This is a prospective, randomized, double-blind, placebo-controlled trial. This trial was registered with the Chinese Clinical Trial Registry on November 26, 2020 (ChiCTR2000040270). This study was approved by the Research Ethics Committee at Guangdong Provincial Hospital of Traditional Chinese Medicine (BF2020-085-01). The trial complies with the Helsinki Declaration and the 2020 Good Clinical Practice guidelines. All 98 patients in this trial will be from Guangdong Provincial Hospital of Traditional Chinese Medicine. After they provide written informed consent, they will be randomly assigned to receive either QSHTD or a placebo. The study will consist of a 12-week intervention phase followed by a 12-week monitoring phase. A schematic representation of the study design is provided in
Study flowchart.
Study procedure table.
| Study phase time | Baseline | Intervention period | Follow-up | ||
|---|---|---|---|---|---|
| −2∼0 weeks | 4 weeks | 8 weeks | 12 weeks | 24 weeks | |
| Data collection at baseline | |||||
| Informed consent | √ | ||||
| Inclusion/exclusion criteria | √ | ||||
| Random number | √ | ||||
| Demographic data | √ | ||||
| Disease condition | √ | ||||
| Medical history | |||||
| Vital signs | √ | √ | |||
| Physical examination | √ | √ | |||
| Medication situation | √ | √ | √ | √ | √ |
| Laboratory testing and other tests | |||||
| Blood analysis | √ | √ | |||
| Urine analysis | √ | √ | |||
| Fecal analysis + OB | √ | √ | |||
| Biological sample | √ | √ | |||
| Electrocardiogram | √ | √ | |||
| Echocardiography | √ | √ | |||
| RTMPE | √ | √ | |||
| Efficiency evaluation | |||||
| TCM symptom scores | √ | √ | √ | ||
| CCSC | √ | √ | √ | ||
| SAQ | √ | √ | √ | ||
| Other data | |||||
| AEs | √ | √ | √ | √ | √ |
| SAEs | √ | √ | √ | √ | √ |
| Compliance | √ | √ | √ | √ | √ |
| Complications | √ | √ | √ | √ | √ |
| Clinical end-point events | √ | √ | √ | √ | √ |
OB, occult blood; HCY, homocysteine; HbA1c, glycated hemoglobin; hsCRP, high sensitivity C-reactive protein; MCE, myocardial contrast echocardiography; AEs, adverse events; SAEs, serious adverse events. “√” Represents the need for implementation at this point in time.
According to the 2013 ESC guidelines on the management of stable coronary artery disease, if coronary angiography results show any coronary artery stenosis exceeding 50%, the patient has CHD (
The calculation was based on the syntax score published in the
The subjects must meet both the 2017 clinical diagnostic criteria for phlegm-damp syndrome in CHD (
Diagnostic criteria for phlegm-damp syndrome.
| Symptom type | Score | Item(s) |
|---|---|---|
| Main symptoms | 3 points/item | 1. Plump and teeth-printed tongue |
| 2. Greasy tongue fur | ||
| 3. Slippery tongue fur | ||
| Secondary symptoms | 2 points/item | 1. Oppression in chest |
| 2. Soft or slippery pulse | ||
| Other symptoms | 1 points/item | 1. Body trapped |
| 2. Sticky and greasy in mouth | ||
| 3. Obesity | ||
| 4. Viscous stool | ||
| 5. Distention and fullness | ||
| 6. Dim and dirty complexion | ||
| 7. Analeptic | ||
| 8. Anorexia |
The diagnosis of phlegm dampness syndrome in coronary heart disease requires a cumulative score of ≥6 points on the indicators mentioned.
Diagnostic criteria for dampness syndrome.
