Inhibition of liver trans-sulphuration pathway by propargylglycine mimics gene expression changes found in the mammary gland of weaned lactating rats: role of glutathione
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Zaragozá Colom, Rosa; García de Mier, Concepción; Rus, Ariana Diana; Pallardó, Federico V.; Barber Sanchis, Teresa; Torres Asensi, Luis; Miralles Fernández, Vicente; Viña Ribes, Juan
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Aquest document és un/a article, creat/da en: 2003
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In the lactatingmammary gland, weaning produces mitochondrial
cytochrome c release and nuclear DNA fragmentation, as determined
by gel electrophoresis. This is followed by a significant
decrease in lactation. Weaning for 2 h produces an early induction
of the tumour suppressor/transcription factor p53, whereas
the oncoprotein c-Jun and c-Jun N-terminal kinase are elevated
after 24 h of weaning when compared with controls. The expression
of p21cip1 and p27kip1, cyclin-dependent kinase inhibitors, was
significantly higher in weaned rats when compared with control
lactating rats. All the changes mentioned above also happen in
the lactatingmammary gland when propargylglycine, an inhibitor
of the liver trans-sulphuration pathway, is administered. This
effect is partially reversed by N-acetylcysteine administration.
The administration of buthionine sulphoximine, an irreversible
inhibitor of γ -glutamylcysteine synthetase, to lactating rats
produces a decrease in GSH levels and changes in protein
concentrations and gene transcripts similar to those in rats with
impaired trans-sulphuration pathway. These data suggest that
the inter-tissue flux of GSH is an important mechanism of Lcysteine
delivery to the lactating mammary gland and emphasize
the importance of this physiological event inmaintaining the gene
expression required to sustain lactation.
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