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首页> 外文期刊>Journal of Pharmacy and Pharmacology >β-Cryptoxanthin suppresses UVB-induced melanogenesis in mouse: Involvement of the inhibition of prostaglandin E 2 and melanocyte-stimulating hormone pathways
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β-Cryptoxanthin suppresses UVB-induced melanogenesis in mouse: Involvement of the inhibition of prostaglandin E 2 and melanocyte-stimulating hormone pathways

机译:β-隐黄质抑制小鼠中UVB诱导的黑色素生成:涉及前列腺素E 2的抑制和刺激黑色素细胞的激素途径

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Objective β-cryptoxanthin (β-CPX) is a carotenoid that is widely contained in the fruits of citrus plants. We evaluated the effect of β-CPX on UVB-induced pigmentation and mRNA expression related to melanogenesis in mouse skin. In addition, changes in melanogenic molecules were evaluated in cultured melanocytes stimulated with prostaglandin (PG) E 2, melanocyte-stimulating hormone (MSH) and endothelin (ET)-1. Methods Mice were irradiated with UVB and were given β-CPX (0.1, 1 and 10 mg/kg) orally for 14 days. Pigmentation was evaluated by skin colour change and microscopic observation. Total RNA was obtained from the skin and the expression of melanogenic mRNA was evaluated by RT-PCR. In cell culture studies, human melanocytes were cultured with β-CPX and melanogenic stimulants (PGE 2, MSH and ET-1) for 6-10 days. Melanin contents, dendricity, melanogenic mRNA and phosphorylation of cyclic AMP response element-binding protein (CREB) were evaluated. Key findings β-CPX (10 mg/kg) significantly suppressed skin pigmentation and mRNA expression of cyclooxygenase-2, ET-1 receptors, low-affinity neurotrophin receptor, PGE 2 receptor (EP1), melanocortin 1 receptor (MC1R), tyrosinase (Tyr), tyrosinase-related protein (Tyrp) 1 and microphthalmia transcription factor. β-CPX (10 μg/ml) suppressed melanogenesis induced by PGE 2, MSH and ET-1. In the PGE 2-stimulated melanocytes, mRNA expressions of EP-1, Tyr and Tyrp1 and phosphorylation of CREB protein were suppressed. In the ET-1-stimulated cells, only expression of CREB protein was suppressed. In the MSH-induced cells, mRNA expression of MC1R and Tyrp1 and protein expression of CREB were suppressed. Conclusion Oral administration of β-CPX was found to suppress UVB-induced melanogenesis. Suppression of melanogenic enzymes, receptors of melanogenic stimulators, expression and phosphorylation of CREB are thought to be involved in the mechanism.
机译:目的β-隐黄质(β-CPX)是类胡萝卜素,广泛存在于柑橘类植物的果实中。我们评估了β-CPX对UVB诱导的色素沉着和小鼠皮肤黑色素生成相关mRNA表达的影响。此外,评估了用前列腺素(PG)E 2,刺激黑素细胞的激素(MSH)和内皮素(ET)-1刺激的培养的黑素细胞中黑素生成分子的变化。方法用紫外线B照射小鼠,口服β-CPX(0.1、1和10 mg / kg)14天。通过皮肤颜色变化和显微镜观察评价色素沉着。从皮肤获得总RNA,并通过RT-PCR评估黑色素mRNA的表达。在细胞培养研究中,人类黑素细胞与β-CPX和黑色素刺激物(PGE 2,MSH和ET-1)一起培养6-10天。评估了黑色素的含量,树突,黑色素mRNA和环状AMP反应元件结合蛋白(CREB)的磷酸化。主要发现β-CPX(10 mg / kg)显着抑制皮肤色素沉着和环氧合酶-2,ET-1受体,低亲和力神经营养蛋白受体,PGE 2受体(EP1),黑皮质素1受体(MC1R),酪氨酸酶( Tyr),酪氨酸酶相关蛋白(Tyrp)1和小眼症转录因子。 β-CPX(10μg/ ml)抑制了PGE 2,MSH和ET-1诱导的黑色素生成。在PGE 2刺激的黑色素细胞中,EP-1,Tyr和Tyrp1的mRNA表达以及CREB蛋白的磷酸化受到抑制。在ET-1刺激的细胞中,仅CREB蛋白的表达被抑制。在MSH诱导的细胞中,MC1R和Tyrp1的mRNA表达和CREB的蛋白表达受到抑制。结论口服β-CPX可抑制UVB诱导的黑色素生成。黑色素生成酶的抑制,黑色素生成刺激物的受体,CREB的表达和磷酸化被认为与该机制有关。

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