Postnatal hypobaric hypoxia in rats impairs water maze learning and the morphology of neurones and macroglia in cortex and hippocampus.

Behav Brain Res

Department of Neuroscience, Center for Cell Therapy and Tissue Repair, Charles University, Second Medical Faculty, 150 18 Prague 5, Czech Republic.

Published: May 2003

AI Article Synopsis

  • Newborn rats exposed to intermittent hypobaric hypoxia showed impaired spatial memory during tests conducted from postnatal days 23 to 32 and 100 to 109, with longer escape latencies compared to controls.
  • Exposure led to an increase in the number of neuronal bodies in certain cortical layers but did not change the overall number of neuronal bodies across the cortex, while also causing a loss of typical organization of neuronal and macroglial processes in the hippocampus.
  • In adult hypoxic rats, neuronal body counts and macroglial immunostaining levels normalized to control levels, but abnormalities in astrocytic and oligodendrocytic processes persisted in the hippocampus, indicating lasting effects on brain maturation and memory capabilities.

Article Abstract

Newborn rats were exposed to intermittent hypobaric hypoxia from birth until the age of 19 days. Spatial memory was tested in a Morris water maze from postnatal day (P) 23 to P32 and from P100 to P109. From P24 to P27 and on days P100 and P101, the escape latencies of hypoxic animals were longer than those of controls. At P24, the number of neuronal bodies increased in cortical layer II of the somatosensory, motor, and auditory areas, and in layer V of the motor area, but the number of neuronal bodies throughout the whole cortical thickness was unchanged. Decreases in the immunostaining density for neurofilaments (anti-NF 160), astrocytes (anti-GFAP), and oligodendrocytes (RIP) were found in the hippocampus, and the typical parallel organisation of neuronal and macroglial processes was lost. Decreases in immunostaining for neurofilaments and oligodendrocytes were also found in the somatosensory cortex and motor cortex. In adult hypoxic rats, at P114-P240, the number of neuronal bodies and the immunostaining density for neurofilaments, astrocytes, and oligodendrocytes in the examined areas were similar to adult controls; however, in the hippocampus we found hypertrophy of fine astrocytic processes and a decreased number of oligodendrocytic processes. We conclude that the neonatal brain damage induced by hypobaric hypoxia impairs spatial memory in infant as well as adult rats. Hypobaric hypoxia delays the maturation of neurones and substantially affects macroglia in the cortex and hippocampus.

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http://dx.doi.org/10.1016/s0166-4328(02)00366-2DOI Listing

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