Differential effects on membrane permeability and viability of human keratinocyte cells undergoing very low intensity megasonic fields
2017
Among different therapeutic applications of Ultrasound (US), transient membrane sonoporation (SP) - a
temporary, non-lethal porosity, mechanically induced in cell membranes through US exposure -
represents a compelling opportunity towards an efficient and safe drug delivery. Nevertheless,
progresses in this field have been limited by an insufficient understanding of the potential cytotoxic
effects of US related to the failure of the cellular repair and to the possible activation of inflammatory
pathway. In this framework we studied the in vitro effects of very low-intensity US on a human
keratinocyte cell line, which represents an ideal model system of skin protective barrier cells which
are the first to be involved during medical US treatments. Bioeffects linked to US application at 1 MHz
varying the exposure parameters were investigated by fluorescence microscopy and fluorescence
activated cell sorting. Our results indicate that keratinocytes undergoing low US doses can uptake drug
model molecules with size and efficiency which depend on exposure parameters. According to subcavitation
SP models, we have identified the range of doses triggering transient membrane SP, actually
with negligible biological damage. By increasing US doses we observed a reduced cells viability and an
inflammatory gene overexpression enlightening novel healthy relevant strategies.
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