Literature DB >> 30484371

Proteomic Analysis and Biochemical Correlates of Mitochondrial Dysfunction after Low-Intensity Primary Blast Exposure.

Hailong Song1, Mei Chen2, Chen Chen3, Jiankun Cui1,4, Catherine E Johnson5, Jianlin Cheng3, Xiaowan Wang6, Russell H Swerdlow6, Ralph G DePalma7,8, Weiming Xia2, Zezong Gu1,4.   

Abstract

Service members during military actions or combat training are frequently exposed to primary blasts by weaponry. Most studies have investigated moderate or severe brain injuries from blasts generating overpressures >100 kPa, whereas understanding the pathophysiology of low-intensity blast (LIB)-induced mild traumatic brain injury (mTBI) leading to neurological deficits remains elusive. Our recent studies, using an open-field LIB-induced mTBI mouse model with a peak overpressure at 46.6 kPa, demonstrated behavioral impairments and brain nanoscale damages, notably mitochondrial and axonal ultrastructural changes. In this study, we used tandem mass tagged (TMT) quantitative proteomics and bioinformatics analysis to seek insights into the molecular mechanisms underlying ultrastructural pathology. Changes in global- and phospho-proteomes were determined at 3 and 24 h and at 7 and 30 days post injury (DPI), in order to investigate the biochemical and molecular correlates of mitochondrial dysfunction. Results showed striking dynamic changes in a total of 2216 proteins and 459 phosphorylated proteins at vary time points after blast. Disruption of key canonical pathways included evidence of mitochondrial dysfunction, oxidative stress, axonal/cytoskeletal/synaptic dysregulation, and neurodegeneration. Bioinformatic analysis identified blast-induced trends in networks related to cellular growth/development/movement/assembly and cell-to-cell signaling interactions. With observations of proteomic changes, we found LIB-induced oxidative stress associated with mitochondrial dysfunction mainly at 7 and 30 DPI. These dysfunctions included impaired fission-fusion dynamics, diminished mitophagy, decreased oxidative phosphorylation, and compensated respiration-relevant enzyme activities. Insights on the early pathogenesis of primary LIB-induced brain damage provide a template for further characterization of its chronic effects, identification of potential biomarkers, and targets for intervention.

Entities:  

Keywords:  mitochondrial dysfunction; open-field LIB; oxidative stress; quantitative proteomics

Year:  2019        PMID: 30484371      PMCID: PMC6909772          DOI: 10.1089/neu.2018.6114

Source DB:  PubMed          Journal:  J Neurotrauma        ISSN: 0897-7151            Impact factor:   5.269


  57 in total

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5.  Blast exposure induces post-traumatic stress disorder-related traits in a rat model of mild traumatic brain injury.

Authors:  Gregory A Elder; Nathan P Dorr; Rita De Gasperi; Miguel A Gama Sosa; Michael C Shaughness; Eric Maudlin-Jeronimo; Aaron A Hall; Richard M McCarron; Stephen T Ahlers
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7.  PINK1 stabilized by mitochondrial depolarization recruits Parkin to damaged mitochondria and activates latent Parkin for mitophagy.

Authors:  Noriyuki Matsuda; Shigeto Sato; Kahori Shiba; Kei Okatsu; Keiko Saisho; Clement A Gautier; Yu-Shin Sou; Shinji Saiki; Sumihiro Kawajiri; Fumiaki Sato; Mayumi Kimura; Masaaki Komatsu; Nobutaka Hattori; Keiji Tanaka
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8.  Proteomic quantification and site-mapping of S-nitrosylated proteins using isobaric iodoTMT reagents.

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Journal:  J Proteome Res       Date:  2014-06-13       Impact factor: 4.466

9.  Gangliosides and ceramides change in a mouse model of blast induced traumatic brain injury.

Authors:  Amina S Woods; Benoit Colsch; Shelley N Jackson; Jeremy Post; Kathrine Baldwin; Aurelie Roux; Barry Hoffer; Brian M Cox; Michael Hoffer; Vardit Rubovitch; Chaim G Pick; J Albert Schultz; Carey Balaban
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1.  Traumatic brain injury recapitulates developmental changes of axons.

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2.  Tandem Mass Tag-based proteomics analysis reveals the vital role of inflammation in traumatic brain injury in a mouse model.

Authors:  Jin-Qian Dong; Qian-Qian Ge; Sheng-Hua Lu; Meng-Shi Yang; Yuan Zhuang; Bin Zhang; Fei Niu; Xiao-Jian Xu; Bai-Yun Liu
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3.  Brain-related proteins as serum biomarkers of acute, subconcussive blast overpressure exposure: A cohort study of military personnel.

Authors:  Angela M Boutté; Bharani Thangavelu; Christina R LaValle; Jeffrey Nemes; Janice Gilsdorf; Deborah A Shear; Gary H Kamimori
Journal:  PLoS One       Date:  2019-08-13       Impact factor: 3.240

4.  Proteomic Analysis Revealed the Characteristics of Key Proteins Involved in the Regulation of Inflammatory Response, Leukocyte Transendothelial Migration, Phagocytosis, and Immune Process during Early Lung Blast Injury.

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Review 5.  Getting on the Same Page: Consolidating Terminology to Facilitate Cross-Disciplinary Health-Related Blast Research.

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7.  Long-Term Effects of Low-Intensity Blast Non-Inertial Brain Injury on Anxiety-Like Behaviors in Mice: Home-Cage Monitoring Assessments.

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Review 8.  Roadmap for Advancing Pre-Clinical Science in Traumatic Brain Injury.

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