Non-familial small bowel carcinomas are relatively rare and have a poor prognosis. Two small bowel carcinoma subsets may arise in distinct immune-inflammatory diseases (celiac disease and Crohn's disease) and have been recently suggested to differ in prognosis, celiac disease-associated carcinoma cases showing a better outcome, possibly due to their higher DNA microsatellite instability and tumor-infiltrating T lymphocytes. In this study, we investigated the histological structure (glandular vs diffuse/poorly cohesive, mixed or solid), cell phenotype (intestinal vs gastric/pancreatobiliary duct type) and Wnt signaling activation (β-catenin and/or SOX-9 nuclear expression) in a series of 26 celiac disease-associated small bowel carcinoma, 25 Crohn's disease-associated small bowel carcinoma and 25 sporadic small bowel carcinoma cases, searching for new prognostic parameters. In addition, non-tumor mucosa of celiac and Crohn's disease patients was investigated for epithelial precursor changes (hyperplastic, metaplastic or dysplastic) to help clarify carcinoma histogenesis. When compared with non-glandular structure and non-intestinal phenotype, both glandular structure and intestinal phenotype were associated with a more favorable outcome at univariable or stage- and microsatellite instability/tumor-infiltrating lymphocyte-inclusive multivariable analysis. The prognostic power of histological structure was independent of the clinical groups while the non-intestinal phenotype, associated with poor outcome, was dominant among Crohn's disease-associated carcinoma. Both nuclear β-catenin and SOX-9 were preferably expressed among celiac disease-associated carcinomas; however, they were devoid, per se, of prognostic value. We obtained findings supporting an origin of celiac disease-associated carcinoma in SOX-9-positive immature hyperplastic crypts, partly through flat β-catenin-positive dysplasia, and of Crohn's disease-associated carcinoma in a metaplastic (gastric and/or pancreatobiliary-type) mucosa, often through dysplastic polypoid growths of metaplastic phenotype. In conclusion, despite their common origin in a chronically inflamed mucosa, celiac disease-associated and Crohn's disease-associated small bowel carcinomas differ substantially in histological structure, phenotype, microsatellite instability/tumor-infiltrating lymphocyte status, Wnt pathway activation, mucosal precursor lesions and prognosis.

Small bowel carcinomas in celiac or Crohn's disease: Distinctive histophenotypic, molecular and histogenetic patterns / Vanoli, A.; Di Sabatino, A.; Martino, M.; Klersy, C.; Grillo, F.; Mescoli, C.; Nesi, G.; Volta, U.; Fornino, D.; Luinetti, O.; Fociani, P.; Villanacci, V.; D'armiento, F. P.; Cannizzaro, R.; Latella, G.; Ciacci, C.; Biancone, L.; Paulli, M.; Sessa, F.; Rugge, M.; Fiocca, R.; Corazza, G. R.; Solcia, E.; Ardizzone, S.; Astegiano, M.; Caio, G.; Calabro, A.; Canzonieri, V.; Cerutti, R.; Ciardi, A.; Coppola, L.; D'inca, R.; Elli, L.; Ferrero, S.; Florena, A. M.; Furlan, D.; Giannone, A. G.; Giuffrida, P.; Macciomei, M. C.; Maccioni, A.; Monteleone, G.; Migliora, P.; Orlandi, A.; Papi, C.; Perfetti, V.; Bonetti, L. R.; Rizzo, A.; Salemme, M.; Sandri, G.; Sampietro, G.; Santeusanio, G.; Santini, D.; Silano, M.; Solina, G.; Tonelli, F.; Trapani, D.; Usai, P.. - In: MODERN PATHOLOGY. - ISSN 0893-3952. - 30:10(2017), pp. 1453-1466. [10.1038/modpathol.2017.40]

Small bowel carcinomas in celiac or Crohn's disease: Distinctive histophenotypic, molecular and histogenetic patterns

Martino M.;Giuffrida P.;Monteleone G.;Bonetti L. R.;Sampietro G.;Santini D.;Usai P.
2017

