., Perini; P., Trande; A., Merighi; R., Lerose; Manenti, Federico. - In: GASTROENTEROLOGY. - ISSN 0016-5085. - STAMPA. - 110:(1996), pp. 1346-1353.

Identification of subjects at risk for colorectal carcinoma through a test based on K-ras determination in the stool

VILLA, Erica;GROTTOLA, Antonella;LOSI, Lorena;MANENTI, Federico
1996

Abstract

Background & Aims: The gold standard for screening for colorectal carcinoma is colonoscopy. The aim of this study was to compare endoscopic results with those obtained using the noninvasive screening test of K-ras determination in the stool in a large population of patients undergoing colonoscopy. Methods: Two hundred thirty consecutive patients were studied by K-ras amplification on stool-derived DNA using polymerase chain reaction and oligomer-specific hybridization. Results: Wild-type K-ras was amplified in 103 of 230 patients (44.8%), the rate of amplification being directly proportional to the presence of an organic disease of the intestine characterized by hyperproliferating mucosa. In 30 of these 103 patients (29.1%), a K-ras mutation was found. Four of 5 with early colorectal carcinoma, all who had K-ras mutations in the tumor, were identified. In first-degree relatives of patients with colorectal carcinoma, all subjects either carrying adenomas >1 cm in diameter or multiple smaller adenomas were identified. In patients with inflammatory bower disease, the test identified the only patient with neoplastic transformation. Conclusions: The sensitivity and specificity of K-ras determination on stool-derived DNA in patients with colorectal carcinoma, in first-degree relatives of patients with colorectal carcinoma, and in patients with inflammatory bowel disease support the opportunity of a large-scale trial to validate its use as a screening test.
1996
110
1346
1353
Identification of subjects at risk for colorectal carcinoma through a test based on K-ras determination in the stool / Villa, Erica; A., Dugani; Am, Rebecchi; A., Vignoli; Grottola, Antonella; P., Buttafoco; Losi, Lorena; M., Perini; P., Trande; A., Merighi; R., Lerose; Manenti, Federico. - In: GASTROENTEROLOGY. - ISSN 0016-5085. - STAMPA. - 110:(1996), pp. 1346-1353.
Villa, Erica; A., Dugani; Am, Rebecchi; A., Vignoli; Grottola, Antonella; P., Buttafoco; Losi, Lorena; M., Perini; P., Trande; A., Merighi; R., Lerose; Manenti, Federico
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11380/612157
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