Longitudinal impact on rat cardiac tissue transcriptomic profiles due to acute intratracheal inhalation exposures to isoflurane.
Sung-Hyun ParkYuting LuYongzhao ShaoColette PropheteLori HortonMaureen SiscoHyun-Wook LeeThomas KluzHong SunMax CostaJudith ZelikoffLung-Chi ChenMitchell D CohenPublished in: PloS one (2021)
Isoflurane (ISO) is a widely used inhalation anesthetic in experiments with rodents and humans during surgery. Though ISO has not been reported to impart long-lasting side effects, it is unknown if ISO can influence gene regulation in certain tissues, including the heart. Such changes could have important implications for use of this anesthetic in patients susceptible to heart failure/other cardiac abnormalities. To test if ISO could alter gene regulation/expression in heart tissues, and if such changes were reversible, prolonged, or late onset with time, SHR (spontaneously hypertensive) rats were exposed by intratracheal inhalation to a 97.5% air/2.5% ISO mixture on two consecutive days (2 hr/d). Control rats breathed filtered air only. On Days 1, 30, 240, and 360 post-exposure, rat hearts were collected and total RNA was extracted from the left ventricle for global gene expression analysis. The data revealed differentially-expressed genes (DEG) in response to ISO (compared to naïve control) at all post-exposure timepoints. The data showed acute ISO exposures led to DEG associated with wounding, local immune function, inflammation, and circadian rhythm regulation at Days 1 and 30; these effects dissipated by Day 240. There were other significantly-increased DEG induced by ISO at Day 360; these included changes in expression of genes associated with cell signaling, differentiation, and migration, extracellular matrix organization, cell-substrate adhesion, heart development, and blood pressure regulation. Examination of consistent DEG at Days 240 and 360 indicated late onset DEG reflecting potential long-lasting effects from ISO; these included DEG associated with oxidative phosphorylation, ribosome, angiogenesis, mitochondrial translation elongation, and focal adhesion. Together, the data show acute repeated ISO exposures could impart variable effects on gene expression/regulation in the heart. While some alterations self-resolved, others appeared to be long-lasting or late onset. Whether such changes occur in all rat models or in humans remains to be investigated.
Keyphrases
- late onset
- heart failure
- early onset
- gene expression
- oxidative stress
- extracellular matrix
- single cell
- liver failure
- blood pressure
- atrial fibrillation
- left ventricular
- air pollution
- respiratory failure
- dna methylation
- newly diagnosed
- end stage renal disease
- drug induced
- heart rate
- ejection fraction
- big data
- stem cells
- binding protein
- adipose tissue
- magnetic resonance imaging
- endothelial cells
- intensive care unit
- machine learning
- cystic fibrosis
- metabolic syndrome
- pulmonary hypertension
- cell therapy
- pulmonary artery
- percutaneous coronary intervention
- risk assessment
- long non coding rna
- peritoneal dialysis
- cardiac resynchronization therapy
- staphylococcus aureus
- mitral valve
- weight loss
- wound healing