The interaction of adenosine and dopamine in modulating the consequences of central nervous system oxygen toxicity

Benming You; Guorong Shi; Yanan Zhang; Xiang Fu; Qian Li; Yu Wang; Guoyang Huang; Yiqun Fang; Runping Li

doi:10.1152/japplphysiol.00500.2024

The interaction of adenosine and dopamine in modulating the consequences of central nervous system oxygen toxicity

J Appl Physiol (1985). 2024 Nov 27. doi: 10.1152/japplphysiol.00500.2024. Online ahead of print.

Authors

Benming You¹, Guorong Shi², Yanan Zhang³, Xiang Fu², Qian Li¹, Yu Wang¹, Guoyang Huang³, Yiqun Fang³, Runping Li³

Affiliations

¹ Department of Pharmacy, Changhai Hospital, Naval Medical University, Shanghai, China.
² Department of Pharmacy, Shidong Hospital of Shanghai Yangpu District, Shanghai, China.
³ Department of Diving and Hyperbaric Medicine, PLA Naval Medical Center, Naval Medical University, Shanghai, China.

PMID: 39601779
DOI: 10.1152/japplphysiol.00500.2024

Abstract

Hyperbaric oxygen (HBO) refers to pure oxygen with a pressure greater than 1 atmospheres absolute (ATA), and when the pressure is too high, it can cause convulsive attacks. Adenosine and dopamine have been shown to be closely associated with HBO induced convulsion seizures, and their receptors exhibited a coexisting relationship of mutual antagonism on the membrane of nerve cells. We explored the influence of adenosine and dopamine interplay on the occurrence of oxygen convulsion. Rats were individually exposed to HBO of 6 ATA and treated with adenosine, dopamine, and their receptor modulators separately and jointly, with the latency of convulsion onset recorded. Additionally, after administering adenosine to rats and exposing them to HBO for 30 min, the content of dopamine and its metabolites, as well as the activity of enzymes related to their metabolism, were measured. The results revealed that dopamine was effective in resisting convulsion (> 60 min vs 32.53±5.31 min, P=0.000), and low-dose adenosine partially counteracted its effect (> 60 min vs 28.18±6.24 min, P=0.002). The combined use of adenosine A1 and dopamine D1 receptor modulators significantly impacted the incidence of convulsion. The activation or inhibition of A2A receptor had a particularly significant impact on convulsion, while modulating D2 receptor did not affect their effects. The combination of A1 agonist and D2 agonist was highly effective in resisting convulsion (> 60 min vs 32.53±5.31 min, P=0.000). Exposure to HBO accelerated the metabolism of dopamine to its end products, which may be related to the enhanced activity of monoamine oxidase (MAO). Adenosine can inhibit MAO activity (0.0766±0.0150 U/mg.prot vs 0.1055±0.0086 U/mg.prot, P=0.004), maintaining a higher level of dopamine (1.820±0.379 mg/g vs 0.602±0.087 mg/g, P=0.000). The study demonstrated that dopamine plays a significant role in oxygen convulsion, and adenosine can affect dopamine metabolism. The interaction between them can have a crucial impact on the occurrence of oxygen convulsion. The findings offer a novel perspective for further investigating the mechanism of oxygen convulsion and exploring effective preventive strategies.

Keywords: adenosine; central nervous system oxygen toxicity; dopamine; interaction; oxygen convulsion.

Grants and funding

82072103/MOST | National Natural Science Foundation of China (NSFC)