| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5558310 | Toxicology and Applied Pharmacology | 2017 | 12 Pages |
â¢TRPA1 protects mice against toxicity and mortality of inhaled high-level acrolein.â¢TRPA1 protection against inhaled high-level acrolein is sex-dependent in mice.â¢Age (5-52 weeks old) was not a determinant of acrolein-induced mortality in mice.â¢TRPA1 antagonist is protective after inhaled high-level acrolein in male mice.
Acrolein is a highly toxic, volatile, unsaturated aldehyde generated during incomplete combustion as in tobacco smoke and indoor fires. Because the transient receptor potential ankyrin 1 (TRPA1) channel mediates tobacco smoke-induced lung injury, we assessed its role in high-level acrolein-induced toxicity in mice. Acrolein (100-275Â ppm, 10-30Â min) caused upper airway epithelial sloughing, bradypnea and oral gasping, hypothermia, cardiac depression and mortality. Male wild-type mice (WT, C57BL/6; 5-52Â weeks) were significantly more sensitive to high-level acrolein than age-matched, female WT mice. Both male and female TRPA1-null mice were more sensitive to acrolein-induced mortality than age- and sex-matched WT mice. Acrolein exposure increased lung weight:body weight ratios and lung albumin and decreased plasma albumin to a greater extent in TRPA1-null than in WT mice. Lung and plasma protein-acrolein adducts were not increased in acrolein-exposed TRPA1-null mice compared with WT mice. To assess TRPA1-dependent protective mechanisms, respiratory parameters were monitored by telemetry. TRPA1-null mice had a slower onset of breathing rate suppression ('respiratory braking') than WT mice suggesting TRPA1 mediates this protective response. Surprisingly, WT male mice treated either with a TRPA1 antagonist (HC030031; 200Â mg/kg) alone or with combined TRPA1 (100Â mg/kg) and TRPV1 (capsazepine, 10Â mg/kg) antagonists at 30Â min post-acrolein exposure (i.e., “real world” delay in treatment) were significantly protected from acrolein-induced mortality. These data show TRPA1 protects against high-level acrolein-induced toxicity in a sex-dependent manner. Post-exposure TRPA1 antagonism also protected against acrolein-induced mortality attesting to a complex role of TRPA1 in cardiopulmonary injury.
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