Development of Novel Mouse Model of Ulcers Induced by Implantation of Magnets

Overview

Journal Sci Rep

Specialty Science

Date 2017 Jul 9

PMID 28687753

Citations 4

Authors

Yuriko Takeuchi

Koji Ueno

Takahiro Mizoguchi

Makoto Samura

Takasuke Harada

Atsunori Oga

Tomoaki Murata

Tohru Hosoyama

Noriyasu Morikage

Kimikazu Hamano

Affiliations

Soon will be listed here.

Abstract

We developed a novel mouse model of human refractory cutaneous ulcers that more faithfully reflects pathology and evaluated the effects of mixed cell sheets comprising peripheral blood mononuclear cells and fibroblasts, which we previously developed for treating refractory cutaneous ulcers. Model development involved sandwiching the skin between two magnets, one of which was implanted under the skin for 7 consecutive days. This magnet-implanted ulcer model produced persistently large amounts of exudate and induced the infiltration of the ulcer with inflammatory cells. The model mice had a thicker epidermis and impaired transforming growth factor-β (TGF-β) signaling followed by SMAD2 down-regulation, which causes epidermal hyperplasia in chronic ulcers. Impaired TGF-β signaling also occurred in the ulcers of critical limb ischemia patients. Mixed cell implantation in this ulcer model reduced TNF-α and IL-6 levels in the tissues surrounding the mixed cell sheet-treated ulcers compared with controls or mice treated with trafermin (FGF2). Seven days after commencing therapy, the epidermis was thinner in mice treated with the mixed cell sheets than in controls. This model may therefore serve as a clinically relevant model of human ulcers, and our mixed cell sheets may effectively relieve chronic inflammation and inhibit refractoriness mechanisms.

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