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Astrocytes prevent neuronal death induced by reactive oxygen and nitrogen species

✍ Scribed by Junya Tanaka; Kazuko Toku; Bo Zhang; Ken Ishihara; Masahiro Sakanaka; Nobuji Maeda


Publisher
John Wiley and Sons
Year
1999
Tongue
English
Weight
653 KB
Volume
28
Category
Article
ISSN
0894-1491

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✦ Synopsis


Reactive oxygen and nitrogen species (RO/NS) such as nitric oxide (NO), hydroxyl radical (OHβ€’), and superoxide anion (O 2 Οͺ ) are generated in a variety of neuropathological processes and damage neurons. In the present study, we investigated the neuroprotective effects of rat astrocytes against RO/NS-induced damage using neuron-glia cocultures, and the effects were compared to those of microglial cells. Sodium nitroprusside (SNP), 3-morpholinosydnonimine (SIN-1), and FeSO 4 were used to generate NO, O 2 Οͺ and NO, and OHβ€’, respectively. Solely cultured neurons, which were transiently exposed to these agents, degenerated, possibly through apoptotic mechanisms as revealed by in situ detection of DNA fragmentation, whereas neurons cocultured with either astrocytes or microglial cells were viable even after exposure to RO/NS. In contrast, most neurons cocultured with meningeal fibroblasts degenerated. Astrocyte-conditioned medium partially attenuated RO/NS-induced neuronal damage. When neurons were cultured on astrocyte-derived extracellular matrix (AsECM), neuronal death induced by SNP and FeSO 4 was almost completely inhibited. AsECM contained significant amounts of laminin and fibronectin, and pure fibronectin and laminin also protected neurons against RO/NS-induced damage in the same manner as AsECM. These results suggest that astrocytes can protect neurons against RO/NSinduced damage by secreting soluble and insoluble factors.


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