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糖皮质激素和盐皮质激素受体在皮肤病理生理学中的作用。

Roles of the Glucocorticoid and Mineralocorticoid Receptors in Skin Pathophysiology.

机构信息

Instituto de Biomedicina de Valencia (IBV)-CSIC, 46010 Valencia, Spain.

出版信息

Int J Mol Sci. 2018 Jun 29;19(7):1906. doi: 10.3390/ijms19071906.

Abstract

The nuclear hormone receptor (NR) superfamily comprises approximately 50 evolutionarily conserved proteins that play major roles in gene regulation by prototypically acting as ligand-dependent transcription factors. Besides their central role in physiology, NRs have been largely used as therapeutic drug targets in many chronic inflammatory conditions and derivatives of their specific ligands, alone or in combination, are frequently prescribed for the treatment of skin diseases. In particular, glucocorticoids (GCs) are the most commonly used compounds for treating prevalent skin diseases such as psoriasis due to their anti-proliferative and anti-inflammatory actions. However, and despite their therapeutic efficacy, the long-term use of GCs is limited because of the cutaneous adverse effects including atrophy, delayed wound healing, and increased susceptibility to stress and infections. The GC receptor (GR/) and the mineralocorticoid receptor (MR/) are members of the NR subclass NR3C that are highly related, both structurally and functionally. While the GR is ubiquitously expressed and is almost exclusively activated by GCs; an MR has a more restricted tissue expression pattern and can bind GCs and the mineralocorticoid aldosterone with similar high affinity. As these receptors share 95% identity in their DNA binding domains; both can recognize the same hormone response elements; theoretically resulting in transcriptional regulation of the same target genes. However, a major mechanism for specific activation of GRs and/or MRs is at the pre-receptor level by modulating the local availability of active GCs. Furthermore, the selective interactions of each receptor with spatio-temporally regulated transcription factors and co-regulators are crucial for the final transcriptional outcome. While there are abundant genome wide studies identifying GR transcriptional targets in a variety of tissue and cell types; including keratinocytes; the data for MR is more limited thus far. Our group and others have studied the role of GRs and MRs in skin development and disease by generating and characterizing mouse and cellular models with gain- and loss-of-function for each receptor. Both NRs are required for skin barrier competence during mouse development and also play a role in adult skin homeostasis. Moreover, the combined loss of epidermal GRs and MRs caused a more severe skin phenotype relative to single knock-outs (KOs) in developing skin and in acute inflammation and psoriasis, indicating that these corticosteroid receptors play cooperative roles. Understanding GR- and MR-mediated signaling in skin should contribute to deciphering their tissue-specific relative roles and ultimately help to improve GC-based therapies.

摘要

核激素受体 (NR) 超家族包含大约 50 种进化上保守的蛋白质,它们主要作为配体依赖性转录因子发挥作用,在基因调控中发挥重要作用。除了在生理学中的核心作用外,NR 还被广泛用作许多慢性炎症疾病的治疗药物靶点,其特定配体的衍生物单独或联合使用,常用于治疗皮肤病。特别是糖皮质激素 (GCs) 是治疗银屑病等常见皮肤病最常用的化合物,因为它们具有抗增殖和抗炎作用。然而,尽管它们具有治疗效果,但由于皮肤不良反应,包括萎缩、伤口愈合延迟以及对压力和感染的敏感性增加,长期使用 GCs 受到限制。GC 受体 (GR/) 和盐皮质激素受体 (MR/) 是 NR3C 亚类 NR 的成员,它们在结构和功能上高度相关。虽然 GR 广泛表达,几乎仅被 GCs 激活;MR 则具有更有限的组织表达模式,并且可以与 GCs 和盐皮质激素醛固酮以相似的高亲和力结合。由于这些受体在 DNA 结合域具有 95%的同源性;两者都可以识别相同的激素反应元件;理论上导致相同靶基因的转录调控。然而,GR 和/或 MR 的特异性激活的主要机制是在受体前水平,通过调节活性 GCs 的局部可用性。此外,每个受体与时空调节转录因子和共调节剂的选择性相互作用对于最终的转录结果至关重要。虽然有大量的全基因组研究确定了各种组织和细胞类型中 GR 的转录靶标,包括角质形成细胞;但迄今为止,MR 的数据更为有限。我们的小组和其他小组通过生成和表征具有每个受体功能获得和功能丧失的小鼠和细胞模型,研究了 GR 和 MR 在皮肤发育和疾病中的作用。这两种 NR 都需要在小鼠发育过程中维持皮肤屏障功能,并且在成人皮肤稳态中也发挥作用。此外,与单敲除 (KO) 相比,表皮 GR 和 MR 的联合缺失导致在发育中的皮肤和急性炎症和银屑病中表现出更严重的皮肤表型,表明这些皮质类固醇受体发挥协同作用。了解 GR 和 MR 介导的皮肤信号转导应该有助于阐明它们在组织中的相对作用,并最终有助于改善基于 GC 的治疗方法。

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