Aims and objectives
This study aims to evaluate the therapeutic effect of Tui-na together with the oral DHJSD on the treatment of KOA in Hong Kong. The study will examine whether the proposed combined therapy can reduce pain intensity and improve knee function for subjects with KOA. The working hypothesis of this study is that application of Tui-na together with the oral administration of DHJSD is effective and safe in the treatment of KOA.
Design and setting
This will be a prospective, randomized wait-list controlled trial in subjects with KOA. After 2 weeks screening period, eligible subjects will be randomly assigned to the treatment group and wait-list control group in a 1:1 ratio. The total study period will be 10 weeks. The study flowchart is shown in Figure 1. The study will be conducted at the Yan Oi Tong - The Chinese University of Hong Kong Chinese Medicine Clinic cum Training and Research Centres (in Tuen Mun and Islands Districts), Hong Kong SAR, China.
Inclusion Criteria
Subjects will be recruited for the study if they meet all of the following criteria:
- Either gender;
- ≥ 50 years of age;
- Meet the criteria of KOA according to the American College of Rheumatology:
- Knee pain, and
- Any 4 of the following:
- ≥ 50 years of age;
- Less than 30 minutes of morning stiffness;
- Crepitus on active motion;
- Bony tenderness;
- Bony enlargement;
- No palpable warmth of synovium; and
- Osteophytes (based on radiographic findings).
- With WOMAC score ≥ 39,
- Able to sign the written informed consent form (for illiterate subjects, their next-of-kin or an impartial witness will sign with subjects’ permission).
Exclusion criteria
Subjects will be excluded if they possess any of the following criteria:
- Known knee pain caused by infection, malignant or autoimmune diseases;
- Knee surgery or arthroscopy in the past year;
- Chondroprotective or intra-articular injection in the past 4 months;
- Systemic corticosteroid treatment in the past 4 months;
- Currently taking anticoagulants, antiplatelets, psychiatric drugs, hormones, antiarrhythmic drugs or diuretics drugs;
- Uncontrolled hypertension;
- Local antiphlogistic treatment, acupuncture, physiotherapy in the past 2 weeks;
- Known history of mental disorder;
- Known history of serious acute organic disease;
- Renal or liver function impairment; and
- Known allergy to or have drug interaction with the study herb.
Recruitment
All subjects will be recruited from the general public via daily outpatient services and advertisements on various social media. Subjects interested in participating in the study will be referred to or self-approach the study sites to undergo eligibility assessment. They will be prescreened through a telephone interview. Potential subjects then will have a face-to-face interview to confirm eligibility. During the interview, assessors will explain the overall objectives and nature of the study, describe the informed consent process, and assess the subjects’ eligibility. The schedule of enrollment, interventions and assessments is shown in Table 1.
Follow-up visits
All subjects will be assessed using Chinese medicine theory by the registered Chinese medicine practitioners (RCMPs). The eligible subjects will be randomized into two groups, i.e., treatment group which will receive the standardized Tui-na and DHJSD, and the wait-list control group which will receive Tui-na alone during the study period. Subjects in the treatment group will undergo 8 sessions of 20 minutes Tui-na therapy, administered over 4 weeks and take study medication twice daily concomitantly for 4 weeks. The wait-list control group will receive standardized Tui-na therapy in the same manner with the treatment group but will not be given the DHJSD. Compensatory medication may be given after the completion of follow-up assessments at subject’s discretion. Both groups will be assessed at day 0 (baseline), day 14 ± 3 days (week 2), and day 28 ± 4 days (week 4), and further followed up on day 56 ± 4 days (at week 8, i.e., 4 weeks after treatment completion).
All outcome assessments will be done at baseline (0 week), 2 weeks, 4 weeks after randomization and follow-up (4 weeks after treatment completion).
If the subject has bilateral KOA and both knees fulfil the eligibility criteria, the WOMAC index and EQ-5D-5L are used for the same knee throughout the whole study period. If the subject is illiterate, the questionnaire content will be explained by trained colleagues who are unrelated to the study.
