γ-Glutamyltranspeptidase in the Rat Liver after Portacaval Shunt

Colombo, J. P.; Peheim, E.; Bachmann, C.; Müller, Edith; Bircher, J

doi:10.1203/00006450-197601000-00004

Cited by 11 publications

(6 citation statements)

References 16 publications

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“…As a direct consequence of portal blood diversion liver shrinkage takes place, the size after 10 days remaining constant (8,10,17). The increased DNA content per unit liver weight in the PCS group and the control group with the same dietary intake compared to unoperated and sham-operated controls show that more cells are present per volume of liver weight.…”

Section: Discussionmentioning

confidence: 83%

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Enzymes of Ammonia Detoxication after Portacaval Shunt in the Rat

Berüter

Bachmann

et al. 1977

Enzyme

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At high systemic blood concentrations ammonia may be partially deviated into the pathway of pyrimidine synthesis, as has been observed in different genetic defects of the urea cycle. The portacaval shunt (PCS) rat presents an animal model to study ammonia detoxication without an underlying enzyme defect in the urea cycle. Since ammonia may induce a deviation into the pyrimidine pathway by influencing enzymatic reactions involved in this pathway, the activity of carbamylphosphate synthetase and aspartate transcarbamyiase in liver as well as the excretion of orotic acid in the urine were measured in rats 10, 20 and 30 days after PCS. The results suggest that in this experimental model ammonia may be channeled into the pyrimidine pathway leading to a stimulation of the first enzymatic step and to an increased excretion of orotic acid.

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Section: Discussionmentioning

confidence: 83%

“…A minor fraction of the circulatalone as has been suggested up to now (10), but may also be connected to the reduced food intake of these animals. It is not clear, however, whether the elevated amount of DNA is due to an augmented production of new but smaller and younger hepatocytes, or to shrinkage of the prevailing cells, or both.…”

Section: Discussionmentioning

confidence: 99%

Enzymes of Ammonia Detoxication after Portacaval Shunt in the Rat

Berüter

Bachmann

et al. 1977

Enzyme

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“…Weinbren (18) has demonstrated that portacaval shunting in rats can produce nodularity in the liver. Colombo et al (19) have shown that the liver parenchyma becomes positive for GGT after portacaval shunting but the enzymes appear primarily in the periportal zones rather than randomly in small foci of hepatocytes as seen in the model described by Solt et al (1). It seems, therefore, that the GGT positivity seen after shunting is in response to physiological modulation rather than a phenotypic marker for preneoplasia.…”

Section: Discussionmentioning

confidence: 98%

The Effect of Portal Diversion on the Early Stages of Liver Carcinogenesis in the Rat

et al. 1982

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The effect of portal diversion by ameroid constriction was studied in the carcinogenic process in the rat after initiation of foci by diethylnitrosamine and after the establishment of putative preneoplastic nodules. Portal diversion or portal diversion plus partial hepatectomy did not act to promote or select for the development of nodules. Furthermore, portal diversion did not alter the natural history of established nodules. These results suggest that vascular factors are not important at these early stages of the carcinogenic process in the rat liver.The theory of multistep progression of carcinogenesis in the liver has recently gained increasing prominence in the literature. Solt et al. (1) have demonstrated that small numbers of liver cells are altered by a single exposure to carcinogens such as diethylnitrosamine (DENA) and that the alteration is "fixed" by a round of cell proliferation. Once "initiation" occurs, these altered cells are capable of proliferation in an environment which inhibits growth of normal surrounding cells, allowing hyperplastic putative preneoplastic nodules to develop (2). The nodules are morphologically and histochemically different from the surrounding liver and are easily identifiable by y-glutamyl transpeptidase (GGT) staining (1, 3). The subsequent fate of the nodules is variable (3); the majority undergo a process of maturation and remodeling and eventually merge with the surrounding liver. A few persist and some develop into hepatocellular carcinomas.One problem with this model is that in order to "select" for development of nodules from initiated cells, conditions must be produced which stimulate liver proliferation but inhibit growth of the normal cells. Farber (2) has used a diet of 0.2% acetylaminofluorene (2-AAF) combined with partial hepatectomy or CCL administration. 2-AAF inhibits the growth of normal liver, but does not do so to the putative preneoplastic-initiated cells which are resistant to this agent (1, 4). 2-AAF is in itself a carcinogen, and this fact is one of the disadvantages of the model for some types of studies.A further problem is that there is variability in the

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“…Whether there exists a common denominator to the elevation of hepatic GGT in PCS and in chemically induced hepatocarcinogenesis is not known. The hypothesis that both procedures represent the reacquisition of a fetal, biochemical feature which is normally repressed in the adult is therefore difficult to prove or disprove (8,9). Everts et al believe that after PCS, the distribution of GGT is periportal, whereas after the administration of chemical carcinogens the enzyme is mostly concentrated in the midzonal areas.…”

Section: Commentsmentioning

confidence: 99%

Portacaval shunt and the reacquisition of γ-glutamyl transpeptidase activity

Colombo

1987

Hepatology

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Portacaval shunt (PCS) operations were performed on male inbred SD rats. The activity of liver γ‐glutamyltranspeptidase (GGT) increased a few days after the operation and remained high after several months. However, the activity was only present in periportal areas of liver lobules and was mainly restricted to the endothelial lining cells of periportal blood vessels. Phenobarbital sodium (CAS: 57–03–7) administration did not change the distribution of GGT. The activity of liver glucose‐6‐phosphatase disappeared in the centrilobular area a few days after the operation but was present in the periportal areas. The distribution of this activity returned to normal after several months. The capacity of liver cells to store glycogen was significantly decreased following the PCS operation. Morphologic changes in hepatocytes observed after the PCS operation did not show similarities to those seen in preneoplastic livers. The nuclei of the small compact hepatocytes found in the animals with PCS were irregular in shape and stained intensively with hematoxylin and eosin. The large pale‐staining cells in the periphery of liver lobes were GGT negative and their nuclei had a normal morphology. Neither morphologic nor histochemical changes consistent with preneoplastic and/or neoplastic stage were observed after 10 months in the liver when the PCS operation was performed on rats having received an ip dose (10 mg/kg) of diethylnitrosamine (CAS: 55–18–5) 2 weeks prior to the operation.

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γ-Glutamyltranspeptidase in the Rat Liver after Portacaval Shunt

Cited by 11 publications

References 16 publications

Enzymes of Ammonia Detoxication after Portacaval Shunt in the Rat

Enzymes of Ammonia Detoxication after Portacaval Shunt in the Rat

The Effect of Portal Diversion on the Early Stages of Liver Carcinogenesis in the Rat

Portacaval shunt and the reacquisition of γ-glutamyl transpeptidase activity

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