| Literature DB >> 29437149 |
Lei-Miao Yin1, Yu-Dong Xu1, Ling-Ling Peng1, Ting-Ting Duan1, Jia-Yuan Liu1, Zhijian Xu2, Wen-Qian Wang1, Nan Guan1, Xiao-Jie Han1, Hai-Yan Li1, Yu Pang1, Yu Wang1, Zhaoqiang Chen2, Weiliang Zhu2, Linhong Deng3, Ying-Li Wu4, Guang-Bo Ge5, Shuang Huang1,6, Luis Ulloa7,8, Yong-Qing Yang9.
Abstract
There is a clinical need for new bronchodilator drugs in asthma, because more than half of asthmatic patients do not receive adequate control with current available treatments. We report that inhibition of metallothionein-2 protein expression in lung tissues causes the increase of pulmonary resistance. Conversely, metallothionein-2 protein is more effective than β2-agonists in reducing pulmonary resistance in rodent asthma models, alleviating tension in tracheal spirals, and relaxing airway smooth muscle cells (ASMCs). Metallothionein-2 relaxes ASMCs via transgelin-2 (TG2) and induces dephosphorylation of myosin phosphatase target subunit 1 (MYPT1). We identify TSG12 as a nontoxic, specific TG2-agonist that relaxes ASMCs and reduces asthmatic pulmonary resistance. In vivo, TSG12 reduces pulmonary resistance in both ovalbumin- and house dust mite-induced asthma in mice. TSG12 induces RhoA phosphorylation, thereby inactivating the RhoA-ROCK-MYPT1-MLC pathway and causing ASMCs relaxation. TSG12 is more effective than β2-agonists in relaxing human ASMCs and pulmonary resistance with potential clinical advantages. These results suggest that TSG12 could be a promising therapeutic approach for treating asthma.Entities:
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Year: 2018 PMID: 29437149 PMCID: PMC6310021 DOI: 10.1126/scitranslmed.aam8604
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956