Activation of TREK-1 (K2P2.1) potassium channels protects against influenza A-induced lung injury

被引:5
作者
Zyrianova, Tatiana [1 ]
Lopez, Benjamin [1 ]
Zou, Kathlyn [1 ]
Gu, Charles [1 ]
Pham, Dayna [1 ]
Talapaneni, Sriharsha [1 ]
Waters, Christopher M. [4 ]
Olcese, Riccardo [2 ,3 ]
Schwingshackl, Andreas [1 ]
机构
[1] Univ Calif Los Angeles, Dept Pediat, Los Angeles, CA 90095 USA
[2] Univ Calif Los Angeles, Dept Anesthesiol & Perioperat Med, Los Angeles, CA USA
[3] Univ Calif Los Angeles, Dept Physiol, Los Angeles, CA USA
[4] Univ Kentucky, Dept Physiol, Lexington, KY USA
关键词
acute lung injury; cytokines; inflammation; influenza virus; TREK-1 (KCNK2) ion channels; VIRUS; IDENTIFICATION; SECRETION; HYPEROXIA; PATHOLOGY; PRESSURE;
D O I
10.1152/ajplung.00116.2022
中图分类号
Q4 [生理学];
学科分类号
071003 ;
摘要
Influenza-A virus (IAV) infects yearly an estimated one billion people worldwide, resulting in 300,000-650,000 deaths. Preventive vaccination programs and antiviral medications represent the mainstay of therapy, but with unacceptably high morbid -ity and mortality rates, new targeted therapeutic approaches are urgently needed. Since inflammatory processes are commonly associated with measurable changes in the cell membrane potential (Em), we investigated whether Em hyperpolarization via TREK-1 (K2P2.1) K thorn channel activation can protect against influenza-A virus (IAV)-induced pneumonia. We infected mice with IAV, which after 5 days caused 10-15% weight loss and a decrease in spontaneous activity, representing a clinically relevant infec-tion. We then started a 3-day intratracheal treatment course with the novel TREK-1 activating compounds BL1249 or ML335. We confirmed TREK-1 activation with both compounds in untreated and IAV-infected primary human alveolar epithelial cells (HAECs) using high-throughput fluorescent imaging plate reader (FLIPR) assays. In mice, TREK-1 activation with BL1249 and ML335 coun-teracted IAV-induced histological lung injury and decrease in lung compliance and improved BAL fluid total protein levels, cell counts, and inflammatory IL-6, IP-10/CXCL-10, MIP-1a, and TNF-a levels. To determine whether these anti-inflammatory effects were mediated by activation of alveolar epithelial TREK-1 channels, we studied the effects of BL1249 and ML335 in IAV-infected HAEC, and found that TREK-1 activation decreased IAV-induced inflammatory IL-6, IP-10/CXCL10, and CCL-2 secretion. Dissection of TREK-1 downstream signaling pathways and construction of protein-protein interaction (PPI) networks revealed NF-kappa B1 and retinoic acid-inducible gene-1 (RIG-1) cascades as the most likely targets for TREK-1 protection. Therefore, TREK-1 activa-tion may represent a novel therapeutic approach against IAV-induced lung injury.
引用
收藏
页码:L64 / L75
页数:12
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