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蜂毒刺激人类黑素细胞的增殖、黑素生成、树突形成和迁移。

Bee venom stimulates human melanocyte proliferation, melanogenesis, dendricity and migration.

作者信息

Jeon Songhee, Kim Nan Hyung, Koo Byung Soo, Lee Hyun Joo, Lee Ai Young

机构信息

Dongguk University Research Institute of Biotechnology, Medical Science Research Center, Goyang 410-773, Korea.

出版信息

Exp Mol Med. 2007 Oct 31;39(5):603-13. doi: 10.1038/emm.2007.66.

Abstract

Pigmentation may result from melanocyte proliferation, melanogenesis, migration or increases in dendricity. Recently, it has been reported that secreted phospholipase A(2)(sPLA(2)) known as a component of bee venom (BV), stimulates melanocyte dendricity and pigmentation. BV has been used clinically to control rheumatoid arthritis and to ameliorate pain via its anti-inflammatory and antinociceptive properties. Moreover, after treatment with BV, pigmentation around the injection sites was occasionally observed and the pigmentation lasted a few months. However, no study has been done about the effect of BV on melanocytes. Thus, in the present study, we examined the effect of BV on the proliferation, melanogenesis, dendricity and migration in normal human melanocytes and its signal transduction. BV increased the number of melanocytes dose and time dependently through PKA, ERK, and PI3K/Akt activation. The level of cAMP was also increased by BV treatment. Moreover, BV induced melanogenesis through increased tyrosinase expression. Furthermore, BV induced melanocyte dendricity and migration through PLA(2) activation. Overall, in this study, we demonstrated that BV may have an effect on the melanocyte proliferation, melanogenesis, dendricity and migration through complex signaling pathways in vitro, responsible for the pigmentation. Thus, our study suggests a possibility that BV may be developed as a therapeutic drug for inducing repigmentation in vitiligo skin.

摘要

色素沉着可能由黑素细胞增殖、黑素生成、迁移或树突增多引起。最近,有报道称,作为蜂毒(BV)成分之一的分泌型磷脂酶A2(sPLA2)可刺激黑素细胞树突增多和色素沉着。BV已在临床上用于控制类风湿性关节炎,并通过其抗炎和抗伤害感受特性来减轻疼痛。此外,用BV治疗后,偶尔会观察到注射部位周围出现色素沉着,且这种色素沉着会持续几个月。然而,尚未有关于BV对黑素细胞影响的研究。因此,在本研究中,我们检测了BV对正常人黑素细胞增殖、黑素生成、树突增多和迁移的影响及其信号转导。BV通过激活PKA、ERK和PI3K/Akt,剂量和时间依赖性地增加黑素细胞数量。BV处理还会增加cAMP水平。此外,BV通过增加酪氨酸酶表达诱导黑素生成。此外,BV通过激活PLA2诱导黑素细胞树突增多和迁移。总体而言,在本研究中,我们证明BV在体外可能通过复杂的信号通路对黑素细胞增殖、黑素生成、树突增多和迁移产生影响,这与色素沉着有关。因此,我们的研究表明BV有可能被开发为一种治疗药物,用于诱导白癜风皮肤复色。

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