Before the commencement of the trial, we will assess the subjects’ vital signs, blood pressure and conduct laboratory tests on complete blood count, renal and liver functions. Post-study blood test will be done on day 28 ± 4 days (week 4) after randomization as a mean for the subjects’ safety monitoring.
For safety concern, we will record medical history, adverse events during the treatment and follow-up period, and give appropriate treatment or referral if needed. Previous researches reported that DHJSD may cause gastrointestinal symptoms, including nausea and diarrhoea [20,21], however, serious adverse events were not found [22]. Treatment will be suspended immediately should treatment-related serious adverse events occur. Further assessment will be needed to decide whether the trial should be suspended. There will have a designated telephone hotline for adverse event reporting. Subjects can call the hotline during office hours but are advised to attend Emergency Department at the nearest hospital during non-office hours if severe adverse event is found.
Randomization and blinding
This study is designed as a randomized, wait-list controlled trial. Eligible subjects will be randomly allocated to one of the two groups: treatment group and wait-list control group. Random Allocation Software (version 1.0.0, Isfahan, Iran) will be used to generate a randomization scheme. An independent colleague who is not involved in the study will conduct the randomization process. The allocations will be concealed and sequentially numbered, and put in opaque, sealed envelopes. The information on the allocation list will remain strictly confidential.
Background of the practitioners
The study treatments will be performed by Registered Chinese Medicine Practitioners (RCMPs) in Hong Kong. The RCMPs can be both the assessors and Tui-na practitioners. The RCMPs will be responsible for consultation, assessment and prescription of study medication while the Tui-na practitioners will perform the Tui-na therapy alone. A CMP can be the assessor or Tui-na practitioner for different subjects; however, the role for each CMP will be fixed to avoid bias. For administering Tui-na therapy, responsible Tui-na CMP practitioners must have at least 2 years of clinical experience. The pre-trial training workshops on Tui-na therapy will be held to ensure standardization of Tui-na manipulation and procedures. Tui-na practitioners will be given a standardized script and instructed not to communicate with the subjects about the treatment effects.
Intervention:
Tui-na manipulation [23]
At the beginning, the subject will take a supine position. The trained Tui-na practitioner will apply rolling manipulation from the quadriceps femoris to the knee cap, and pressing, kneading both sides of knee cap for 5 minutes. Pressing and kneading Xuehai (SP10), Liangqiu (ST34), Heding (Ex-LE2), Dubi (ST35), Neixiyan (Ex-LE4) and Yanglingquan (GB34) for 1 minute each.
Subsequently, the subject will take a prone position. The Tui-na practitioner will apply rolling manipulation from the bottom of the thigh to the top of the calf for 5 minutes. Weizhong (BL40) and Chengshan (BL57) are pressed for 1 minute each.
Next, the patient takes a supine position, with the affected knee and hip flexed. The Tui-na practitioner supports the upper part of the knee to fix it with one hand and holds the heel with the other hand to rotate the knee joint clockwise, then counterclockwise for 5 times each.
The Tui-na practitioner will then hold the ankle and lift the treated extremity. The lower extremity should be raised to form a 30 degrees angle between the extremity and the bed. While pulling with slight force, shake constantly up and down in a small amplitude for 10 seconds.
Finally, the Tui-na practitioner will rub the sides of the knee joint, the edge of knee cap for 15 seconds. The names and locations of acupoints are listed in Table 2.
