## Abstract ## BACKGROUND Hypoglycemia is a side effect of diabetes therapy and causes abnormal heart development. Embryonic heart cells are largely resistant to teratogenโinduced apoptosis. ## METHODS Hypoglycemia was tested for effects on cell death and cell proliferation in embryonic heart ce
CHANGES IN POLYAMINE METABOLISM DURING GLUCOCORTICOID-INDUCED PROGRAMMED CELL DEATH IN MOUSE THYMUS
โ Scribed by Cecilia Hegardt; Gunnar Andersson; Stina M. Oredsson
- Publisher
- Elsevier Science
- Year
- 2000
- Tongue
- English
- Weight
- 172 KB
- Volume
- 24
- Category
- Article
- ISSN
- 1065-6995
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โฆ Synopsis
Abstract
When mice are injected with dexamethasone, cortical thymocytes are deleted through programmed cell death (PCD). We have used this in vivo model system to investigate the kinetics of PCD and cell proliferation in relation to polyamine metabolism for 16h after injection of dexamethasone. As a marker for PCD, we used the appearance of a subโG~1~peak in the DNA histogram. When a subโG~1~peak appeared at 4h after dexamethasone treatment, the activity of the polyamine catabolic enzyme spermidine/spermine N^1^โacetyltransferase (SSAT) was significantly increased and the activity of the polyamine biosynthetic enzyme Sโadenosylmethionine decarboxylase (AdoMetDC) was significantly decreased compared to the activities found in the thymi of control mice. Despite the significant changes in the activities of SSAT and AdoMetDC, the only change in the polyamine pool during the experimental period was that of putrescine. Presumably the complexity of this in vivo system masks changes in the spermidine and spermine pools that were expected in relation to the increased SSAT activity and decreased AdoMetDC activity.
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