| Literature DB >> 30185909 |
Masakazu Kurita1,2, Toshikazu Araoka1,3, Tomoaki Hishida1, David D O'Keefe1, Yuta Takahashi1, Akihisa Sakamoto1,3, Masahiro Sakurai1,3, Keiichiro Suzuki1, Jun Wu1, Mako Yamamoto1, Reyna Hernandez-Benitez1, Alejandro Ocampo1, Pradeep Reddy1, Maxim Nikolaievich Shokhirev4, Pierre Magistretti5, Estrella Núñez Delicado3, Hitomi Eto2, Kiyonori Harii2, Juan Carlos Izpisua Belmonte6.
Abstract
Large cutaneous ulcers are, in severe cases, life threatening1,2. As the global population ages, non-healing ulcers are becoming increasingly common1,2. Treatment currently requires the transplantation of pre-existing epithelial components, such as skin grafts, or therapy using cultured cells2. Here we develop alternative supplies of epidermal coverage for the treatment of these kinds of wounds. We generated expandable epithelial tissues using in vivo reprogramming of wound-resident mesenchymal cells. Transduction of four transcription factors that specify the skin-cell lineage enabled efficient and rapid de novo epithelialization from the surface of cutaneous ulcers in mice. Our findings may provide a new therapeutic avenue for treating skin wounds and could be extended to other disease situations in which tissue homeostasis and repair are impaired.Entities:
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Year: 2018 PMID: 30185909 DOI: 10.1038/s41586-018-0477-4
Source DB: PubMed Journal: Nature ISSN: 0028-0836 Impact factor: 49.962