Undifferentiated columnar cells in colorectal adenomas and familial adenomatous polyposis

Superficial colonic cells were taken from normal-appearing mucosa at 2, 5, and 10 cm proximal and distal to colorectal cancer margins in 37 patients. The DNA ploidy and proliferative pattern of each sample were determined using flow cytometry. In 11 patients, histology of mucosal sections from the same sites also was analyzed. We found a higher frequency of aneuploidy than previously reported in mucosa up to 10 cm from a colorectal cancer; 62% (23/37) of the primary cancers were aneuploid, and of these, 48% (11/23) were associated with adjacent aneuploid mucosa. The mucosa adjacent to the 14 diploid cancers had only diploid characteristics. The proliferative activity (as reflected by synthetic (S) phase fraction) of aneuploid cancers (21.1 +/- 2.0% SEM) and aneuploid mucosa as far as 10 cm away (21.2 +/- 2.1% SEM) was higher than in normal controls (10.2 +/- 0.7% SEM) (P less than 0.0005). Parallel cytology excluded shed cancer cells as an explanation for these findings. Histology showed diffuse, generally mild and reactive, mucosal abnormalities in eight of 11 patients. Ploidy did not correlate with histologic abnormalities. The findings of aneuploidy and high S-phase fraction in uninvolved superficial mucosa provide evidence for a field defect in mucosa adjacent to colorectal cancer and support the concept that the large bowel mucosa behaves as a unit in carcinogenesis.

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Abnormal DNA ploidy and proliferative patterns in superficial colonic epithelium adjacent to colorectal cancer

Ngoi

Staiano‐Coico

Godwin

et al. 1990

Cancer

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Intestinal-Type Gastric Carcinoma and Colonic Carcinoma: A Common Pathogenesis?

Newbold

1989

The Lancet

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Notable intrafamilial phenotypic variability in a kindred with familial adenomatous polyposis and an APC mutation in exon 9

Rozen¹,

Samuel²,

Shomrat³

et al. 1999

Gut

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Background-The phenotypic spectrum of familial adenomatous polyposis (FAP) varies from the classic appearance of hundreds of adenomatous colonic polyps in the young adult and early onset colorectal cancer, to the occurrence of sparse adenomas in the older adult, "attenuated" FAP, due to mutations at the 5' or 3' ends of the APC gene. Aims-To investigate marked intrafamilial phenotypic variation occurring in a family with an APC gene mutation in exon 9. Patients-An extended kindred of 22 people of whom 16 had colorectal neoplasia and/or were APC mutation carriers. Results-Phenotypic manifestation varied from classic FAP to a complete lack of clinical or endoscopic, or bioptic disease in five people in three diVerent generations. This occurred in four of them over two generations, in spite of having a confirmed 11 bp insertion causing a frame shift and stop codon (363) in exon 9 of the APC gene. Conclusions-At present, it is assumed that in this family there is alternative splicing of the APC gene, and/or unidentified modifying genetic factors. The family illustrates the importance of genetic testing in evaluating carrier status and not just clinical examination. This clinical observation also highlights the dilemma in recognising the possible contribution of low penetrance germline APC mutations to what has been considered "sporadic" colorectal neoplasia. (Gut 1999;45:829-833)

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Undifferentiated columnar cells in colorectal adenomas and familial adenomatous polyposis

Cited by 3 publications

References 6 publications

Abnormal DNA ploidy and proliferative patterns in superficial colonic epithelium adjacent to colorectal cancer

Abnormal DNA ploidy and proliferative patterns in superficial colonic epithelium adjacent to colorectal cancer

Intestinal-Type Gastric Carcinoma and Colonic Carcinoma: A Common Pathogenesis?

Notable intrafamilial phenotypic variability in a kindred with familial adenomatous polyposis and an APC mutation in exon 9

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