Study Medication
Subjects in the treatment group will be prescribed and dispensed with oral study medicine by the RCMPs. This study medication is Du-Huo-Ji-Sheng Decoction (DHJSD) [24] in concentrated Chinese medicine granule form. Each daily dose of DHJSD consists of Du-huo (AngelicaePubescentis Radix) 2g, Sang-ji-sheng (TaxilliHerba) 3g, Du-zhong (Eucommiae Cortex) 2g, Niu-xi (AchyranthisBidentatae Radix) 2.4g, Xi-xin (Asari Radix et Rhizoma) 0.2g, Qin-jiao (GentianaeMacrophyllae Radix) 2g, Fu-ling (Poria) 3g, Fang-feng (Saposhnikoviae Radix) 2g, Chuan-xiong (Chuanxiong Rhizoma) 1.2g, Dang-shen (Codonopsis Radix) 3g, Gan-cao (Glycyrrhizae Radix et Rhizoma) 1.2g, Bai-shao (Paeoniae Radix Alba) 2.4g, Di-huang (Rehmanniae Radix) 3g, Ji-xue-teng (Spatholobi Caulis) 2.4g [9] , Cu-yan-hu-suo (Corydalis Rhizoma) 0.6g [9] . The study medication will be taken twice daily for 4 consecutive weeks.
The study medication will be adjusted according to subjects’ clinical manifestation pattern based on Chinese medicine theory. If the subject manifests excessive dampness pattern, Fang-ji (StephaniaeTetrandrae Radix) 2g, Yi-yi-ren (Coicis Semen) 3g and Cang-zhu (AtractylodisRhizoma) 1.8g will be added [24]. If the participant manifests a blood stasis pattern, Tao-ren (Persicae Semen) 2g, Hong-hua (CarthamiFlos) 1.2g will be added instead [25]. Prescription of the core formula and the addition of herbs are listed in Table 3.
The granules used in this study will be manufactured under Good Manufacturing Practice (GMP) standard. Subjects will be explained clearly on how to administer and consume the study medicine. An instruction sheet (Appendix I) will be delivered to the subjects together with the pre-packed granule bags. This includes the storage and administering information of the medicine, as well as its common side-effects. Since the study medication will be prescribed and dispensed by RCMPs, it is not categorized as proprietary Chinese medicine, therefore the trial does not require Certificate for Clinical Trial and Medicinal Test.
Permitted and prohibited concomitant treatments
All Chinese herbal medicine or Chinese medicine therapies such as acupuncture & moxibustion other than study treatment will be prohibited.
Study termination
Subject’s participation would be terminated if he/she has:
1) developed severe adverse event;
2) hypersensitivity towards study treatment;
3) participated in another interventional research project;
4) life-threatening disease; or
5) decided to withdraw from the trial.
The whole research would be terminated under the following circumstances:
1) presence of serious adverse events related to the study medication; or
2) completion of all follow-up assessments.
Outcome measurements
Primary outcome measure
The primary outcome measure will be rated using the WOMAC in Cantonese version [15,16] (Appendix II) at 4 weeks after randomization. The WOMAC is a self-administered 3-dimensional questionnaire that assesses pain, stiffness and physical functional disability in subjects with KOA using a series of 24 questions. It is a 5-point scale from 0 to 4 (0 = none, 1 = mild, 2 = moderate, 3 = severe, 4 = extreme).
Secondary outcome measure
Secondary outcome measures include WOMAC in Cantonese version undertaken at 2 weeks and 8 weeks after randomization. The health-related quality of life using the EQ-5D-5L in Chinese version [17-19] (Appendix III) will also be used. Outcomes will be documented at 2 weeks, 4 weeks after randomization and follow-up (8 weeks after randomization). The patient is asked to indicate his/her health state by ticking the box in EQ-5D next to the most appropriate statement in each of the five dimensions. The EQ VAS records the patient’s self-rated health on a vertical visual analogue scale, where the endpoints are labelled ‘The best health you can imagine’ and ‘The worst health you can imagine’.
