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黑皮质素受体辅助蛋白2(MRAP2)与斑马鱼黑皮质素1受体(MC1R)相互作用,但对其药理学特性没有影响。

Melanocortin receptor accessory protein 2 (MRAP2) interplays with the zebrafish melanocortin 1 receptor (MC1R) but has no effect on its pharmacological profile.

作者信息

Cortés Raúl, Agulleiro Maria Josep, Navarro Sandra, Guillot Raúl, Sánchez Elisa, Cerdá-Reverter José Miguel

机构信息

Department of Fish Physiology and Biotechnology, Instituto de Acuicultura de Torre de la Sal, Consejo Superior de Investigaciones Científicas (IATS-CSIC), Ribera de Cabanes, Castellón, Spain.

Department of Fish Physiology and Biotechnology, Instituto de Acuicultura de Torre de la Sal, Consejo Superior de Investigaciones Científicas (IATS-CSIC), Ribera de Cabanes, Castellón, Spain.

出版信息

Gen Comp Endocrinol. 2014 May 15;201:30-6. doi: 10.1016/j.ygcen.2014.03.009. Epub 2014 Apr 5.

DOI:10.1016/j.ygcen.2014.03.009
PMID:24709359
Abstract

The melanocortin system is probably one of the most complex hormonal systems since it integrates agonist, encoded in the proopiomelanocortin precursor, endogenous antagonist, agouti signaling protein and agouti-related protein, five different G-protein coupled receptors and two accessory proteins. These accessory proteins interact with melanocortin receptors to allow traffic to the plasma membrane or to regulate the pharmacological profile. The MC1R fill the extension locus, which is primarily responsible for the regulation of pigmentation. In zebrafish, both MC1R and MRAP2 system are expressed in the skin. We demonstrate that zebrafish MC1R physically, or closely, interacts with the MRAP2 system, although this interaction did not result in modification of the studied pharmacological profile. However, progressive fasting induced skin darkening but also an upregulation of the MRAP2 expression in the skin, suggesting an unknown role for MRAP2a that could involve receptor desensitization processes. We also demonstrate that crowding stress induces skin darkening and a downregulation of MC1R expression in the skin.

摘要

黑皮质素系统可能是最复杂的激素系统之一,因为它整合了源自阿黑皮素原前体编码的激动剂、内源性拮抗剂刺鼠信号蛋白和刺鼠相关蛋白、五种不同的G蛋白偶联受体以及两种辅助蛋白。这些辅助蛋白与黑皮质素受体相互作用,以实现向质膜的转运或调节药理学特性。MC1R填补了延伸位点,该位点主要负责色素沉着的调节。在斑马鱼中,MC1R和MRAP2系统均在皮肤中表达。我们证明斑马鱼MC1R与MRAP2系统存在物理上或紧密的相互作用,尽管这种相互作用并未导致所研究的药理学特性发生改变。然而,渐进性禁食会导致皮肤变黑,同时皮肤中MRAP2的表达上调,这表明MRAP2a可能具有未知作用,可能涉及受体脱敏过程。我们还证明拥挤应激会导致皮肤变黑以及皮肤中MC1R表达下调。

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