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Exploring a role for regulatory miRNAs in wound healing during ageing: involvement of miR-200c in wound repairAunin, Eerik, Broadley, David, Ahmed, Mohammed I., Mardaryev, Andrei N., Botchkareva, Natalia V. 12 June 2017 (has links)
Yes / Multiple factors and conditions can lead to impaired wound healing. Chronic non-healing wounds
are a common problem among the elderly. To identify microRNAs negatively impacting the wound
repair, global miRNA profiling of wounds collected from young and old mice was performed. A
subset of miRNAs that exhibited an age-dependent expression pattern during wound closure was
identified, including miR-31 and miR-200c. The expression of miR-200 family members was markedly
downregulated upon wounding in both young and aged mice, with an exception of acute
upregulation of miR-200c at the early phase of wound healing in aged skin. In unwounded aged skin
(versus unwounded younger skin), the level of miR-200c was also found elevated in both human and
mice. Overexpression of miR-200c in human ex vivo wounds delayed re-epithelialisation and
inhibited cell proliferation in the wound epithelium. Modulation of miR-200c expression in both
human and mouse keratinocytes in vitro revealed inhibitory effects of miR-200c on migration, but
not proliferation. Accelerated wound closure in vitro induced by anti-miR-200c was associated with
upregulation of genes controlling cell migration. Thus, our study identified miR-200c as a critical
determinant that inhibits cell migration during skin repair after injury and may contribute to ageassociated
alterations in wound repair. / Supported by a grant from Medical Research Council UK (MR/K011324/1)
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OPTIMIZATION OF NON-VIRAL GENE DELIVERY SYSTEM FOR IMAGE-GUIDED THERAPY FOR TRIPLE NEGATIVE BREAST CANCERSchilb, Andrew L. 30 August 2021 (has links)
No description available.
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