首页> 外文期刊>Developmental biology >Dynamic regulation of retinoic acid-binding proteins in developing, adult and neoplastic skin reveals roles for beta-catenin and Notch signalling.
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Dynamic regulation of retinoic acid-binding proteins in developing, adult and neoplastic skin reveals roles for beta-catenin and Notch signalling.

机译:在发育中,成年和赘生性皮肤中视黄酸结合蛋白的动态调节揭示了β-连环蛋白和Notch信号的作用。

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摘要

Retinoic acid (RA) signalling is essential for epidermal differentiation; however, the mechanisms by which it acts are largely unexplored. Partitioning of RA between different nuclear receptors is regulated by RA-binding proteins. We show that cellular RA-binding proteins CRABP1 and CRABP2 and the fatty acid-binding protein FABP5 are dynamically expressed during skin development and in adult tissue. CRABP1 is expressed in embryonic dermis and in the stroma of skin tumours, but confined to the hair follicle dermal papilla in normal postnatal skin. CRABP2 and FABP5 are expressed in the differentiating cells of sebaceous gland, interfollicular epidermis and hair follicles, with FABP5 being a prominent marker of sebaceous glands and anagen follicle bulbs. All three proteins are upregulated in response to RA treatment or Notch activation and are negatively regulated by Wnt/beta-catenin signalling. Ectopic follicles induced by beta-catenin arise from areas of the sebaceous gland that have lost CRABP2 and FABP5; conversely, inhibition of hair follicle formation by N-terminally truncated Lef1 results in upregulation of CRABP2 and FABP5. Our findings demonstrate that there is dynamic regulation of RA signalling in different regions of the skin and provide evidence for interactions between the RA, beta-catenin and Notch pathways.
机译:维甲酸(RA)信号对于表皮分化至关重要。然而,它的作用机理在很大程度上尚未被探索。 RA结合蛋白可调节RA在不同核受体之间的分配。我们显示细胞RA结合蛋白CRABP1和CRABP2和脂肪酸结合蛋白FABP5在皮肤发育过程中和在成人组织中动态表达。 CRABP1在胚胎真皮和皮肤肿瘤基质中表达,但仅限于正常产后皮肤的毛囊真皮乳头。 CRABP2和FABP5在皮脂腺,小泡间表皮和毛囊的分化细胞中表达,FABP5是皮脂腺和生长期毛囊的突出标志。这三种蛋白质均响应RA治疗或Notch激活而上调,并受Wnt /β-catenin信号负调控。 β-catenin诱导的异位卵泡来自皮脂腺中丢失CRABP2和FABP5的区域。相反,N末端截短的Lef1抑制毛囊形成会导致CRABP2和FABP5上调。我们的发现表明,皮肤不同区域内RA信号的动态调节,为RA,β-catenin和Notch途径之间的相互作用提供了证据。

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