To the Editor:
Obstructive sleep apnea (OSA) can cause cognitive impairment, affect the quality of life of patients, and increase the burden on families and society. It has attracted the attention of more and more researchers, and there are also studies that point out the cognitive function of OSA. Most of them are mainly mild damage, and the specific mechanism is still unclear (1).With interest, we read the paper by Djonlagic and colleagues (2), which indicates that 3 months of nocturnal continuous positive airway pressure (CPAP) treatment can increase N3 sleep proportionally to the level of the healthy control group, thereby alleviating the declarative memory deficits of patients with OSA. From the data in the study, it can be seen that apnea–hypopnea index has dropped from 34.7 ± 7.5 to 3.6 ± 0.7 events/h, which reduces arousal and increases the time of the deep sleep N3 phase (mainly slow-wave sleep). The increase of slow-wave sleep helps the recovery of the key memory system in the brain.
Djonlagic and colleagues (2) did not show whether declarative memory deficit is related to hypoxia, because the oxygen nadir of patients with OSA is lower than normal, and it increases after treatment. However, studies have shown that sleep deprivation in individuals without OSA can severely impair cognitive functions such as attention, memory, and decision-making, especially affecting the execution of tasks that require a high degree of concentration and rapid response (3). The study by Canessa and colleagues (4) found that before CPAP treatment, most areas of cognitive function of patients were impaired. These damages are related to the decrease in the volume of gray matter in the left hippocampus, left posterior parietal cortex, and right frontal gyrus. After 3 months of CPAP treatment, the patients’ memory, attention, and executive functions improved significantly, which paralleled the increase in the volume of gray matter in the hippocampus and frontal lobe structure. It is believed that the cognitive impairment and brain structure damage in patients with OSA may be related to sleep deprivation and repeated intermittent hypoxemia at night, and these damages can be restored by continuous and thorough CPAP treatment. It provides an anatomical basis for OSA cognitive dysfunction and confirms the importance of early diagnosis and treatment of OSA. The possible mechanism is that sleep apnea in patients with OSA leads to hypoxia and changes in sleep structure, which disrupts the functional homeostasis of brain cells and changes the activity of neurons and glial cells in specific areas of the brain (such as frontal and temporal lobes) (5). Some scholars also believe that sleep fragmentation is one of the key mechanisms of OSA cognitive impairment (6).
These findings give us important hints that slow-wave sleep is very important for stabilizing and strengthening declarative memory traces. The question remains whether the duration of the N3 period in sleep monitoring can be used as a predictive indicator to assess the cognitive function of patients, the cutoff of which can be obtained by monitoring in a large sample of patients with and without cognitive dysfunction, so as to screen out high-risk cognitive dysfunction populations for further examination and then targeted treatment for the patients. With the aging of the population and the increasing incidence of cognitive dysfunction, early screening and early intervention are of great significance.
Based on the above points of view, although the sample size is small, the study by Djonlagic and colleagues (2) showed that the shortened N3 stage of sleep of patients with OSA leads to declarative memory deficit and that CPAP can be used to recover. Whether N3 sleep can be used as a predictor of early cognitive dysfunction is worth exploring.
Acknowledgments
Acknowledgment
The authors thank Prof. Nanshan Zhong from the State Key Laboratory of Respiratory Disease for the constructive advice he gave.
Footnotes
Supported by the Natural Science Foundation of Guangdong Province (No. 2021A1515011373), the Zhongnanshan Medical Foundation of Guangdong Province, and the Penghua Care Fund to the Medical Pioneers against COVID-19 of Shenzhen Social Commonwealth Foundation (2020B1111340010).
Author Contributions: All authors contributed to the writing, review, and approval of the final copy of the manuscript.
Originally Published in Press as DOI: 10.1164/rccm.202105-1231LE on September 3, 2021
Author disclosures are available with the text of this letter at www.atsjournals.org.
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