Tyrosinase induction and inactivation in normal cultured human melanocytes by endothelin-1.

A Monji, H Inoue, H Oshima, M Aihara, M Tomioka, N Kumagai
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Abstract

Since endothelin was found to be expressed in epithelial cells as well as in vascular endothelial cells, the functional regulation of melanocytes with endothelin has been actively investigated. In particular, it has been suggested that endothelin may influence pigmentation and depigmentation, which are mediated by melanocytes. In the present study, we investigated the regulation of melanocyte function and tyrosinase expression by endothelin from the point of view of tyrosinase protein expression and enzyme activity. The influence of endothelins on melanocyte function was assessed. Melanocytes showed a dose-dependent increase in cell proliferation with the addition of endothelin-1. When the confluence of melanocytes was cultured with endothelin-1 for 72 h, tyrosinase activity in melanocytes was significantly and dose-dependently decreased. In contrast, there was no significant change with endothelin-3. However, tyrosinase protein expression of melanocytes was significantly and dose-dependently increased by endothelin-1, but endothelin-3 had no effect. Both the suppression of enzyme activity and the enhanced protein expression were regulated by the ETA receptor antagonist, BQ123. In view of these observations, we conclude that endothelin-1-induced tyrosinase is mediated by ETA receptors. However, the reason for the decrease in the specific activity of tyrosinase remains unknown, and our results suggest that another mechanism underlying the activation of tyrosinase is present in addition to the inductive action of endothelin-1 on tyrosinase.

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内皮素-1对正常培养人黑素细胞酪氨酸酶的诱导和失活。
由于内皮素在上皮细胞和血管内皮细胞中均有表达,因此内皮素对黑素细胞的功能调控已被积极研究。特别是,有人认为内皮素可能影响由黑素细胞介导的色素沉着和脱色。本研究从酪氨酸酶蛋白表达和酶活性的角度探讨了内皮素对黑素细胞功能和酪氨酸酶表达的调节作用。评估内皮素对黑素细胞功能的影响。随着内皮素-1的加入,黑素细胞的增殖呈剂量依赖性增加。内皮素-1与黑素细胞融合培养72 h后,黑素细胞酪氨酸酶活性显著且呈剂量依赖性降低。内皮素-3无明显变化。然而,内皮素-1可显著且剂量依赖性地增加黑素细胞酪氨酸酶蛋白的表达,而内皮素-3则无影响。ETA受体拮抗剂BQ123对酶活性的抑制和蛋白表达的增强均有调控作用。鉴于这些观察结果,我们认为内皮素-1诱导的酪氨酸酶是由ETA受体介导的。然而,酪氨酸酶特异性活性下降的原因尚不清楚,我们的研究结果表明,除了内皮素-1对酪氨酸酶的诱导作用外,酪氨酸酶激活的另一种机制也存在。
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