Study objective
The objectives of the experiment is to study the efficacy and safety data of Chinese medicine therapy for dampness syndrome of hyperuricemia; And to screen possible related intuitive small molecules/microbial material basis.
Study design
This is a 12 weeks, single-center prospective, double-blinded, randomized, placebo controlled clinical trial. We used the SPIRIT reporting guidelines to perfecting this protocol[19]. From March 2020 to December 2021. Incorporate 30 asymptomatic hyperuricemia subjects, which will be randomly 1:1 assigned to receive Chinese medicine or placebo.
Sample size
This study will enroll 30 subjects. Further large-scale RCT trial will estimate the size of sample according to the results of the main outcome indicators obtained from this study, use the sample content estimation formula for comparing the two means to calculate the sample content, α=0.025,β=0.2, The sample size ratio of test group and control group is 1, The lost follow-up rate is set according to the pre-experiment lost follow-up rate.
Recruitment
Most asymptomatic patients with hyperuricemia do not seek for medical attention, so we will recruit subjects through recruitment advertisements. The advertisements will be placed in the hospital building, and be broad through the hospital official account.
Study setting
Guangdong provincial hospital of Chinese medicine will be the only study setting.
The study’s key problem
Dampness is involved with Hyperuricemia developing. The key of prevent gout, cardiovascular disease and uratic nephropathy is control the serum uric acid level. Weather Chinese medicine can improve the outcomes of hyperuricemia population, access the goal of early prevent disease?
Eligibility criteria
Inclusion criteria:
- Aged between 18-75 years(including 18 years and 75 years;
- Meet the diagnosis of asymptomatic hyperuricemia;
- Meet the dampness syndrome inclusion criteria;
- Sign the informed consent.
Exclusion criteria:
1) Secondary hyperuricemia,for instance,secondary to malignancy,hemopathy,nephropathy,chronic intoxication;
2)History of alcoholism without abstinence in recent 3 months;
3)Had one or more attacks of gout arthritis in the past;
4)Received urate-lowing drugs or drugs that may increase serum uric acid in recent 4 weeks: (1) antituberculotic:Pyrazinamide/ethambutanol/isoniazid, (2) low dose aspirin, (3) Loop diuretics and thiazide diuretics and blood pressure medications containing diuretics, (4) niacin, (5) large dosage of vitamin C, (6) chemotherapeutic drugs, (7) cyclosporin;
5) Pregnancy and lactation population, or has possibility of conception but failure to use effective contraception;
6) Alanine aminotransferase or aspartate aminotransferase or creatinine 2 times or more than the normal value;
7) Combined with serious organic lesions, mental disorders or other reasons can not cooperate with treatment; 8) Allergic or ineffective to the test drug ingredients.
Randomization and allocation
Adopting simple block group randomization, the allocation ratio will be 1:1. Use SAS9.2 PROC PLAN to carry out procedure coding and random sequence generation by methodology team.
The random distribution results will released through the “Interactive network response random distribution System for Clinical Research in Guangdong provincial hospital of Chinese medicine. The random assignment table in the random Center will be kept strictly confidential until the end of the study.
After the patients are screened as qualified subjects and given informed consent, the clinicians will log on the Internet to apply for the randomization system to obtain the randomization results. Physicians execute the results according to random grouping, and print and paste them on the corresponding position of CRF.
Blind
Adopt double-blinded, placebo controlled design, both the investigators and the subjects are blinded.All data will be evaluated and statistically processed by a third-party after the clinical research.
The blindness should be broken if there is a serious adverse event that may be related to the experimental drug, so we can know which group the subject was enrolled in to decide the rescue plan. The blindness should be broken in the presence of principal investigator and funders. The time, reason, procedure of the unblinding and the the researchers involved in the unblinding should be recorded. After the blindness was broken, the subject will be terminated from the study, and the experimental data will be included in the safety analysis data set, and the subject was given timely treatment and follow-up.
Comparators
Many Chinese medicine studies set Chinese medicine plus western medicine as the experimental group and soly modern medicine as the control group. This may lead to bias. So we use placebo control group as the comparators.
Chinese medicine syndrome subgroups
All enrolled subjects will be assigned to subgroups: cold-dampness disturbing spleen and damp-heat retention spleen. The definition of which is to draw up with refer to “The guiding Principles for clinical Research of New Chinese medicines (trial)” in 2002, which was edited by Zheng Xiaoyu[20].
Interventions
Subjects will be given therapeutic agent (Chinese medicine) or placebo.
Chinese medicine intervention group: 1) Cold-dampness disturbing spleen: Tuckahoe alisma soup, one dose a day, warm take after meal. 2) Damp-heat retention spleen: Scutellaria and ginger pinellia soup, one dose a day, warm take after meal.
Chinese medicine placebo internal administration: the size, appearance, package and the the administration method are the same as the therapeutic drugs. During the trial, the investigators will monitor dietary and exercise conditions of subjects everyday.
Eliminate and Termination Criteria
Eliminate criteria: 1) Serious violation of exclusion standards after enrollment; 2)Not completing the experimental drug administration during the experimental period as required after enrollment; 3) Incomplete one month follow up, no test records were available for evaluation.
