Background: Iron supplementation is recommended during pregnancy to meet the needs of the rapidly growing fetus.
However, its intake is associated with the generation of destructive free radicals, i.e., oxidative damage to the fetal
brain. Folic acid supplementation is needed during pregnancy to reduce the risk of neural tube defects. Hypothesis:
Intake of folic acid can ameliorate the morphological features of cell damage in the striatal tissue (brain of neonatal
rats) associated with the intake of iron. Objectives and methods: To test this hypothesis, an animal model (pregnant
Albino rats) was established. The animals were divided into three groups: group A, control animals treated with
saline only; group B, animals treated with iron gluconate; and group C, animals treated concomitantly with iron
gluconate and folic acid. The striatal brain tissues of the neonates were examined for features of cellular damage,
using immunohistological and ultrastructural methods. Results: The authors found significant variations among the
three groups. The intake of iron (group B) and its deposition in the striatal tissue (neurons and glial cells) was associated
with changes indicative of both cellular injury and regeneration. The former includes neuronal apoptosis and
necrosis, and destruction of the organelles, including the mitochondria, endoplasmic reticulum, Golgi apparatus, and
lysosomes of the neurons and glial cells. The latter includes microgliosis, astrogliosis, upregulation of glial fibrillary
acidic protein, and inducible nitric oxide synthase. These changes were absent in the striatal tissue of the control
group (group A) and in animals treated concomitantly with both iron gluconate and folic acid (group C). Conclusion:
Intake of folic acid can protect the neonatal striatal tissue against iron-induced oxidative stress damage.
Research Department	
              
          Research Journal	
              Ultrastructural Pathology
          Research Member	
          
      Research Rank	
              1
          Research Vol	
              Vol. 36. No.2
          Research Year	
              2012
          Research_Pages	
              PP. 89–101
          Research Abstract	
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