AVR Consulting, Northwich, Cheshire, UK.
Department of Pharmaceutics, UCL School of Pharmacy, London, UK.
Int J Cosmet Sci. 2024 Aug;46(4):623-642. doi: 10.1111/ics.12955.
Over the past 50 years there have been great strides made in the discovery of the composition and relevance of the total stratum corneum (SC) ceramide matrix. However, the focus of this review is on the free intercellular class of ω-linoleoyloxyacylceramides, corneocyte-bound ceramides and associated lipids known as the corneocyte lipid envelope (CLE) together with their processing enzymes involved in aiding ceramide attachment the corneocyte protein envelope (CPE). Two structural models and partially shared biosynthetic pathways have been proposed for the attachment of CPE-bound O-ceramides (ω-hydroxyceramides attached to glutamate residues of proteins in the (CPE) using the 12R-lipoxygenase (12R-LOX)/epidermal lipoxygenase-3 (eLOX3)/epoxide hydrolase-3 (EPHX3)/unknown esterase/ transglutaminase-1 (TG1) attachment pathway) and CPE-bound EO-ceramides (epoxy-enone ceramides attached to cysteine residues of proteins in the CPE using the 12R-LOX/eLOX3/short chain dehydrogenase/reductase family 9C member 7 (SDR9C7)/non-enzymatic attachment pathway), i.e. there is a bifurcation step beyond epidermal eLOX3. Their formation and structures will be discussed as well as their relevance in compromised skin barrier conditions together with our own work on SC maturation examined by proteomics, lipidomics, enzyme immunolocalization studies, mechanical fragility assays and Nile red staining of corneocyte envelopes (CE). Reduced levels of 12R-LOX, eLOX3, SDR9C7 and TG1 were observed in photodamaged skin of the cheeks that were associated with reduced SC maturation as evidenced by Nile red staining and increased CE fragility. In the severely photodamaged cheeks of Albino African SC we also observed increased levels of acylceramides. Concomitantly by reducing the activity of 12R-LOX by antibody inhibition and TG1 inhibition with a known chemical inhibitor, we demonstrated in a humidity-based ex vivo SC maturation model that these enzymes contributed to increased CE hydrophobicity and mechanical integrity. We hypothesize that at least the CPE-bound O-ceramide pathway is operational in the SC. Nevertheless, our understanding of the full complexity of ω-linoleoyloxyacylceramides and the composition of the CLE is limited particularly on cosmetically relevant body sites such as the face.
在过去的 50 年中,人们在发现总角质层(SC)神经酰胺基质的组成和相关性方面取得了巨大进展。然而,本综述的重点是细胞间游离的 ω-亚油酰基神经酰胺类、角质细胞结合神经酰胺和被称为角质细胞脂质包膜(CLE)的相关脂质,以及参与促进神经酰胺附着到角质细胞蛋白包膜(CPE)的相关加工酶。已经提出了两种结构模型和部分共享的生物合成途径,用于附着 CPE 结合的 O-神经酰胺(使用 12R-脂氧合酶(12R-LOX)/表皮脂氧合酶-3(eLOX3)/环氧化物水解酶-3(EPHX3)/未知酯酶/转谷氨酰胺酶-1(TG1)附着途径连接到 CPE 中蛋白的谷氨酸残基上的 ω-羟基神经酰胺)和 CPE 结合的 EO-神经酰胺(使用 12R-LOX/eLOX3/短链脱氢酶/还原酶家族 9C 成员 7(SDR9C7)/非酶附着途径连接到 CPE 中蛋白的半胱氨酸残基上的环氧烯酮神经酰胺),即表皮 eLOX3 之后存在一个分支步骤。将讨论它们的形成和结构,以及它们在受损皮肤屏障条件下的相关性,以及我们使用蛋白质组学、脂质组学、酶免疫定位研究、机械脆性测定和尼罗红染色角质细胞包膜(CE)检查的 SC 成熟方面的工作。在脸颊光损伤皮肤中观察到 12R-LOX、eLOX3、SDR9C7 和 TG1 的水平降低,这与尼罗红染色和增加的 CE 脆性表明 SC 成熟度降低有关。在严重光损伤的非裔美国人 SC 的脸颊中,我们还观察到酰基神经酰胺水平升高。通过用已知的化学抑制剂抑制 TG1 活性和用抗体抑制 12R-LOX 活性,我们在基于湿度的体外 SC 成熟模型中证明,这些酶有助于增加 CE 的疏水性和机械完整性。我们假设至少 CPE 结合的 O-神经酰胺途径在 SC 中起作用。然而,我们对 ω-亚油酰基神经酰胺的全部复杂性和 CLE 的组成的理解是有限的,特别是在与化妆品相关的身体部位,如面部。
