1972
DOI: 10.1159/000197221
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Cell Renewal in the Gastric Mucosa

Abstract: The mechanisms controlling cell division in the stomach are still unknown. Among the procedures available for determining kinetic parameters in the mucosa, autoradiographic methods with 3H-thymidine are the most widely used. As yet, they have allowed observation of two basic control factors in the gastric mucosa: A tissue specific inhibitory substance of mitotic activity called ‘gastric chalone’ and a stimulating hormone released after food ingestion, which is most probably gastrin. Other possible f… Show more

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Cited by 34 publications
(12 citation statements)
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“…We have been unable to confirm the very early commencement of mitotic activity as reported by Hunt (7), which is also not to be expected on the basis of recent data concerning the cell cycle time in the rat stomach mucosa (20). It is impossible to estimate to which extend the elevated borders around the lesion are due to contraction in the lesion area or to an active 'piling up' o f epithelial material as a consequence of locally increased mitotic activity.…”
Section: Discussioncontrasting
confidence: 85%
“…We have been unable to confirm the very early commencement of mitotic activity as reported by Hunt (7), which is also not to be expected on the basis of recent data concerning the cell cycle time in the rat stomach mucosa (20). It is impossible to estimate to which extend the elevated borders around the lesion are due to contraction in the lesion area or to an active 'piling up' o f epithelial material as a consequence of locally increased mitotic activity.…”
Section: Discussioncontrasting
confidence: 85%
“…Thus, in both models . The cell cycle phase duration (Tc) was estimated following the method described by Willems (Willems, 1972). Percentage of positive mitotic figures refers to the ratio between BrdU labelled and total (labelled + unlabelled) mitosis.…”
Section: Discussionmentioning
confidence: 99%
“…After BrdU administration, the locusts were dissected at 30·min, at 1·h and then every hour until 24·h had elapsed. To determine the cell cycle phases we used the method of Willems (Willems, 1972). This method extrapolates cell cycle duration from the graphical representation of the BrdU labelled/ unlabelled mitosis ratio against time.…”
Section: Cell Cycle Experimentsmentioning
confidence: 99%
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“…It is hardly probable that reduced new cell pro duction is a primary effect of PGEs. A more likely but hypothetical explanation is that the reduced MI is a secondary phenomenon and a result of a negative feedback from the hyperplastic epithelium [2,9,16,17], If so the primary action of the compound should be to prolong the survival time of gastroin testinal epithelial cells by reducing losses of cells into the lumen and/or slowing of the cell migration time. As expected, such a sec ondary reduction of mitotic activity took place firstly in the antral mucosa, where tro phic changes are most prominent.…”
Section: Discussionmentioning
confidence: 99%