Margarita Schratter, David Holubek, Lukas Koeffler, Thomas Züllig, Thomas O Eichmann, Heimo Wolinski, Monika Oberer, Achim Lass, Franz P W Radner
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We analyzed seven disease-associated ABHD5 missense mutations and found that they disrupt PNPLA1 localization and function by distinct mechanisms: (i) mutations affecting the PNPLA1 binding region of ABHD5 impair PNPLA1 recruitment to intracellular lipid droplets (LDs), thus reducing acylCer synthesis; (ii) mutations in potential perilipin-binding domains of ABHD5 prevent ABHD5 association with LDs, thereby disrupting PNPLA1-LD localization. Despite these defects, restoring co-localization of ABHD5 mutants with PNPLA1 in proteoliposomes rescued full PNPLA1 enzyme activity, indicating that spatial proximity rather than direct protein binding is sufficient to facilitate acylCer formation. In summary, our findings establish a co-localization-driven model of PNPLA1 regulation, in which ABHD5 ensures proper PNPLA1 targeting to LDs and simultaneously enables its enzymatic activation. This model suggests that pharmacological strategies aimed at restoring PNPLA1 localization to LDs may represent a potential therapeutic approach for ichthyosis in ABHD5-sEDD. By elucidating the molecular mechanisms underlying disease pathogenesis, our study provides important new insights into epidermal lipid metabolism and therapeutic targeting.</p>","PeriodicalId":16209,"journal":{"name":"Journal of Lipid Research","volume":" ","pages":"100875"},"PeriodicalIF":4.1000,"publicationDate":"2025-09-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC12465037/pdf/","citationCount":"0","resultStr":"{\"title\":\"Defective targeting of PNPLA1 to lipid droplets causes ichthyosis in ABHD5-syndromic epidermal differentiation disorder.\",\"authors\":\"Margarita Schratter, David Holubek, Lukas Koeffler, Thomas Züllig, Thomas O Eichmann, Heimo Wolinski, Monika Oberer, Achim Lass, Franz P W Radner\",\"doi\":\"10.1016/j.jlr.2025.100875\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><p>ABHD5-syndromic epidermal differentiation disorder (ABHD5-sEDD; also known as Chanarin-Dorfman syndrome) is a rare autosomal recessive disorder caused by mutations in the α/β-hydrolase domain-containing 5 (ABHD5) gene, leading to systemic accumulation of neutral lipids and ichthyosis due to impaired activation of patatin-like phospholipase domain-containing (PNPLAs) proteins. 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引用次数: 0
摘要
abhd5综合征表皮分化障碍(ABHD5-sEDD;也称为Chanarin-Dorfman综合征)是一种罕见的常染色体隐性遗传病,由α/β-水解酶结构域5 (ABHD5)基因突变引起,由于patatin样磷脂酶结构域(PNPLAs)蛋白的激活受损,导致中性脂的系统性积累和鱼鳞病。虽然ABHD5是一种众所周知的脂肪甘油三酯脂肪酶(ATGL,也称为PNPLA2)的共激活剂,但其在表皮脂质代谢中的作用尚不完全清楚。在这里,我们发现ABHD5是PNPLA1的关键调节因子,PNPLA1是ω- o -酰基神经酰胺(acylCer)合成和皮肤屏障形成所必需的酶。我们分析了7种与疾病相关的错义突变,发现它们通过不同的机制破坏了PNPLA1的定位和功能:(i)影响ABHD5的PNPLA1结合区域的突变损害了PNPLA1向细胞内脂滴(ld)的募集,从而减少了酰基胞苷的合成;(ii) ABHD5潜在的perilipin结合域的突变阻止了ABHD5与ld的结合,从而破坏了PNPLA1-LD的定位。尽管存在这些缺陷,在蛋白脂质体中恢复与PNPLA1共定位的ABHD5突变体恢复了完全的PNPLA1酶活性,这表明空间接近而不是直接的蛋白质结合足以促进酰基cer的形成。总之,我们的研究结果建立了PNPLA1调控的共定位驱动模型,其中ABHD5确保PNPLA1适当靶向lld,同时使其酶促激活。该模型表明,旨在恢复PNPLA1定位到ld的药理学策略可能是ABHD5-sEDD鱼鳞病的潜在治疗方法。通过阐明疾病发病机制的分子机制,我们的研究为表皮脂质代谢和治疗靶向提供了重要的新见解。
Defective targeting of PNPLA1 to lipid droplets causes ichthyosis in ABHD5-syndromic epidermal differentiation disorder.
ABHD5-syndromic epidermal differentiation disorder (ABHD5-sEDD; also known as Chanarin-Dorfman syndrome) is a rare autosomal recessive disorder caused by mutations in the α/β-hydrolase domain-containing 5 (ABHD5) gene, leading to systemic accumulation of neutral lipids and ichthyosis due to impaired activation of patatin-like phospholipase domain-containing (PNPLAs) proteins. While ABHD5 is a well-known co-activator of adipose triglyceride lipase (ATGL, also referred to as PNPLA2), its role in epidermal lipid metabolism is incompletely understood. Here, we identify ABHD5 as a key regulator of PNPLA1, an enzyme essential for ω-O-acylceramide (acylCer) synthesis and skin barrier formation. We analyzed seven disease-associated ABHD5 missense mutations and found that they disrupt PNPLA1 localization and function by distinct mechanisms: (i) mutations affecting the PNPLA1 binding region of ABHD5 impair PNPLA1 recruitment to intracellular lipid droplets (LDs), thus reducing acylCer synthesis; (ii) mutations in potential perilipin-binding domains of ABHD5 prevent ABHD5 association with LDs, thereby disrupting PNPLA1-LD localization. Despite these defects, restoring co-localization of ABHD5 mutants with PNPLA1 in proteoliposomes rescued full PNPLA1 enzyme activity, indicating that spatial proximity rather than direct protein binding is sufficient to facilitate acylCer formation. In summary, our findings establish a co-localization-driven model of PNPLA1 regulation, in which ABHD5 ensures proper PNPLA1 targeting to LDs and simultaneously enables its enzymatic activation. This model suggests that pharmacological strategies aimed at restoring PNPLA1 localization to LDs may represent a potential therapeutic approach for ichthyosis in ABHD5-sEDD. By elucidating the molecular mechanisms underlying disease pathogenesis, our study provides important new insights into epidermal lipid metabolism and therapeutic targeting.
期刊介绍:
The Journal of Lipid Research (JLR) publishes original articles and reviews in the broadly defined area of biological lipids. We encourage the submission of manuscripts relating to lipids, including those addressing problems in biochemistry, molecular biology, structural biology, cell biology, genetics, molecular medicine, clinical medicine and metabolism. Major criteria for acceptance of articles are new insights into mechanisms of lipid function and metabolism and/or genes regulating lipid metabolism along with sound primary experimental data. Interpretation of the data is the authors’ responsibility, and speculation should be labeled as such. Manuscripts that provide new ways of purifying, identifying and quantifying lipids are invited for the Methods section of the Journal. JLR encourages contributions from investigators in all countries, but articles must be submitted in clear and concise English.
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