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Merck

Effects of salbutamol and phlorizin on acute pulmonary inflammation and disease severity in experimental sepsis.

PloS one (2019-09-20)
Léia Cardoso-Sousa, Emilia Maria Gomes Aguiar, Douglas Carvalho Caixeta, Danielle Diniz Vilela, Danilo Pereira da Costa, Tamires Lopes Silva, Thúlio Marquez Cunha, Paulo Rogério Faria, Foued Salmen Espindola, Ana Carolina Jardim, Alexandre Antônio Vieira, Tales Lyra Oliveira, Luiz Ricardo Goulart, Robinson Sabino-Silva
ABSTRAKT

Respiratory infection can be exacerbated by the high glucose concentration in the airway surface liquid (ASL). We investigated the effects of salbutamol and phlorizin on the pulmonary function, oxidative stress levels and SGLT1 activity in lung, pulmonary histopathological damages and survival rates of rats with sepsis. Sepsis was induced by cecal ligation and puncture surgery (CLP). Twenty-four hours after surgery, CLP rats were intranasally treated with saline, salbutamol or phlorizin. After 2 hours, animals were anesthetized and sacrificed. Sepsis promoted atelectasis and bronchial inflammation, and led to increased expression of SGLT1 on cytoplasm of pneumocytes. Salbutamol treatment reduced bronchial inflammation and promoted hyperinsuflation in CLP rats. The interferon-ɤ and Interleucin-1β concentrations in bronchoalveolar lavage (BAL) were closely related to the bronchial inflammation regulation. Salbutamol stimulated SGLT1 in plasma membrane; whereas, phlorizin promoted the increase of SGLT1 in cytoplasm. Phlorizin reduced catalase activity and induced a significant decrease in the survival rate of CLP rats. Taken together, sepsis promoted atelectasis and lung inflammation, which can be associated with SGLT1 inhibition. The loss of function of SGLT1 by phlorizin are related to the augmented disease severity, increased atelectasis, bronchial inflammation and a significant reduction of survival rate of CLP rats. Alternatively salbutamol reduced BAL inflammatory cytokines, bronchial inflammation, atelectasis, and airway damage in sepsis. These data suggest that this selective β2-adrenergic agonist may protect lung of septic acute effects.

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Sigma-Aldrich
Anti-SGLT-1 (Sodium Glucose Co-transporter-1) Antibody, serum, from rabbit