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Development of ulcerative colitis and its associated colorectal neoplasia as a model of the organ‐specific chronic inflammation‐carcinoma sequence
Author(s) -
Okayasu Isao
Publication year - 2012
Publication title -
pathology international
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.73
H-Index - 74
eISSN - 1440-1827
pISSN - 1320-5463
DOI - 10.1111/j.1440-1827.2012.02807.x
Subject(s) - inflammation , ulcerative colitis , colorectal cancer , pathology , inflammatory bowel disease , colitis , medicine , carcinoma , cancer research , biology , immunology , cancer , disease
The organ‐specific chronic inflammation‐carcinoma sequence was summarized and proposed. As a typical model, the ulcerative colitis (UC)—UC‐associated carcinoma sequence was selected, and the mechanism of development of UC and UC‐associated carcinoma was reviewed, referring mainly to our data. Intestinal commensal bacteria, including Fusobacterium varium , obtained from the colonic mucosa of UC patients, can enter colonic epithelia and induce secretion of inflammatory cytokines, resulting in early inflammatory lesions consisting of cryptitis and crypt abscess. Inflammatory oxidative stress causes epithelial cell DNA‐damage followed by p53 dependent G1 checkpoint activation and overloading, which causes p53 mutation. In long‐standing UC, mucosal remodeling, including possible loss of crosstalk between epithelium and stroma may be critical for the development of UC‐associated carcinoma, as well as accumulation of early p53 mutation at the crypt level and increase of other stem cell mutated crypts, telomere shortening, and genomic instability of epithelial and stromal cells, including subepithelial myofibroblasts (corresponding to colonic stellate cells or Ito cells) and interstitial cells. Thus, the stochastic (probabilistic) pathway to tumor development over time gains commonalty through chronic inflammation stimulation. For the prevention of cancer development, appropriate anti‐inflammatory therapy is important with an accurate assessment of the inflammation status in the colorectum.