Contribution of Connexin Hemichannels to the Pathogenesis of Acute Lung Injury

Connexin (Cx) family members form hemichannels (HCs) and gap junctions (GJs). Biological functions of Cx HCs have not been adequately characterized due to the inability to selectively target HCs or GJs. Recently, we developed a 6-mer peptide mimetic (P5) of the first extracellular loop of Cx43 and s...

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Published inMediators of inflammation Vol. 2020; no. 2020; pp. 1 - 10
Main Authors Li, Wei, Miller, Edmund J., Chen, Na, Zhou, Nannan, Bai, Yu, Sun, Yafang, Wang, Shuaiwei, Zhang, Yijie
Format Journal Article
LanguageEnglish
Published Cairo, Egypt Hindawi Publishing Corporation 2020
Hindawi
Hindawi Limited
Wiley
Subjects
Acute respiratory distress syndrome
Alveoli
Amino acids
Astrocytes
Bronchus
Chromosomal proteins
Connexin 43
Endothelial cells
Ethylenediaminetetraacetic acid
Fibroblasts
Gap junctions
High mobility group proteins
HMGB1 protein
Inflammation
Leukocytes (neutrophilic)
Lungs
Medical prognosis
Microvasculature
Monocytes
Mortality
Pathogenesis
Penicillin
Peptides
Permeability
Sepsis
Somatotropin
Trachea
China
United States > US
Germany
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Summary:Connexin (Cx) family members form hemichannels (HCs) and gap junctions (GJs). Biological functions of Cx HCs have not been adequately characterized due to the inability to selectively target HCs or GJs. Recently, we developed a 6-mer peptide mimetic (P5) of the first extracellular loop of Cx43 and showed that it can block the permeability of HCs but not GJs formed by Cx43. In this study, we further characterized the HC blocking property of P5 and investigated the role of Cx HCs in acute lung injury (ALI). We found that P5 administration decreased HC permeability, in pulmonary microvascular endothelial cells, HepG2 cells, and even Cx43-deficient astrocytes, which express different sets of Cxs, suggesting that P5 is a broad spectrum Cx HC blocker. In addition, P5 reduced HC permeability of alveolar cells in vivo. Moreover, P5 decreased endotoxin-induced release, by vascular endothelial cells in vitro, of high mobility group box protein 1 (HMGB1), a critical mediator of acute lung injury (ALI), and reduced HMGB1 accumulation in bronchoalveolar lavage fluid (BALF) of mice subjected to intratracheal endotoxin instillation. Furthermore, P5 administration resulted in a significant decrease in the concentrations of ALT, AST, and LDH in the BALF, the accumulation of leukocytes in alveoli, and the mortality rate of mice subjected to ALI. Wright-Giemsa staining showed that P5 caused similar reductions of both neutrophils and monocytes in BALF of ALI mice. Together, these results suggest that Cx HCs mediate HMGB1 release, augment leukocyte recruitment, and contribute to ALI pathology.
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Academic Editor: Ronald Gladue
ISSN:0962-9351
1466-1861
DOI:10.1155/2020/8094347