Prof. Akasaka (front row, second from right) and members of the Department of Pathology
Figure 1. Attenuation of dermal fibrosis by miRNA146b-5p in skin wounds. The proportion of fibrotic area in miRNA146b-5p mimic-treated wounds was significantly smaller than that in scrambled RNA-treated wounds. In contrast, the proportion of fibrotic area at day 10 in miRNA146b-5p inhibitor-treated wounds was significantly larger than that in scrambled RNA-treated wounds. Y. Akasaka et al. The role for miRNA146b-5p in the attenuation of dermal fibrosis and angiogenesis by targeting PDGFRα in skin wounds. Reprinted with permission from https://doi.org/10.1016/j.jid.2021.11.037.
Figure 2. Wound adipose tissue cells exhibit CD81 exosomes containing miRNA146b-5p. Combined staining with miRNA146b-5p (red) and CD81 (green) highlights double-positive granules for CD81 and miRNA146b-5p (yellow) in the adipose tissue cells of mimic-transfected wounds. Y. Akasaka et al. The role for miRNA146b-5p in the attenuation of dermal fibrosis and angiogenesis by targeting PDGFRα in skin wounds. Reprinted with permission from https://doi.org/10.1016/j.jid.2021.11.037.
Figure 3. miRNA146b-5p-targeted repression of PDGFRα in adipose tissue cells can lead to a loss of their PDGFRα-induced profibrotic activities, resulting in reduction in skin wound fibrosis. MF, myofibroblast; SMA, smooth muscle actin. Y. Akasaka et al. The role for miRNA146b-5p in the attenuation of dermal fibrosis and angiogenesis by targeting PDGFRα in skin wounds. Reprinted with permission from https://doi.org/10.1016/j.jid.2021.11.037.
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