Category

Archives

Nrf2 transcriptional activity in the mouse affects the physiological response to tribromoethanol

Up to date, there is no information on the influence of 2,2,2-tribromoethanol (TBE; Avertin), a commonly used anaesthetic, on mice with impaired antioxidant capacity. We aimed to analyse the effect of a single dose of Avertin on anaesthesia duration time, inflammatory response, oxidative stress and collagen deposition in the large intestine of Nrf2 transcriptional knockout mice (tNrf2-/-). The studies were performed on six-month-old female mice Nrf2+/+ and tNrf2-/- randomly assigned to Avertin (250 mg/kg b.w. single i.p. injection) or vehicle group. We observed a 2-fold increase in anaesthesia time and longer recovery time (p = 0.015) in tNrf2-/- in comparison to Nrf2+/+. However, no hepato- or nephrotoxicity was detected. Interestingly, we found severe changes in colon morphology of untreated tNrf2-/- mice associated with colon shortening (p = 0.02) and thickening (p = 0.015). Avertin treatment caused colon damage manifested with epithelial layer damage and goblet depletion in Nrf2+/+ mice but not in tNrf2-/- individuals. Additionally, Avertin did not induce oxidative stress in colon tissue, but it increased leukocyte infiltration in Nrf2+/+ mice (p = 0.02). Immunofluorescent staining also revealed enhanced deposition of collagen I and collagen III in the colon of untreated tNrf2-/- mice. Avertin contributed to increased deposition of collagen I in Nrf2+/+ mice but reduced deposition of collagen I and III in tNrf2-/- individuals. In conclusion, tNrf2-/- respond to Avertin with prolonged anaesthesia that is not associated with acute toxicity, inflammatory reaction or enhanced oxidative stress. Avertin does not impair intestine morphology in tNrf2-/- mice but can normalise the enhanced fibrosis.

 

Comments:

It seems that your study aimed to investigate the effects of 2,2,2-tribromoethanol (TBE; Avertin) on mice with impaired antioxidant capacity. Here is a summary of your findings:

A single dose of Avertin (250 mg/kg b.w. single i.p. injection) caused a 2-fold increase in anaesthesia time and longer recovery time in tNrf2-/- mice compared to Nrf2+/+ mice.
Avertin did not cause hepato- or nephrotoxicity in either tNrf2-/- or Nrf2+/+ mice.
Untreated tNrf2-/- mice showed severe changes in colon morphology, including colon shortening and thickening, as well as enhanced deposition of collagen I and collagen III in the colon.
Avertin caused colon damage manifested with epithelial layer damage and goblet depletion in Nrf2+/+ mice but not in tNrf2-/- individuals.
Avertin did not induce oxidative stress in colon tissue, but it increased leukocyte infiltration in Nrf2+/+ mice.
Avertin contributed to increased deposition of collagen I in Nrf2+/+ mice but reduced deposition of collagen I and III in tNrf2-/- individuals.
Based on these findings, it appears that tNrf2-/- mice respond to Avertin with prolonged anaesthesia without acute toxicity, inflammatory reaction, or enhanced oxidative stress. Avertin does not impair intestine morphology in tNrf2-/- mice but can normalize the enhanced fibrosis. These results suggest that Nrf2 deficiency may affect the response to Avertin anesthesia and should be taken into account in future studies.

Related Products

Cat.No. Product Name Information
S4508 2,2,2-Tribromoethanol 2,2,2-Tribromoethanol (TBE, Tribromoethanol) is an organic compound used to anesthetize animals.

Related Targets

Others