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Postnatal irradiation-induced hippocampal neuropathology, cognitive impairment and aging. | LitMetric

Postnatal irradiation-induced hippocampal neuropathology, cognitive impairment and aging.

Brain Dev

Temasek Laboratories, National University of Singapore, 5A, Engineering Drive 1, Singapore 117411, Singapore.

Published: April 2017

AI Article Synopsis

  • Early brain irradiation can trigger lasting abnormal development, negatively impacting quality of life and leading to cognitive impairment and aging in individuals.
  • Studies on animals show that even low doses of postnatal brain irradiation can hinder neurogenesis and cause neuronal loss, neuroinflammation, and changes in blood vessel formation in the brain.
  • Understanding the molecular effects of radiation, particularly at low doses, could uncover mechanisms behind these negative impacts and inform future diagnostics and therapies to mitigate cognitive decline related to radiation exposure.

Article Abstract

Irradiation of the brain in early human life may set abnormal developmental events into motion that last a lifetime, leading to a poor quality of life for affected individuals. While the effect of irradiation at different early developmental stages on the late human life has not been investigated systematically, animal experimental studies suggest that acute postnatal irradiation with ⩾0.1Gy may significantly reduce neurogenesis in the dentate gyrus and endotheliogenesis in cerebral vessels and induce cognitive impairment and aging. Fractionated irradiation also reduces neurogenesis. Furthermore, irradiation induces hippocampal neuronal loss in CA1 and CA3 areas, neuroinflammation and reduces gliogenesis. The hippocampal neurovascular niche and the total number of microvessels are also changed after radiation exposures. Each or combination of these pathological changes may cause cognitive impairment and aging. Interestingly, acute irradiation of aged brain with a certain amount of radiation has also been reported to induce brain hormesis or neurogenesis. At molecular levels, inflammatory cytokines, chemokines, neural growth factors, neurotransmitters, their receptors and signal transduction systems, reactive oxygen species are involved in radiation-induced adverse effect on brain development and functions. Further study at different omics levels after low dose/dose rate irradiation may not only unravel the mechanisms of radiation-induced adverse brain effect or hormesis, but also provide clues for detection or diagnosis of radiation exposure and for therapeutic approaches to effectively prevent radiation-induced cognitive impairment and aging. Investigation focusing on radiation-induced changes of critical brain development events may reveal many previously unknown adverse effects.

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Source
http://dx.doi.org/10.1016/j.braindev.2016.11.001DOI Listing

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