Abstract

Non-familial small bowel carcinomas are relatively rare and have a poor prognosis. Two small bowel carcinoma subsets may arise in distinct immune-inflammatory diseases (celiac disease and Crohn's disease) and have been recently suggested to differ in prognosis, celiac disease-associated carcinoma cases showing a better outcome, possibly due to their higher DNA microsatellite instability and tumor-infiltrating T lymphocytes. In this study, we investigated the histological structure (glandular vs diffuse/poorly cohesive, mixed or solid), cell phenotype (intestinal vs gastric/pancreatobiliary duct type) and Wnt signaling activation (β-catenin and/or SOX-9 nuclear expression) in a series of 26 celiac disease-associated small bowel carcinoma, 25 Crohn's disease-associated small bowel carcinoma and 25 sporadic small bowel carcinoma cases, searching for new prognostic parameters. In addition, non-tumor mucosa of celiac and Crohn's disease patients was investigated for epithelial precursor changes (hyperplastic, metaplastic or dysplastic) to help clarify carcinoma histogenesis. When compared with non-glandular structure and non-intestinal phenotype, both glandular structure and intestinal phenotype were associated with a more favorable outcome at univariable or stage- and microsatellite instability/tumor-infiltrating lymphocyte-inclusive multivariable analysis. The prognostic power of histological structure was independent of the clinical groups while the non-intestinal phenotype, associated with poor outcome, was dominant among Crohn's disease-associated carcinoma. Both nuclear β-catenin and SOX-9 were preferably expressed among celiac disease-associated carcinomas; however, they were devoid, per se, of prognostic value. We obtained findings supporting an origin of celiac disease-associated carcinoma in SOX-9-positive immature hyperplastic crypts, partly through flat β-catenin-positive dysplasia, and of Crohn's disease-associated carcinoma in a metaplastic (gastric and/or pancreatobiliary-type) mucosa, often through dysplastic polypoid growths of metaplastic phenotype. In conclusion, despite their common origin in a chronically inflamed mucosa, celiac disease-associated and Crohn's disease-associated small bowel carcinomas differ substantially in histological structure, phenotype, microsatellite instability/tumor-infiltrating lymphocyte status, Wnt pathway activation, mucosal precursor lesions and prognosis.
2017
30
10
1453
1466
WOS:000412100400011
2-s2.0-85030631722
28664941
Small bowel carcinomas in celiac or Crohn's disease: Distinctive histophenotypic, molecular and histogenetic patterns / Vanoli, A.; Di Sabatino, A.; Martino, M.; Klersy, C.; Grillo, F.; Mescoli, C.; Nesi, G.; Volta, U.; Fornino, D.; Luinetti, O.; Fociani, P.; Villanacci, V.; D'armiento, F. P.; Cannizzaro, R.; Latella, G.; Ciacci, C.; Biancone, L.; Paulli, M.; Sessa, F.; Rugge, M.; Fiocca, R.; Corazza, G. R.; Solcia, E.; Ardizzone, S.; Astegiano, M.; Caio, G.; Calabro, A.; Canzonieri, V.; Cerutti, R.; Ciardi, A.; Coppola, L.; D'inca, R.; Elli, L.; Ferrero, S.; Florena, A. M.; Furlan, D.; Giannone, A. G.; Giuffrida, P.; Macciomei, M. C.; Maccioni, A.; Monteleone, G.; Migliora, P.; Orlandi, A.; Papi, C.; Perfetti, V.; Bonetti, L. R.; Rizzo, A.; Salemme, M.; Sandri, G.; Sampietro, G.; Santeusanio, G.; Santini, D.; Silano, M.; Solina, G.; Tonelli, F.; Trapani, D.; Usai, P.. - In: MODERN PATHOLOGY. - ISSN 0893-3952. - 30:10(2017), pp. 1453-1466. [10.1038/modpathol.2017.40]
Vanoli, A.; Di Sabatino, A.; Martino, M.; Klersy, C.; Grillo, F.; Mescoli, C.; Nesi, G.; Volta, U.; Fornino, D.; Luinetti, O.; Fociani, P.; Villanacci...espandi
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