AI Article Synopsis

  • The retinal pigment epithelium (RPE) is crucial for eye health by protecting photoreceptors and removing waste during light exposure.
  • Melatonin enhances the expression of key proteins like prohibitin and β-tubulin, affecting the RPE's cytoskeletal structure and aiding in oxidative stress protection.
  • The study suggests melatonin could be a promising treatment for ocular diseases such as age-related macular degeneration by promoting healthier RPE cell morphology and function.

Article Abstract

The retinal pigment epithelium (RPE) plays imperative roles in normal retinal function by photoreceptor protection from light and phagocytosis of rod and cone outer segments during disc shedding. Melatonin is the free radical scavenger and circadian determinant to protect the RPE and retina from oxidative stress and regulate the circadian clock. The current study tested the hypothesis whether melatonin could affect cytoskeletal structure within RPE. Our Western blot analysis demonstrated that melatonin treatment up-regulated prohibitin 3-fold compared to control. β-tubulin levels were also up-regulated by melatonin but to a lesser extent. Initial cell shape of ARPE-19 is epitheloid, however, after 30-minute treatment with melatonin, RPE cells undergo a morphological change to a fusiform shape with spindle outgrowth. Cells return to epitheloid shape after 12 hours in untreated medium. Melatonin treated cells showed increased and dissimilar distribution of prohibitin and β-tubulin compared to non-treated cells, thus altered cytoskeletal and mitochondrial structure in the RPE. Our data implies that melatonin may play a protective role under oxidative stress, which is shown by the marker prohibitin in terms of increased expression and nuclear distribution. During the protective process, cells change their morphology. Our results suggest that melatonin treatment could be beneficial to protect mitochondria under oxidative stress and treat certain ocular diseases, including age-related macular degeneration.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5568856PMC
http://dx.doi.org/10.14299/ijser.2017.07.001DOI Listing

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