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Gamma-linolenic
acid (GLA) is cytotoxic to 36B10 malignant rat astrocytoma cells but not to
'normal' rat astrocytes
Vartak S, McCaw R, Davis CS, Robbins ME, Spector AA
Radiation Research Laboratory, Department of Radiology,
University of Iowa, Iowa City 52242, USA
This study compares the effect of gamma-linolenic acid (GLA) and its
precursor linoleic acid (LA) on survival of 36B10 malignant rat astrocytoma
cells and 'normal' rat astrocytes.
GLA was cytotoxic to 36B10 cells but not to astrocytes.
By contrast, LA supplementation did not affect the survival of either cell
types.
There were minor differences in the uptake, distribution and use of
radiolabelled GLA and LA by the 36B10 cells and astrocytes.
GLA and LA supplementation increased the total polyunsaturated fatty acid (PUFA)
content of the cells indicating increased oxidative potential.
However, elevated levels of 8-isoprostane, an indicator of increased oxidative
stress, were only observed in the GLA supplemented 36B10 cells.
Addition of the antioxidant trolox to GLA-enriched 36B10 cells blocked the
cytotoxic effect.
Further, GLA enhanced the radiation sensitivity of the astrocytoma cells but not
the astrocytes; trolox blocked the GLA-mediated increase in astrocytoma cell
radiosensitivity.
LA did not affect the radiation response of either cell type.
While cyclo-oxygenase inhibitors did not affect GLA cytotoxicity, they blocked
the enhanced radiation response of GLA-supplemented cells.
The lipoxygenase inhibitor NDGA did not affect the toxicity produced by GLA.
Thus, GLA is toxic to the neoplastic astrocytoma cells but not to normal
astrocytes.
PMID: 9635836 [PubMed - indexed for MEDLINE]
Source:
http://www.ncbi.nlm.nih.gov/entrez/query.fcgi?cmd=Retrieve&db=PubMed&list_uids=9635836&dopt=Abstract
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