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EXPERIMENTAL PRODUCTION OF DIGESTIVE TRACT ULCERATIONS

We have attempted to reproduce in animal experiments a group of pathological findings which we have observed to be associated with shock. In order to simulate the compensatory vasomotor reactions occurring in shock, we have utilized the intraperitoneal injection of adrenalin hydrochloride in dogs, c...

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Autores principales: Penner, Abraham, Bernheim, Alice Ida
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1939
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2133803/
https://www.ncbi.nlm.nih.gov/pubmed/19870922
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author Penner, Abraham
Bernheim, Alice Ida
author_facet Penner, Abraham
Bernheim, Alice Ida
author_sort Penner, Abraham
collection PubMed
description We have attempted to reproduce in animal experiments a group of pathological findings which we have observed to be associated with shock. In order to simulate the compensatory vasomotor reactions occurring in shock, we have utilized the intraperitoneal injection of adrenalin hydrochloride in dogs, cats, rabbits and guinea pigs. That the effect of adrenalin hydrochloride when injected by this route is of long duration has been shown by the prolonged hyperglycemia which it produces. Our experiments have resulted in the production of a lesion in the digestive tract which is identical in the gross with those which we observed in our human material. The histological changes, however, have been found to differ from those encountered in the latter. These differences have been noted to occur only in the dog and cat, where the initial changes take place in the mucosa, and the alterations in the submucosa appear secondary to these. In the rabbit and guinea pig the histogenesis of the lesions is identical with that observed in man, the lesions first manifesting themselves in changes in the submucosa, congestion, edema and hernorrhage. Only later are similar changes seen in the mucosa, progressing finally to necrosis and ulceration. The cause of the histological differences has been found in the presence of arteriovenous anastomoses which occur in the submucosa in the case of the dog and cat and in the mucosa in the case of the rabbit, guinea pig and man. We have pointed out that variations in blood flow through the intestinal wall may result from the short circuiting of the blood through the arteriovenous anastomoses. This, associated with the vasoconstriction known to occur in shock, may if severe and prolonged, result in necrosis of the intestinal wall. We have experimentally reproduced the same lesion by the injection of adrenalin, which acts in a similar way. The experimentally produced anatomical changes offer additional evidence in support of the clinical occurrence of a vasospasm which is of sufficient severity and duration to cause tissue necrosis.
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spelling pubmed-21338032008-04-18 EXPERIMENTAL PRODUCTION OF DIGESTIVE TRACT ULCERATIONS Penner, Abraham Bernheim, Alice Ida J Exp Med Article We have attempted to reproduce in animal experiments a group of pathological findings which we have observed to be associated with shock. In order to simulate the compensatory vasomotor reactions occurring in shock, we have utilized the intraperitoneal injection of adrenalin hydrochloride in dogs, cats, rabbits and guinea pigs. That the effect of adrenalin hydrochloride when injected by this route is of long duration has been shown by the prolonged hyperglycemia which it produces. Our experiments have resulted in the production of a lesion in the digestive tract which is identical in the gross with those which we observed in our human material. The histological changes, however, have been found to differ from those encountered in the latter. These differences have been noted to occur only in the dog and cat, where the initial changes take place in the mucosa, and the alterations in the submucosa appear secondary to these. In the rabbit and guinea pig the histogenesis of the lesions is identical with that observed in man, the lesions first manifesting themselves in changes in the submucosa, congestion, edema and hernorrhage. Only later are similar changes seen in the mucosa, progressing finally to necrosis and ulceration. The cause of the histological differences has been found in the presence of arteriovenous anastomoses which occur in the submucosa in the case of the dog and cat and in the mucosa in the case of the rabbit, guinea pig and man. We have pointed out that variations in blood flow through the intestinal wall may result from the short circuiting of the blood through the arteriovenous anastomoses. This, associated with the vasoconstriction known to occur in shock, may if severe and prolonged, result in necrosis of the intestinal wall. We have experimentally reproduced the same lesion by the injection of adrenalin, which acts in a similar way. The experimentally produced anatomical changes offer additional evidence in support of the clinical occurrence of a vasospasm which is of sufficient severity and duration to cause tissue necrosis. The Rockefeller University Press 1939-10-31 /pmc/articles/PMC2133803/ /pubmed/19870922 Text en Copyright © Copyright, 1939, by The Rockefeller Institute for Medical Research New York This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Penner, Abraham
Bernheim, Alice Ida
EXPERIMENTAL PRODUCTION OF DIGESTIVE TRACT ULCERATIONS
title EXPERIMENTAL PRODUCTION OF DIGESTIVE TRACT ULCERATIONS
title_full EXPERIMENTAL PRODUCTION OF DIGESTIVE TRACT ULCERATIONS
title_fullStr EXPERIMENTAL PRODUCTION OF DIGESTIVE TRACT ULCERATIONS
title_full_unstemmed EXPERIMENTAL PRODUCTION OF DIGESTIVE TRACT ULCERATIONS
title_short EXPERIMENTAL PRODUCTION OF DIGESTIVE TRACT ULCERATIONS
title_sort experimental production of digestive tract ulcerations
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2133803/
https://www.ncbi.nlm.nih.gov/pubmed/19870922
work_keys_str_mv AT pennerabraham experimentalproductionofdigestivetractulcerations
AT bernheimaliceida experimentalproductionofdigestivetractulcerations