Montelukast, Leukotriene Inhibitor, Reduces LPS-Induced Acute Lung Inflammation and Human Neutrophil Activation

Davino-Chiovatto, Jaime Eduardo; Carneiro Oliveira-Junior, Manoel; MacKenzie, BreAnne; Santos-Dias, Alana; Almeida-Oliveira, Ana Roberta; Comin Jonco Aquino-Junior, Jefferson; Brito, Auriléia Aparecida; Rigonato-Oliveira, Nicole Cristine; Damaceno-Rodrigues, Nilsa Regina; Ligeiro Oliveira, Ana Paula; Pereira Silva, Alessandro; Consolim-Colombo, Fernanda Marciano; Aimbire, Flavio; Caire Castro-Faria-Neto, Hugo; Paula Vieira, Rodolfo

Montelukast, Leukotriene Inhibitor, Reduces LPS-Induced Acute Lung Inflammation and Human Neutrophil Activation / El montelukast, un inhibidor de leucotrienos, reduce la inflamación pulmonar aguda inducida por LPS y la activación de neutrófilos humanos

Davino-Chiovatto, Jaime Eduardo; Carneiro Oliveira-Junior, Manoel; MacKenzie, BreAnne; Santos-Dias, Alana; Almeida-Oliveira, Ana Roberta; Comin Jonco Aquino-Junior, Jefferson; Brito, Auriléia Aparecida; Rigonato-Oliveira, Nicole Cristine; Damaceno-Rodrigues, Nilsa Regina; Ligeiro Oliveira, Ana Paula; Pereira Silva, Alessandro; Consolim-Colombo, Fernanda Marciano; Aimbire, Flavio; Caire Castro-Faria-Neto, Hugo; Paula Vieira, Rodolfo.

Affiliation

Davino-Chiovatto, Jaime Eduardo; Nove de Julho University (UNINOVE). São Paulo. Brazil
Carneiro Oliveira-Junior, Manoel; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
MacKenzie, BreAnne; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
Santos-Dias, Alana; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
Almeida-Oliveira, Ana Roberta; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
Comin Jonco Aquino-Junior, Jefferson; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
Brito, Auriléia Aparecida; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
Rigonato-Oliveira, Nicole Cristine; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
Damaceno-Rodrigues, Nilsa Regina; University of São Paulo. School of Medicine. Department of Pathology. São Paulo. Brazil
Ligeiro Oliveira, Ana Paula; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
Pereira Silva, Alessandro; s.af
Consolim-Colombo, Fernanda Marciano; Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE). São José dos Campos. Brazil
Aimbire, Flavio; Federal University of Sao Paulo (UNIFESP). São José dos Campos. Brazil
Caire Castro-Faria-Neto, Hugo; Osvaldo Cruz Institute (IOC). Laboratory of Immunopharmacology. Rio de Janeiro. Brazil
Paula Vieira, Rodolfo; Anhembi Morumbi University. School of Medicine. São José dos Campos. Brazil

Arch. bronconeumol. (Ed. impr.) ; 55(11): 573-580, nov. 2019. graf, ilus

Article in English | IBECS | ID: ibc-186325

Responsible library: ES1.1

Localization: BNCS

ABSTRACT
RESUMEN

ABSTRACT

Objectives:

Some pro-inflammatory lipids derived from 1 lipooxygenase enzyme are potent neutrophil chemoattractant, a cell centrally involved in acute respiratory distress syndrome (ARDS); a syndrome lacking effective treatment. Considering the beneficial effects of the leukotriene receptor inhibitor, montelukast, on other lung diseases, whether montelukast attenuates inflammation in a mouse model of ARDS, and whether it reduces LPS stimulated activation of human neutrophils was investigated.

Methods:

Thirty-five C57Bl/6 mice were distributed into control (PBS) + 24h, LPS + 24h (10 μg/mouse), control + 48 h, LPS+48 h, and LPS 48 h+Montelukast (10 mg/kg). In addition, human neutrophils were incubated with LPS ( 1μg/mL) and treated with montelukast (10 μM).

