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基于液相色谱-质谱联用的血浆分析表明,轻度爆炸暴露会使代谢途径和关联网络失调。

Mild Blast Exposure Dysregulates Metabolic Pathways and Correlation Networking as Evident from LC-MS-Based Plasma Profiling.

作者信息

Baghel Ruchi, Maan Kiran, Dhariwal Seema, Kumari Megha, Sharma Apoorva, Manda Kailash, Trivedi Richa, Rana Poonam

机构信息

Radiological, Nuclear and Imaging Sciences (RNAIS), Institute of Nuclear Medicine and Allied Science (INMAS), DRDO, New Delhi, 110054, India.

Department of Health Research (DHR), IRCS Building, 2 FloorRed Cross Road, New Delhi, 110001, India.

出版信息

Mol Neurobiol. 2025 Mar;62(3):3143-3166. doi: 10.1007/s12035-024-04429-5. Epub 2024 Sep 5.

Abstract

Blast-induced trauma is emerging as a serious threat due to its wide pathophysiology where not only the brain but also a spectrum of organs is being affected. In the present study, we aim to identify the plasma-based metabolic dysregulations along with the associated temporal changes at 5-6 h, day 1 and day 7 post-injury in a preclinical animal model for blast exposure, through liquid chromatography-mass spectrometry (LC-MS). Using significantly advanced metabolomic and statistical bioinformatic platforms, we were able to elucidate better and unravel the complex networks of blast-induced neurotrauma (BINT) and its interlinked systemic effects. Significant changes were evident at 5-6 h with maximal changes at day 1. Temporal analysis also depicted progressive changes which continued till day 7. Significant associations of metabolic markers belonging to the class of amino acids, energy-related molecules, lipids, vitamin, hormone, phenolic acid, keto and histidine derivatives, nucleic acid molecules, uremic toxins, and uronic acids were observed. Also, the present study is the first of its kind where comprehensive, detailed pathway dysregulations of amino acid metabolism and biosynthesis, perturbed nucleotides, lipid peroxidation, and nucleic acid damage followed by correlation networking and multiomics networking were explored on preclinical animal models exposed to mild blast trauma. In addition, markers for systemic changes (renal dysfunction) were also observed. Global pathway predictions of unannotated peaks also presented important insights into BINT pathophysiology. Conclusively, the present study depicts important findings that might help underpin the biological mechanisms of blast-induced brain or systemic trauma.

摘要

由于其广泛的病理生理学,爆炸引起的创伤正成为一种严重威胁,不仅大脑,而且一系列器官都受到影响。在本研究中,我们旨在通过液相色谱 - 质谱联用(LC-MS),在爆炸暴露的临床前动物模型中,确定伤后5 - 6小时、第1天和第7天基于血浆的代谢失调以及相关的时间变化。使用显著先进的代谢组学和统计生物信息学平台,我们能够更好地阐明并揭示爆炸诱导的神经创伤(BINT)及其相互关联的全身效应的复杂网络。在5 - 6小时时明显出现显著变化,第1天变化最大。时间分析还描绘了持续到第7天的渐进变化。观察到属于氨基酸、能量相关分子、脂质、维生素、激素、酚酸、酮和组氨酸衍生物、核酸分子、尿毒症毒素和糖醛酸类别的代谢标志物之间存在显著关联。此外,本研究是同类研究中的首例,在暴露于轻度爆炸创伤的临床前动物模型上,探索了氨基酸代谢和生物合成、核苷酸紊乱、脂质过氧化和核酸损伤的全面、详细的途径失调,随后进行了相关网络分析和多组学网络分析。此外,还观察到了全身变化(肾功能障碍)的标志物。未注释峰的全局途径预测也为BINT病理生理学提供了重要见解。总之,本研究描述了可能有助于支撑爆炸诱导的脑或全身创伤生物学机制的重要发现。

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