| Indicator type | Content | |
|---|---|---|
| Specific indicators | Category 1 | 1.1 Greasy tongue |
| 1.2 Slippery coating | ||
| 1.3 Thick coating | ||
| Category 2 | 2.1 Head heaviness as if being wrapped up | |
| 2.2 Body heaviness | ||
| 2.3 Limb heaviness | ||
| 2.4 Limited joint motion with heavy sensation | ||
| Category 3 | 3.1 Sticky stool with non-smooth bowel movement | |
| 3.2 Sticky and greasy sensation in mouth | ||
| 3.3 Excessive morbid leucorrhea/moist scrotum | ||
| 3.4 Greasy hair | ||
| Sensitivity indicators | Items | 1. Obesity |
| 2. Somnolence | ||
| 3. Idleness and laziness | ||
| 4. Non-smooth hidrosis | ||
| 5. Dirty face | ||
| 6. Dizziness | ||
| 7. Fullness and oppression in chest | ||
| 8. Excessive phlegm | ||
| 9. Distention and fullness in the epigastric region | ||
| 10. Lower abdominal fullness | ||
| 11. Soreness and weakness in the waist and knees | ||
| 12. Soreness in the joints and muscles | ||
| 13. Absence of thirst or thirst without desire to drink | ||
| 14. Poor appetite | ||
| 15. Loose stool | ||
| 16. Fetid mouth odor | ||
| 17. Enlarged tongue | ||
| 18. Soft pulse | ||
| 19. Slippery pulse | ||
The diagnostic principle of dampness syndrome: If any one of the following conditions is met, dampness syndrome can be diagnosed: ① Meeting any one category of a specific indicator. ② Having three sensitivity indicator items. Note 1: Specific indicators are measured in category units; sensitivity indicators are measured in item units. Note 2: Specific indicators belonging to the same category, whether there is only one or multiple at the same time, are counted as one specific indicator of the same category.
Age range is from 18 to 80 years old.
PCI performed within the previous 2 years and rSS ≥ 2 points; or PCI was performed at least 2 years before and coronary angiography was performed within the previous 2 years with rSS ≥ 2 points; or PCI was performed at least 2 years before and there is untreated or unsuccessfully treated chronic total occlusion.
Meet the 2017 clinical diagnostic criteria for phlegm-damp syndrome in CHD, as well as the dampness syndrome diagnostic criteria.
Agree to undergo adenosine stress real-time myocardial perfusion echocardiography (RTMPE).
A signed consent form is required.
Cardiogenic shock.
Severe heart failure (New York Heart Association classification stages II–IV, or left ventricular ejection fraction ≤ 50%), or comorbid with severe valvular disease.
Severe liver or kidney dysfunction (serum alanine aminotransferase of at least double the normal upper limit and/or serum creatinine ≥ 265 μmol/L).
Patients with other vascular diseases, such as cerebrovascular disease, arteriosclerosis obliterans of the lower limbs or diabetes nephropathy.
Patients with active bleeding or severe hematopoietic system disease.
Patients with malignant tumors who are undergoing chemotherapy or radiotherapy who have not been clinically cured, or those who have been treated with special drugs for malignant tumors, or with life expectancy under 3 years.
Taken antibiotics within the previous 2 weeks.
Pregnant (or preparing to become pregnant) women, lactating women.
Have participated in, or are participating in, other clinical trials within the past 3 months.
The researcher determined that the participant was unable to finish the study or adhere to its requirements.
The research will include participants from both the outpatient and inpatient departments of the Guangdong Provincial Hospital of Traditional Chinese Medicine. Subjects who meet the eligibility criteria and provide informed consent will advance to a screening phase, while those who do not fulfill these requirements will be excluded prior to randomization. Principal investigators and attending physicians will jointly conduct eligibility assessment for enrolled participants based on specific inclusion/exclusion criteria. Registered participants will then be allocated through an online system for intervention and follow-up phases of the experiment. Ineligible individuals' demographic data, as well as any reasons for non-participation, will also be documented alongside strict confidentiality measures.
The randomization process will employ a block randomization method. 98 patients will be randomly allocated into two groups at a ratio of 1:1 using block randomization. Each block will consist of 49 cases with random sequence arrangements within the blocks. We plan to use the PROC PLAN procedure in SAS V9.4 for this study. The results of both the randomization and the allocation procedures were conducted by researchers from the Clinical Research Methodology Team at Guangdong Provincial Hospital of Traditional Chinese Medicine. The random assignment procedure was registered with the TCM Clinical Research Methodology Team at Guangdong Provincial Hospital of Traditional Chinese Medicine. Random assignment results will be generated and released via a centralized randomization management system. Researchers will log into an online randomization system to apply for randomization and receive the randomization results.
This trial will be conducted in a double-blind manner, ensuring that neither the participants nor the research staff are aware of the group assignments. The Jiangyin Tianjiang Pharmaceutical Co., Ltd. (Jiangyin, China) will produce both the QSHTD and the placebo granules. The placebo will be designed to closely resemble the QSHTD in all aspects, such as color and flavor. All medications will adhere to the standards set by the National Drug Manufacturing Code of China. The blinding process and the maintenance of the blind will be handled by the TCM Clinical Research Methodology Team at Guangdong Provincial Hospital of Traditional Chinese Medicine. An emergency letter for each drug code will be created during the randomization and blinding process, and it will be securely sealed according to the corresponding drug group. If a serious adverse event (SAE) occurs or if urgent medical care is required, the principal investigator can use the online randomization system to request unblinding. When unblinding becomes inevitable, the participant will be excluded from the study, and the investigator must inform the examiner of the cause within 24 h. If unblinding is essential, the individual will be removed from the research, and the investigator must convey the reasons to the examiner within a 24-hour period.
