Literature DB >> 32579402

Vascular permeability disruption explored in the proteomes of mouse lungs and human microvascular cells following acute bromine exposure.

Dylan R Addis1,2,3, Saurabh Aggarwal1,2, Stephen F Doran1,2, Ming-Yuan Jian1,2, Israr Ahmad1,2, Kyoko Kojima4, David A Ford5, Sadis Matalon1,2, James A Mobley1,2,4.   

Abstract

Bromine (Br2) is an organohalide found in nature and is integral to many manufacturing processes. Br2 is toxic to living organisms, and high concentrations can prove fatal. To meet industrial demand, large amounts of purified Br2 are produced, transported, and stored worldwide, providing a multitude of interfaces for potential human exposure through either accidents or terrorism. To identify the key mechanisms associated with acute Br2 exposure, we have surveyed the lung proteomes of C57BL/6 male mice and human lung-derived microvascular endothelial cells (HMECs) at 24 h following exposure to Br2 in concentrations likely to be encountered in the vicinity of industrial accidents. Global discovery proteomics applications combined with systems biology analysis identified robust and highly significant changes in proteins associated with three biological processes: 1) exosome secretion, 2) inflammation, and 3) vascular permeability. We focused on the latter, conducting physiological studies on isolated perfused lungs harvested from mice 24 h after Br2 exposure. These experiments revealed significant increases in the filtration coefficient (Kf) indicating increased permeability of the pulmonary vasculature. Similarly, confluent monolayers of Br2 and Br-lipid-treated HMECs exhibited differential levels of zona occludens-1 that were found to be dissociated from cell wall localization, an increase in phosphorylation and internalization of E-cadherin, as well as increased actin stress fiber formation, all of which are consistent with increased permeability. Taken as a whole, our discovery proteomics and systems analysis workflow, combined with physiological measurements of permeability, revealed both profound and novel biological changes that contribute to our current understanding of Br2 toxicity.

Entities:  

Keywords:  ESI-MS2; actin; bromine; discovery; halogen; proteomics; systems biology; vascular permeability

Mesh:

Substances:

Year:  2020        PMID: 32579402      PMCID: PMC7473936          DOI: 10.1152/ajplung.00196.2020

Source DB:  PubMed          Journal:  Am J Physiol Lung Cell Mol Physiol        ISSN: 1040-0605            Impact factor:   5.464


  53 in total

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Journal:  Anal Chem       Date:  2009-12-01       Impact factor: 6.986

6.  Formation of chlorinated lipids post-chlorine gas exposure.

Authors:  David A Ford; Jaideep Honavar; Carolyn J Albert; Mark A Duerr; Joo Yeun Oh; Stephen Doran; Sadis Matalon; Rakesh P Patel
Journal:  J Lipid Res       Date:  2016-06-20       Impact factor: 5.922

7.  Regulation of alveolar epithelial Na+ channels by ERK1/2 in chlorine-breathing mice.

Authors:  Ahmed Lazrak; Lan Chen; Asta Jurkuvenaite; Stephen F Doran; Gang Liu; Qian Li; Jack R Lancaster; Sadis Matalon
Journal:  Am J Respir Cell Mol Biol       Date:  2011-10-13       Impact factor: 6.914

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Journal:  J Biol Chem       Date:  1995-02-17       Impact factor: 5.157

Review 9.  The paraoxonases: role in human diseases and methodological difficulties in measurement.

Authors:  Jordi Camps; Judit Marsillach; Jorge Joven
Journal:  Crit Rev Clin Lab Sci       Date:  2009       Impact factor: 6.250

10.  Halogen gas exposure: toxic effects on the parturient.

Authors:  Dylan R Addis; James A Lambert; David A Ford; Tamas Jilling; Sadis Matalon
Journal:  Toxicol Mech Methods       Date:  2020-03-30       Impact factor: 4.019

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  1 in total

Review 1.  Halogen-Induced Chemical Injury to the Mammalian Cardiopulmonary Systems.

Authors:  Dylan R Addis; Saurabh Aggarwal; Ahmed Lazrak; Tamas Jilling; Sadis Matalon
Journal:  Physiology (Bethesda)       Date:  2021-09-01
  1 in total

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