Termination Criteria: 1)Have a gout attack; 2) sever adverse events; 3) Condition deteriorated and required urgent medical attention; 4) The researcher recommended terminate test because of the safety of the subjects. 5)People unwilling to continue to participate in this study for personal reasons.
We will keep in touch with the subjects who drop out to observe any subsequent adverse event and collect subsequent data.
Strategies to improve adherence to interventions
The compliance of investigators and subjects is essential factors of clinical research process and clinical effect. To ensure compliance, investigators or the designated representative must explain the detailed information about the clinical trail to the subjects, and to obtain informed consent after sufficient and detailed explanation.
The compliance evaluation of the subjects is mainly judged from the status recorded by the subject's log card and the status questioned by the researchers.
Plans to promote participant retention and complete follow-up
First, the investigators will keep in touch with the subjects, regular telephone follow-ups and reminders for follow-up visits will be implement. Second, our research system will prompt the prescription a day in advance. Third, the subjects will receive free tests. Forth, transportation subsidies will be given after each follow-up visit to encourage subjects to remain engaged and complete follow-up surveys.
Outcome measures
Primary outcome measure
The reduction of serum uric acid.
Secondary outcome measures
1)Chinese syndrome score, measurement of the channels and collaterals, tongue diagnosis evaluation; 2) Glomerular filtration rate, Urinary β2 microglobulin, uric acid excretion fraction; 3) Incidence rate of complications, such as gout, hyperlipemia, cardiovascular events, diabetes, etc; 4) Ultrasound of double ankles and the first metatarsophalangeal joints[21]; 5) Evaluation index of metabolite: blood, urine metabolite. 6) Inflammation index: hsCRP, TNF-a, IL-6, IL-8; 7) Intestinal microecology( Note: This index is tested by setting a separate subject).
Security indicators
1)Liver function(ALT, AST) , renal function(Urea, Cr); 2) Blood routine, urine routine, stool routine + occult blood; 3) lectrocardiogram, ultrasound of the urinary system.
Data collection and analysis
Within 12 weeks course there will be 4 times of visits: 0 week, 4 weeks± 3days, 12 weeks± 5days, and the date collection and the filling of the CRF will be performed by two research assistants who have no idea about the subjects grouping. Adopt EPIdata3.1 database software package to establish a database for data entry, use double input data for data entry.
The clinical trial monitors check the quality of data entry regularly. The checked database is then checked by logic inspection and the original laboratory documents of outliers, and the finally checked database is converted into the DATABASE in the format of SPSS statistical software package and locked for statistical analysis.
Statistical analysis
All statistical tests are two-sided, α=0.05 will be found statistically.
We will use t-test (or wilcoxon matched-pairs signed-ranks test if the data is non-normal distribution with uneven variances) to compare the decrease in the uric acid between two groups.
For secondary outcomes, the t-test and Wilcoxon test will be conducted to compare the differences in measurement data (such as index’s mean and standard deviation, median) between the groups. The Repeated measures analysis of variance will be used to compare multiple measures of the scale and symptom rating among groups. The Chi-square test (or Fisher’s Exact test) and 3×C table will be utilized to determine the differences in the proportion, frequency, total effective rate of the indices in Chinese medicine group and placebo group.
To analysis the influence factors of curative effect, the nonconditional logistic regression analysis will be performed.For missing data from long-term follow-up, the last carry-over method (LOCF)will be used.
Safety analysis
Safety data is consist of adverse events and clinical laboratory tests. We will describe specific manifestations of adverse reactions and compare the incidence of adverse events and sever adverse events between two groups. The changes of laboratory test results before and after the test, abnormal changes and their relationship with Chinese medicine will be analysis.
Compliance analysis
A descriptive analysis are will be exploit to analyze compliance among the subgroups included in the study, and between the two groups for baseline of abscission cases.
Adverse events Management
The type, degree, occurrence time, duration, treatment measures, treatment process and follow-up results of adverse events occurred during the trial will be recorded in the case report form, and the correlation between the adverse events and the experimental drugs will be evaluated on the basis of comprehensive consideration of the complications and combined use of drugs, which will also be recorded in detail by the physician.
For non-serious adverse event, the observation physician may decide whether to suspend observation based on the disease condition. Cases that withdrawal drugs due to adverse event will be followed up and reexaminate the lab security indicators.
For serious adverse event, drug taking will be stopped immediately. Regardless of whether it is related to the experimental drug,the investigators should report to the Ethics Committee of Guangdong province hospital of Chinese medicine within 24 hours after its occurrence.
If a serious adverse event occurs during the course of the study, the research team and the hospital will be responsible for subsequent treatment and financial compensation.
Protocol amendments
If a protocol change is required, the risk to the subject should be fully assessed and reviewed by the Ethics Committee.Inform all members after the new scheme has been approved by email and face-to-face meeting.
Confidentiality
Subjects have independent codes and only enter codes when uploading test data. Encryption system will be utilized to upload and store datas. The final statistically process will be administrated by a third-party.