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一种经过优化的调节缩醛磷脂的膳食补充剂,在扩张型心肌病雄性小鼠模型中比在雌性小鼠模型中能提供更强的保护作用。

An optimized plasmalogen modulating dietary supplement provides greater protection in a male than female mouse model of dilated cardiomyopathy.

作者信息

Belkin Teleah G, Masterman Emma I, Yildiz Gunes S, Kiriazis Helen, Mellett Natalie A, Cross Jonathon, Grigolon Kyah, Dogra Akshima, Donner Daniel, Chooi Roger, Liang Amy, Kompa Andrew R, Sadoshima Junichi, Edgley Amanda J, Greening David W, Meikle Peter J, Tham Yow Keat, McMullen Julie R

机构信息

Baker Heart and Diabetes Institute, Melbourne, VIC, Australia.

Department of Medicine, The University of Melbourne, VIC, Australia.

出版信息

J Mol Cell Cardiol Plus. 2024 Dec 4;11:100273. doi: 10.1016/j.jmccpl.2024.100273. eCollection 2025 Mar.

Abstract

We previously reported that plasmalogens, a class of phospholipids, were decreased in a setting of dilated cardiomyopathy (DCM). Plasmalogen levels can be modulated via a dietary supplement called alkylglycerols (AG) which has demonstrated benefits in some disease settings. However, its therapeutic potential in DCM remained unknown. To determine whether an optimized AG supplement could restore plasmalogen levels and attenuate cardiac dysfunction/pathology, we placed a cardiac-specific transgenic DCM mouse model of both sexes on chow +/-1.5 % AG supplementation at ∼10 weeks of age for 16 weeks. Cardiac function was assessed by echocardiography, tissues were collected for histological and molecular analyses including lipidomics and proteomics via liquid chromatography-mass spectrometry. AG supplementation increased total plasmalogens in DCM hearts and attenuated lung congestion of both sexes, but only prevented cardiac dysfunction in males. This was associated with attenuated cardiac and renal enlargement, a more favorable pro-cardiac gene expression profile, and a trend for lower cardiac fibrosis. By lipidomics, specific d18:1 ceramide species associated with cardiac pathology were lower in the DCM hearts from mice on the AG diet, and tetralinoleoyl cardiolipins, a lipid crucial for mitochondrial function was restored with AG supplementation. Proteomic analysis of hearts from male DCM mice receiving AG supplementation revealed enrichment in mitochondrial protein network, as well as upregulation of extracellular matrix binding proteins including agrin, a protein associated with cardiac regeneration. In summary, AG supplementation restored plasmalogens in DCM hearts but showed greater therapeutic potential in males than females.

摘要

我们之前报道过,一类磷脂——缩醛磷脂,在扩张型心肌病(DCM)患者体内含量降低。缩醛磷脂水平可通过一种名为烷基甘油(AG)的膳食补充剂进行调节,AG已在某些疾病环境中显示出益处。然而,其在DCM中的治疗潜力仍不明确。为了确定优化后的AG补充剂是否能恢复缩醛磷脂水平并减轻心脏功能障碍/病理变化,我们在大约10周龄时,将一种心脏特异性转基因DCM雌雄小鼠模型置于含或不含1.5%AG补充剂的饲料中喂养16周。通过超声心动图评估心脏功能,收集组织进行组织学和分子分析,包括通过液相色谱 - 质谱法进行脂质组学和蛋白质组学分析。补充AG可增加DCM心脏中的总缩醛磷脂含量,并减轻雌雄小鼠的肺充血,但仅预防了雄性小鼠的心脏功能障碍。这与心脏和肾脏肿大减轻、更有利的心脏相关基因表达谱以及心脏纤维化降低的趋势有关。通过脂质组学分析,AG饮食喂养的小鼠DCM心脏中与心脏病理相关的特定d18:1神经酰胺种类较低,而四亚油酰心磷脂(一种对线粒体功能至关重要的脂质)通过补充AG得以恢复。对接受AG补充的雄性DCM小鼠心脏进行蛋白质组学分析发现,线粒体蛋白网络富集,以及细胞外基质结合蛋白上调,包括聚集蛋白(一种与心脏再生相关的蛋白质)。总之,补充AG可恢复DCM心脏中的缩醛磷脂水平,但在雄性小鼠中显示出比雌性小鼠更大的治疗潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2850/11708127/19a57ede23fb/ga1.jpg

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