Review on the possible pathophysiological mechanisms underlying visual display terminal-associated dry eye disease.
Ketil FjaervollHaakon FjaervollMorten Schjerven MagnoSara Tellefsen NølandDarlene A DarttJelle VehofTor P UtheimPublished in: Acta ophthalmologica (2022)
Visual display terminal (VDT) use appears to induce DED through both direct and indirect routes. Decreased blink rates and increased incomplete blinks increase the exposed ocular evaporative area and inhibit lipid distribution from meibomian glands. Although not adequately investigated, changes in parasympathetic signalling may impair lacrimal gland and goblet cell function, promoting tear film instability. More studies are needed to better target and improve the treatment and prevention of VDT-associated DED.