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肿瘤坏死因子-α、干扰素-γ和 P 物质是人类皮肤中脑垂体以外催乳素表达的新型调节因子。

Tumour necrosis factor alpha, interferon gamma and substance P are novel modulators of extrapituitary prolactin expression in human skin.

机构信息

Dermatology Research Centre, Manchester Academic Health Science Centre, and Institute of Inflammation and Repair, University of Manchester, Manchester, United Kingdom.

出版信息

PLoS One. 2013 Apr 23;8(4):e60819. doi: 10.1371/journal.pone.0060819. Print 2013.

Abstract

Human scalp skin and hair follicles (HFs) are extra-pituitary sources of prolactin (PRL). However, the intracutaneous regulation of PRL remains poorly understood. Therefore we investigated whether well-recognized regulators of pituitary PRL expression, which also impact on human skin physiology and pathology, regulate expression of PRL and its receptor (PRLR) in situ. This was studied in serum-free organ cultures of microdissected human scalp HFs and skin, i.e. excluding pituitary, neural and vascular inputs. Prolactin expression was confirmed at the gene and protein level in human truncal skin, where its expression significantly increased (p = 0.049) during organ culture. There was, however, no evidence of PRL secretion into the culture medium as measured by ELISA. PRL immunoreactivity (IR) in female human epidermis was decreased by substance P (p = 0.009), while neither the classical pituitary PRL inhibitor, dopamine, nor corticotropin-releasing hormone significantly modulated PRL IR in HFs or skin respectively. Interferon (IFN) γ increased PRL IR in the epithelium of human HFs (p = 0.044) while tumour necrosis factor (TNF) α decreased both PRL and PRLR IR. This study identifies substance P, TNFα and IFNγ as novel modulators of PRL and PRLR expression in human skin, and suggests that intracutaneous PRL expression is not under dopaminergic control. Given the importance of PRL in human hair growth regulation and its possible role in the pathogenesis of several common skin diseases, targeting intracutaneous PRL production via these newly identified regulatory pathways may point towards novel therapeutic options for inflammatory dermatoses.

摘要

人体头皮皮肤和毛囊(HFs)是催乳素(PRL)的垂体外来源。然而,PRL 的皮内调节仍知之甚少。因此,我们研究了是否公认的调节垂体 PRL 表达的调节剂,这些调节剂也影响人类皮肤的生理学和病理学,是否调节 PRL 和其受体(PRLR)的原位表达。这是在微切割的人体头皮 HFs 和皮肤的无血清器官培养中进行的研究,即排除垂体、神经和血管输入。PRL 的表达在人体躯干皮肤的基因和蛋白质水平上得到了证实,其表达在器官培养期间显著增加(p=0.049)。然而,通过 ELISA 测量,没有证据表明 PRL 分泌到培养基中。在女性人体表皮中,P 物质(p=0.009)降低了 PRL 免疫反应性(IR),而经典的垂体 PRL 抑制剂多巴胺或促肾上腺皮质激素释放激素分别对 HFs 或皮肤中的 PRL IR 均无显著调节作用。干扰素(IFN)γ增加了人体 HFs 上皮中的 PRL IR(p=0.044),而肿瘤坏死因子(TNF)α降低了 PRL 和 PRLR IR。本研究确定 P 物质、TNFα 和 IFNγ 为人类皮肤中 PRL 和 PRLR 表达的新型调节剂,并表明皮内 PRL 表达不受多巴胺能控制。鉴于 PRL 在人类头发生长调节中的重要性及其在几种常见皮肤病发病机制中的可能作用,通过这些新发现的调节途径靶向皮内 PRL 产生可能为炎症性皮肤病提供新的治疗选择。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/afdf/3634033/2dc5af4d06df/pone.0060819.g001.jpg

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