| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5846858 | Toxicology and Applied Pharmacology | 2011 | 7 Pages |
The increasing use of the antimicrobial triclocarban (TCC) in personal care products (PCPs) has resulted in concern regarding environmental pollution. TCC is a potent inhibitor of soluble epoxide hydrolase (sEH). Inhibitors of sEH (sEHIs) are anti-inflammatory, anti-hypertensive and cardio-protective in multiple animal models. However, the in vivo effects anticipated from a sEHI have not been reported for TCC. Here we demonstrated the anti-inflammatory effects in vivo of TCC in a murine model. TCC was employed in a lipopolysaccharide (LPS)-challenged murine model. Systolic blood pressure, plasma levels of several inflammatory cytokines and chemokine, and metabolomic profile of plasma oxylipins were determined. TCC significantly reversed LPS-induced morbid hypotension in a time-dependent manner. TCC significantly repressed the increased release of inflammatory cytokines and chemokine caused by LPS. Furthermore, TCC significantly shifted the oxylipin profile in vivo in a time-dependent manner towards resolution of inflammation as expected from a sEHI. These results demonstrated that at the doses used TCC is anti-inflammatory in the murine model. This study suggests that TCC may provide some benefits in humans in addition to its antimicrobial activities due to its potent inhibition of sEH. It may be a promising starting point for developing new low volume high value applications of TCC. However these biological effects also caution against the general over use of TCC in PCPs.
Graphical abstractDownload high-res image (63KB)Download full-size imageResearch Highlights⺠Anti-microbial triclocarban (TCC) is anti-inflammatory in a murine model. ⺠TCC significantly shifted the oxylipin profile in vivo as expected from a sEHI. ⺠TCC significantly reversed LPS-induced morbid hypotension in a time-dependent manner. ⺠TCC significantly repressed LPS-induced increased release of inflammatory cytokines.
