JM25-1, a Lidocaine Analog Combining Airway Relaxant and Antiinflammatory Properties: Implications for New Bronchospasm Therapy

BACKGROUND:Inhaled lidocaine antagonized bronchospasm in animal models and patients, but adverse effects limited its efficacy. This study evaluated the antibronchospasm potential of the analog JM25-1, exploring in vitro mechanisms and translation to an animal model. METHODS:The effectiveness of JM25...

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Published in:Anesthesiology (Philadelphia) 2016-01, Vol.124 (1), p.109-120
Main Authors: Serra, Magda F, Neves, Josiane S, Couto, Gina C, Cotias, Amanda C, Pão, Camila R, Olsen, Priscilla C, de Carvalho, Katharinne I Moraes, Anjos-Valotta, Edna A, Faria, Robson X, Costa, Jorge C S, Cordeiro, Renato S B, Silva, Patricia M R, Martins, Marco A
Format: Article
Language:English
Subjects:
Anesthetics, Local - pharmacology
Animals
Anti-Inflammatory Agents - pharmacology
Bronchial Spasm
Disease Models, Animal
Inflammation - drug therapy
Inflammation - physiopathology
Lidocaine - analogs & derivatives
Lidocaine - pharmacology
Mice
Rats
Rats, Wistar
Trachea - drug effects
Trachea - physiopathology
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Summary:BACKGROUND:Inhaled lidocaine antagonized bronchospasm in animal models and patients, but adverse effects limited its efficacy. This study evaluated the antibronchospasm potential of the analog JM25-1, exploring in vitro mechanisms and translation to an animal model. METHODS:The effectiveness of JM25-1 was assessed in GH3 cells, rat tracheal rings, mouse lymphocytes, and human eosinophil systems in vitro, assessing changes in Na current, contraction, proliferation, and survival, respectively. Lung function and inflammatory changes were studied in ovalbumin-sensitized mice. RESULTS:The efficacy of JM25-1 was higher than lidocaine in inhibiting carbachol-induced and calcium-induced tracheal contractions (maximum effect inhibition at 1 mM [%]67 ± 10 [JM25-1] vs. 41 ± 11 [lidocaine] [P < 0.001] for carbachol; 100 ± 3 [JM25-1] vs. 36 ± 26 [lidocaine] [P < 0.001] for Ca; mean ± SD; n = 9 each) but lower in Na current (50% inhibitory concentration = 151.5, n = 8 vs. 0.2 mM; n = 5; P < 0.001). JM25-1 also inhibited eosinophil survival (dead cells [%]65 ± 6; n = 4; P < 0.001 at 1 mM) and lymphocyte proliferation (cells in phase S + G2 [%]94 ± 10; n = 6; P < 0.001) at 0.6 mM. Aerosolized JM25-1 (1%) decreased lung eosinophil numbers from 13.2 ± 2.4 to 1.7 ± 0.7 × 10/μm (n = 6; P < 0.001) and neutrophils from 1.9 ± 0.4 to 0.2 ± 0.1 × 10/μm (n = 7; P < 0.001). Other parameters, including airway hyperreactivity, cytokines, mucus, and extracellular matrix deposition, were also sensitive to aerosolized JM25-1. CONCLUSION:These findings highlight the potential of JM25-1, emphasizing its putative value in drug development for clinical conditions where there is bronchospasm.
ISSN:0003-3022
1528-1175
DOI:10.1097/ALN.0000000000000919