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鞘脂介导的白发小鼠模型体内Mitf表达恢复及色素再生

Sphingolipid-mediated restoration of Mitf expression and repigmentation in vivo in a mouse model of hair graying.

作者信息

Saha Bidisha, Singh Suman Kumar, Mallick Shampa, Bera Rabindranath, Datta Pijush K, Mandal Mriganka, Roy Syamal, Bhadra Ranjan

机构信息

Infectious Diseases and Immunology Division, Indian Institute of Chemical Biology, Jadavpur, Kolkata, India.

出版信息

Pigment Cell Melanoma Res. 2009 Apr;22(2):205-18. doi: 10.1111/j.1755-148X.2009.00548.x. Epub 2009 Jan 22.

DOI:10.1111/j.1755-148X.2009.00548.x
PMID:19207217
Abstract

Recent advances in the identification and characterisation of stem cell populations has led to substantial interest in understanding the precise triggers that would operate to induce activation of quiescent stem cells. Melanocyte stem cells (MSCs) reside in the bulge region of the hair follicles and are characterised by reduced expression of the microphthalmia-associated transcription factor (Mitf) and its target genes implicated in differentiation. Vitiligo is characterised by progressive destruction of differentiated melanocytes. However, therapies using UV irradiation therapy can induce a degree of repigmentation, suggesting that MSCs may be activated. As Mitf is implicated in control of proliferation, we have explored the possibility that inducing Mitf expression via lipid-mediated activation of the p38 stress-signalling pathway may represent a re-pigmentation strategy. Here we have isolated from placental extract a C18:0 sphingolipid able to induce Mitf and tyrosinase expression via activation of the p38 stress-signalling pathway. Strikingly, in age-onset gray-haired C57BL/6J mice that exhibit decaying Mitf expression, topical application of placental sphingolipid leads to increased Mitf in follicular melanocytes and fresh dense black hair growth. The results raise the possibility that lipid-mediated activation of the p38 pathway may represent a novel approach to an effective vitiligo therapy.

摘要

干细胞群体识别与特征鉴定方面的最新进展引发了人们对了解激活静止干细胞的精确触发因素的浓厚兴趣。黑素细胞干细胞(MSCs)位于毛囊的隆突区,其特征是小眼相关转录因子(Mitf)及其参与分化的靶基因表达降低。白癜风的特征是分化的黑素细胞逐渐被破坏。然而,紫外线照射疗法可诱导一定程度的色素再生,这表明MSCs可能被激活。由于Mitf参与增殖控制,我们探讨了通过脂质介导激活p38应激信号通路诱导Mitf表达可能代表一种色素再生策略的可能性。在此,我们从胎盘提取物中分离出一种C18:0鞘脂,它能够通过激活p38应激信号通路诱导Mitf和酪氨酸酶表达。令人惊讶的是,在表现出Mitf表达衰减的老年白发C57BL/6J小鼠中,局部应用胎盘鞘脂可导致毛囊黑素细胞中Mitf增加,并长出新鲜浓密的黑色毛发。这些结果提示,脂质介导的p38通路激活可能代表一种有效的白癜风治疗新方法。

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