Savory Signaling: T1R Umami Receptor Modulates Endoplasmic Reticulum Calcium Store Content and Release Dynamics in Airway Epithelial Cells.
Derek B McMahonJennifer F JolivertLi Eon KuekNithin D AdappaJames N PalmerRobert J LeePublished in: Nutrients (2023)
T1Rs are expressed in solitary chemosensory cells of the upper airway where they detect apical glucose levels and repress bitter taste receptor Ca 2+ signaling pathways. Microbial growth leads to a decrease in apical glucose levels. T1Rs detect this change and liberate bitter taste receptor signaling, initiating an innate immune response to both kill and expel pathogens through releasing antimicrobial peptides and increasing nitric oxide production and ciliary beat frequency. However, chronic inflammation due to disease, smoking, or viral infections causes a remodeling of the epithelial airway. The resulting squamous metaplasia causes a loss of multi-ciliated cells and solitary chemosensory cells, replaced by basal epithelial cells. To understand how T1R function is altered during disease, we used basal epithelial cells as a model to study the function of T1R3 on Ca 2+ signaling dynamics. We found that both T1R1 and T1R3 detect amino acids and signal via cAMP, increasing the responsiveness of the cells to Ca 2+ signaling stimuli. Either knocking down T1R1/3 or treating wild-type cells with MEM amino acids caused a reduction in ER Ca 2+ content through a non-cAMP signaled pathway. Treatment with amino acids led to a reduction in downstream denatonium-induced Ca 2+ -signaled caspase activity. Thus, amino acids may be used to reduce unwanted apoptosis signaling in treatments containing bitter compounds.
Keyphrases
- induced apoptosis
- cell cycle arrest
- amino acid
- endoplasmic reticulum stress
- oxidative stress
- cell death
- nitric oxide
- signaling pathway
- endoplasmic reticulum
- sars cov
- high grade
- adipose tissue
- blood pressure
- metabolic syndrome
- multidrug resistant
- microbial community
- low grade
- blood glucose
- insulin resistance
- hydrogen peroxide
- diabetic rats
- replacement therapy