Results:

Oral-tracheal administration of montelukast significantly attenuated total cells (P < .05), macrophages (P < .05), neutrophils (P < .01), lymphocytes (P < .001) and total protein levels in BAL (P < .05), as well as IL-6 (P < .05), CXCL1/KC (P < .05), IL-17 (P < .05) and TNF-alfa (P < .05). Furthermore, montelukast reduced neutrophils (P < .001), lymphocytes (P < .01) and macrophages (P < .01) in the lung parenchyma. In addition, montelukast restored BAL VEGF levels (P < .05). LTB4 receptor expression (P < .001) as well as NF-κB (P <. 001), a downstream target of LPS, were also reduced in lung parenchymal leukocytes. Furthermore, montelukast reduced IL-8 (P < .001) production by LPS-treated human neutrophils.

Conclusion:

In conclusion, montelukast efficiently attenuated both LPS-induced lung inflammation in a mouse model of ARDS and in LPS challenged human neutrophils

RESUMEN

Objetivos:

Algunos lípidos proinflamatorios derivados de la enzima lipooxigenasa 1 son potentes quimioatrayentes de neutrófilos, un tipo celular con una implicación principal en el síndrome de distrés respiratorio agudo (SDRA), para el que no hay tratamiento efectivo. Considerando los efectos beneficiosos del inhibidor de los receptores de leucotrienos montelukast en otras enfermedades pulmonares, se investigó si este fármaco era capaz de atenuar la inflamación en un modelo de ratón de SDRA y de reducir la activación de los neutrófilos humanos inducida por LPS.

Métodos:

Se utilizaron 35 ratones C57BL/6 distribuidos en los siguientes grupos control (PBS) + 24 h, LPS+(24 h [10 μg/ratón]), control + 48 h y LPS 48 h + montelukast (10 mg/kg). Por otro lado, se incubaron neutrófilos humanos con LPS (1 μg/ml) y se trataron con montelukast (10 μM).

Resultados:

La administración orotraqueal de montelukast redujo el número total de células (p < 0,05), de macrófagos (p < 0,05), de neutrófilos (p < 0,01), de linfocitos (p < 0,001) y los niveles totales de proteína en el lavado broncoalveolar (p < 0,05), así como de IL-6 (p < 0,05), CXCL1/KC (p < 0,05), IL-17 (p < 0,05) y TNF-alfa (p < 0,05). Además, el montelukast redujo los neutrófilos (p < 0,001), los linfocitos (p < 0,01) y los macrófagos (p < 0,01) en el parénquima pulmonar. Asimismo, restauró los niveles de VEGF en el lavado broncoalveolar (p < 0,05) y disminuyó la expresión del receptor LTB4 (p < 0,001) y de NF-κB (p < 0,001), una diana downstream del LPS, en los leucocitos del parénquima pulmonar. Por último, redujo la producción de IL-8 por parte de los neutrófilos humanos tratados con LPS.

Conclusión:

En conclusión, el montelukast atenuó de manera eficaz tanto la inflamación pulmonar inducida por LPS en un modelo de ratón de SDRA como en neutrófilos humanos estimulados con LPS

Subject(s)

Animals; Mice; Leukotriene Antagonists/therapeutic use; Lipopolysaccharide Receptors/administration & dosage; Pneumonia/chemically induced; Respiratory Distress Syndrome/diagnosis; Respiratory Distress Syndrome/complications; Pneumonia/drug therapy; Pneumonia/veterinary; Cytokines/therapeutic use; Bronchoalveolar Lavage/veterinary; Anti-Asthmatic Agents/therapeutic use

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Collection: National databases / Spain Database: IBECS Main subject: Pneumonia / Respiratory Distress Syndrome / Lipopolysaccharide Receptors / Leukotriene Antagonists Limits: Animals Language: English Journal: Arch. bronconeumol. (Ed. impr.) Year: 2019 Document type: Article Institution/Affiliation country: Anhembi Morumbi University/Brazil / Brazilian Institute of Teaching and Research in Pulmonary and Exercise Immunology (IBEPIPE)/Brazil / Federal University of Sao Paulo (UNIFESP)/Brazil / Nove de Julho University (UNINOVE)/Brazil / Osvaldo Cruz Institute (IOC)/Brazil / University of São Paulo/Brazil

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