Pulmonary implications of acetaminophen exposures independent of hepatic toxicity.
Evgenia DobrinskikhSaif I Al-JubooriMiguel A ZarateLijun ZhengRobyn De DiosDurga BalasubramaniyanLaura G SherlockDavid J OrlickyClyde J WrightPublished in: American journal of physiology. Lung cellular and molecular physiology (2021)
Both preclinical and clinical studies have demonstrated that exposures to acetaminophen (APAP) at levels that cause hepatic injury cause pulmonary injury as well. However, whether exposures that do not result in hepatic injury have acute pulmonary implications is unknown. Thus, we sought to determine how APAP exposures at levels that do not result in significant hepatic injury impact the mature lung. Adult male ICR mice (8-12 wk) were exposed to a dose of APAP known to cause hepatotoxicity in adult mice [280 mg/kg, intraperitoneal (ip)], as well as a lower dose previously reported to not cause hepatic injury (140 mg/kg, ip). We confirm that the lower dose exposures did not result in significant hepatic injury. However, like high dose, lower exposure resulted in increased cellular content of the bronchoalveolar lavage fluid and induced a proinflammatory pulmonary transcriptome. Both the lower and higher dose exposures resulted in measurable changes in lung morphometrics, with the lower dose exposure causing alveolar wall thinning. Using RNAScope, we were able to detect dose-dependent, APAP-induced pulmonary Cyp2e1 expression. Finally, using FLIM we determined that both APAP exposures resulted in acute pulmonary metabolic changes consistent with mitochondrial overload in lower doses and a shift to glycolysis at a high dose. Our findings demonstrate that APAP exposures that do not cause significant hepatic injury result in acute inflammatory, morphometric, and metabolic changes in the mature lung. These previously unreported findings may help explain the potential relationship between APAP exposures and pulmonary-related morbidity.
Keyphrases
- air pollution
- pulmonary hypertension
- drug induced
- high dose
- liver injury
- liver failure
- oxidative stress
- low dose
- metabolic syndrome
- type diabetes
- stem cell transplantation
- mesenchymal stem cells
- adipose tissue
- long non coding rna
- diabetic rats
- young adults
- hepatitis b virus
- childhood cancer
- cell therapy
- mechanical ventilation