Literature DB >> 4005149

The permeability of normal, adenomatous, ulcerative colitic and malignant large bowel epithelial cell membranes to inulin.

T J Chambers, E P Serafini.   

Abstract

We measured the permeability of normal, adenomatous, colitic and malignant large bowel epithelial cells by immersing fragments of large bowel mucosa in radiolabelled inulin and comparing autoradiograph grain density inside and outside cells after incubation. All the carcinomas studied showed extensive uptake of inulin within 5 min, while normal, adenomatous and colitic epithelial cells completely excluded inulin for 30 min. We found no difference in the proportion of epithelial cells incorporating uridine into RNA in carcinomatous and normal mucosa, and this suggests that the increased inulin permeability of carcinoma cell membranes was not due to leakage into non-viable cells. Experiments with cytochalasin B also showed that increased pinocytosis by carcinoma cells could not account for the difference. The relative impermeability of adenomatous and colitic cells suggests that increased permeability is not caused by increased proliferation. The consistent finding of increased permeability in the plasma membranes of carcinoma cells suggests that this may be more than an epiphenomenon of malignancy. It also suggests that measurement of cell permeability may have a role in distinguishing malignant from benign epithelial neoplasms.

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Year:  1985        PMID: 4005149      PMCID: PMC2041061     

Source DB:  PubMed          Journal:  Br J Exp Pathol        ISSN: 0007-1021


  9 in total

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6.  Rectal biopsy as an aid to cancer control in ulcerative colitis.

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7.  A new marker for human cancer cells. 1 The Ca antigen and the Ca1 antibody.

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8.  Rate and pattern of epithelial cell proliferation in ulcerative colitis.

Authors:  E P Serafini; A P Kirk; T J Chambers
Journal:  Gut       Date:  1981-08       Impact factor: 23.059

9.  Aetiology of adenoma--carcinoma sequence in large bowel.

Authors:  M J Hill; B C Morson; H J Bussey
Journal:  Lancet       Date:  1978-02-04       Impact factor: 79.321

  9 in total
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