The last two decades of research on carbon dioxide have demonstrated that CO(2) is far more than a waste product of aerobic metabolism leading to acidosis, and that it elicits biological responses directly via non-pH-dependent molecular interactions. New specialized methodologies have mapped CO(2) incorporation into specific regions of CO(2)-sensitive proteins and linked these events to altered cellular function. CO(2) affects a host of biological responses related to respiratory disease, including control of respiration, protein maturation, alveolar fluid homeostasis, wound repair, innate immunity, host defense, and airway contractility. Elevated CO(2) (hypercapnia) appears to be primarily deleterious in pulmonary diseases, leading to a heightened interest in strategies to reduce excess CO(2) in patients with hypercapnic respiratory failure. Here, we summarize recently generated knowledge on molecular CO(2) sensing and signaling, and the potential translational relevance of these processes in the context of respiratory disease. We need to grow this field further by encouraging experts in basic and translational science to contribute to more fully elucidating CO(2) sensing, signaling and downstream effects. Understanding the biology and clinical consequences of perturbations in CO(2) homeostasis should no longer be considered secondary to studying oxygen sensing and signaling in respiratory medicine.
- Vadász, I.
- Cummins, E. P.
- Brotherton, D. H.
- Casalino Matsuda, S. M.
- Dada, L. A.
- Green, O.
- King, D. T.
- Kryvenko, V.
- Shigemura, M.
- Sporn, P. H. S.
- Strowitzki, M. J.
- Cann, M. J.
- Sznajder, J. I.
Keywords
- CO2 sensing
- CO2 signaling
- carbon dioxide
- hypercapnia
- respiratory failure