Referring to the 2018 ESC Guidelines for Coronary Artery Revascularization, all subjects will be given antiplatelet drugs, statin lipid-lowering drugs, nitrate esters, anticoagulants, and
The participants in the experimental group will receive standard care along with QSHTD (two 7.4 g packets, taken orally twice daily after meals) for a duration of 12 weeks, and the entire observation and follow-up period will span 24 weeks.
The control group participants will receive standard care along with placebo granules (two 7.4 g packets, taken orally twice daily after meals) for a duration of 12 weeks. The entire observation and follow-up period will span 24 weeks.
Use of any other traditional Chinese patent medicines or decoctions will be prohibited during the test.
Any patients entering the screening period must discontinue the usage of any long-acting nitrate drugs (such as long-acting nitroglycerin) or any other anti-angina treatments. However, they may continue using a beta-blocker and/or calcium channel blocker if they are taking one.
Throughout the study period, patients will be prohibited from adding or using any of the following medications, in addition to maintaining their original medication: beta blockers, calcium antagonists, nitrate drugs (except for the use of short-acting nitroglycerin for angina attacks).
Any medications or treatments necessary for managing coexisting conditions should be documented, including the drug name (or other treatment name), dosage, frequency of use, and duration. This data is crucial for both analysis and reporting.
The main endpoint is the change in myocardial blood flow (MBF), assessed through adenosine stress RTMPE, following a 12-week treatment period.
(1) Canadian Cardiovascular Society Classification (
Our team will meticulously document the exact timing, intensity, duration, interventions applied, and potential outcomes of all adverse incidents. For each documented incident, the investigator will also assess the connection between the adverse events and the medications under study. In line with ICH guidelines, SAEs will be classified as any occurrences that could lead to hospitalization, inability to work, birth defects, or fatalities (
The sample size calculation will be based on the mean and standard deviation of the variation in MBF. According to the literature, the MBF variation in a conventional treatment group increased by 0.52 ± 0.72 (dB/s) after 12 weeks, while in the conventional combined TCM treatment group, MBF variation increased by 0.97 ± 0.68 (dB/s) after 12 weeks (
Data analysis will be performed using SAS 9.2 (SAS Institute Inc., USA) according to a pre-established statistical plan. The evaluation of effectiveness will adhere to the intention-to-treat principle. Quantitative data will be analyzed using methods such as ANOVA. Categorical data will be evaluated with chi-square tests and Fisher's exact test, while non-parametric rank sum tests and CMH chi-square tests will be used for ordinal data. The significance level will be set at
To guarantee the enforcement of quality control and assurance in clinical research, the researchers will carry out their responsibilities, adhere to the clinical trial protocol, utilize standard operating procedures, and validate all pertinent observations and results. In these studies, the allocation of participants must be based on the study design. For a randomized assignment, the statistical unit will determine each participant's treatment group, and this information will be kept confidential from the researchers. Researchers are required to provide essential training to all personnel involved in the clinical trial, disseminate relevant data, operational procedures, and/or roles, and ensure that the data is reliable, precise, comprehensive, and timely. This data must also be legally documented in medical records and CRFs, which should be stored securely. Monitors will conduct systematic reviews of the activities and materials pertaining to clinical trials must be evaluated for adherence to the study protocol, standard operating procedures, and pertinent legal and regulatory requirements. It is essential that all clinical laboratory results are documented, with a duplicate of the initial report appended to the CRFs. The clinical investigation will follow the sanctioned protocol, with any deviations from it being documented. Any adjustments to the study protocol must be detailed and submitted to the ethics committee for authorization before being enacted. Participants adhering to the regimen for 80% or more of the prescribed time will be considered highly compliant. All non-adherence instances and their causes will be documented.
Physicians participating in clinical trials must provide subjects with detailed information about the clinical trial, so that they can comprehend and voluntarily sign an informed consent form before the clinical trial commences. Participants are free to exit the trial at any point and for any cause; signing the informed consent document and meeting the eligibility criteria will not impact their future medical care. Although individuals have the freedom to exit the study whenever they wish and for any reason, it is advisable to refrain from doing so unless there is a significant necessity. Additionally, measures should be undertaken to complete as much follow-up as possible. This will enable the evaluation of its efficacy and safety.