Jiao-tai-wan for insomnia symptoms caused by the disharmony of the heart and kidney: a study protocol for a randomized, double-blind, placebo-controlled trial

The PSQI will be used at the baseline and the end of the drug intervention. The PSQI version used in this study is a 19-item self-reported retrospective questionnaire to access the quality of sleep in the past 7 days, and it is designed to measure seven domains called component scores: subjective sleep quality; sleep latency; sleep duration; habitual sleep efficiency; sleep disturbances; use of sleep medications; and daytime dysfunction [16, 17]. Component scores range from 0 (no difficulty) to 3 points (severe difficulty), and when summed, produce a global score in the range of 0–21. A higher score denotes worse sleep. These syndromes are categorized as mild (0–1), moderate (2–7), or severe (≥ 8) [18]. Then, the scores the participants obtained at baseline will be recorded as score 0, and the scores obtained at the end of drug intervention will be recorded as score 1. The recorder will calculate the reduction rate (RR) according to the following formula: RR = (score 1–score 0)/score 0*100%. Finally, we will assess the clinical curative effect of every participant based on the results of the RR. RR values > 75% will be regarded as a clinical cure, RR values between 50%–75% will be considered as a clinical effective, RR values between 25%–50% will be recognized as a clinical success, and RR values < 25% will be considered ineffective. The primary outcome is defined to have a value of 0 if RR is < 25% (ineffective) and 1 if RR is > 25% (clinical cure, clinically effective, or clinical success). The proportion of 1s (i.e. RR ≥ 25%) will be compared between the treatment and placebo groups.

In addition, Liu et al. [18] presented their opinion that the PSQI is suitable for Chinese patients after they conducted reliability and validity tests [19].

Polysomnography (PSG) will be taken twice, at both the baseline and the end of the drug intervention. On the first night, participants will adapt themselves to the laboratory environment. On the second night, participants will be placed on PSG monitoring to record the multiple physiological sleep parameters. The parameters [20, 21] will include total sleep time, sleep efficiency, sleep latency, rapid eye movement (REM) stage latency, wake after sleep onset, and the time duration of the particular sleep stages (such as N1, N2, N3). The mean changes of all the parameters from the baseline to the end of the drug intervention will be used to measure the changes in sleep quality.

PSG is considered the gold standard for scoring sleep disorders. The scoring of sleep and arousals relies on visual inspection of continuous surface electroencephalography (EEG), electromyography (EMG), and electrooculography (EOG) during PSG and then divides human sleep into five stages: wakefulness (W); REM; non-rapid eye movement (NREM); and N1, N2, and N3 [22]. The American Academy of Sleep Medicine (AASM) defined the quantitative reference standard in PSG for adult insomnia as follows [23]: sleep latency ≥ 30 min; total sleep time < 390 min; number of wake after sleep onset (WASO) ≥ 2 or time of WASO ≥ 40 min; time in N1/total sleep time > 60%; time in N2 / total sleep time > 60% or time in N3/total sleep time < 10%, or time in REM / total sleep time < 20%. A higher or lower score corresponds to more severe symptoms.

¹H-magnetic resonance spectroscopy (¹H-MRS) will also be taken at the baseline and the end of the drug intervention. ¹H-MRS, with its unique non-invasive advantages, is able to detect and quantify the important metabolites of living brain tissue, including N-acetylaspartate (NAA), choline (Cho), creatine (Cr), gamma-aminobutyric acid (GABA), and myo-intositol (mI) [24]. In the present study, single voxel hippocampus and thalamus metabolite ratios of GABA with Cr will be measured. The altered ratios of GABA with Cr between baseline and the end of the drug intervention will be the second outcome measure.

Studies have revealed that the GABA/Cr ratio in the frontal lobe is significantly lower [25], and the average brain GABA levels are nearly 30% lower in patients with primary insomnia [26].

The Disharmony of Heart and Kidney Scoring System will be used at the baseline and the end of drug intervention. It is a checklist covering one indispensable and seven accompanying items. These items are the symptoms and signs of the disharmony of heart and kidney pattern according to the theory of the pattern identification system in traditional East Asia medicine. The score of the indispensable item uses a 4-point scale (0, 3, 6, and 9) depending on the severity of the insomnia (0 = none, 9 = very severe). The seven accompanying items including palpitations, dizziness, spermatorrhea or menstrual irregularity, and night sweat and use scale of 0–4 points based on their frequency. A total score of > 9 out of 30 points is thought to demonstrate disharmony of the heart and kidney [27, 28].

Although there is no accurate evidence to explain the validity and reliability of this questionnaire, no other methods are currently available to identify the disharmony of heart and kidney pattern.

Blood tests consists of the levels of adenosine (AD) and melatonin (N-acetyl-5- methoxytryptamine) in blood samples will be recorded at the baseline and the end of the drug intervention and will then be analyzed by the clinical lab.

Sleep homeostasis in adults is affected by the sleep-regulatory substances AD and melatonin [29, 30]. AD is a product of brain metabolism and is closely related to sleep parameters. A previous study [31] showed that AD levels were elevated as a consequence of sustained wakefulness. Melatonin is an endogenous hormone produced by the pineal gland and is released exclusively at night. Melatonin has been shown to synchronize the circadian rhythms, and improve the onset, duration, and quality of sleep. Takaesu et al. thought that reduced secretion of melatonin may be involved in the mechanism of insomnia [32].

In the present study, high-performance liquid chromatography (HPLC) will be developed to determine the levels of adenosine, and an enzyme-linked immunosorbent assay will be used to detect the concentration of melatonin.