Known herb-drug interaction and adverse events
For the herb drug interaction, Du-huo (AngelicaePubescentis Radix) may pose moderate risk to subjects taking cytochrome P450 1A2 (CYP1A2) substrates. Dang-shen (Codonopsis Radix) and Bai-shao (Paeoniae Radix Alba) may pose moderate risk to subjects taking anticoagulant or antiplatelet drugs. Besides, Bai-shao may pose moderate risk to subjects taking clozapine and phenytoin. Gan-cao (Glycyrrhizae Radix et Rhizoma) may pose moderate risk to subjects taking antiarrhythmic drugs, antihypertensive drugs, diuretics, positive inotropic drugs, corticosteroids, hypnotics, anxiolytics, estrogen and testosterone. It is also suggested that Gan-cao may pose major risk when it is concurrently used with warfarin. Di-huang (Rehmanniae Radix) may pose moderate risk to subjects taking antiplatelet drugs [26]. For other herbs used in this study, no clinical trials or case reports of suspected herb drug interaction were identified. In addition, the DHJSD may induce mild gastrointestinal discomfort such as vomiting and diarrhea, while Tui-na may induce mild local pain. All these adverse events are known and will usually disappear in a short period of time.
Dropouts and withdrawals
All dropouts and attrition during the courses of the study will be monitored, and the respective reasons for withdrawal recorded.
Data management
This is a 10-week clinical trial, in which subjects must take treatment for 4 weeks (during 2nd - 6th weeks), attend four assessment visits, complete a set of questionnaires, and stop taking other medications to avoid interference of the trial. All collected information will be input into a designed database with password protection. Study documents will be kept for 7 years. We will explain the details of the study schedule, treatment, risk and benefits of the study, the responsibility of both assessors and the subjects during the consent process. In addition, before each visit, the delegated colleague will contact the subject to re-confirm the schedule. If a subject shows signs of wanting to withdraw, we would try to understand the underlying reasons and to explore the possibility to continue with the study.
Sample size calculation
The sample size calculation is based on the primary outcome i.e., the WOMAC. We assumed Tui-na combined with Chinese herbal medicine could have a 20-point superior than the wait-list control group at week 4. According to the previous study, the Tui-na could decrease WOMAC by 17.44, with the standard deviation of 23.61 [27]. The µsample size could be calculated according to the following formula
The µ1-µ2 is the difference in the means, which is 2.616. The σ was 23.61. We define α as 0.05 and β as 0.1, the tα and tβ are 1.96 and 1.282 respectively. The sample size for each group is 29. Considering 20% drop-out, the total sample size will be 70.
Statistical analysis
All efficacy and safety analyses will be conducted according to the intention-to-treat (ITT) principle. Missing values will be imputed by the last-observation-carried forward method. The statistical analysis will be performed using the Statistical Packages for the Social Sciences (SPSS) for Windows, version 22.0. Statistical significance is defined as a two-sided p value of < 0.05. Baseline characteristics will be reported as mean ± SD. Comparisons between groups will be conducted by using an analysis of covariance (ANCOVA) with baseline as a covariate. All items and subscales will be compared between groups for each 4-week period using ANCOVA, with treatment group as a factor in the model and baseline as the covariate. The changes in scores from baseline to the end-point of treatment will be tested using ANOVA. Within-group differences will be assessed using a paired t-test for normally distributed data and a Wilcoxon signed-rank test for non-normally distributed data.
Study monitoring
A dedicated team from the Hospital Authority Chinese Medicine Department (HACMD) that is completely independent in the running of the study and has no competing interests will be responsible for monitoring the study progress. Pre-trial and post-trial onsite inspections and quarterly monitoring meetings will be held to oversee the progress of the study and ensure it is conducted, recorded, and reported in accordance with the protocol, Good Clinical Practice (GCP) guidelines, and applicable regulatory requirements. Although a separate data monitoring committee will not be established, the HACMD will serve this function to ensure scientific validity, scientific integrity, and data accuracy through the regular monitoring of this clinical trial.
Ethical consideration and dissemination of information
The ethical validity of the study was approved by the Joint Chinese University of Hong Kong – New Territories East Cluster Clinical Research Ethics Review Committee (CREC Ref. No. 2019.538). Any modifications to the protocol are reported to this committee, and amendment approval should be obtained before any changes can take place. The written consent from individual subjects will be obtained voluntarily before the intervention. All patient data will be coded and anonymized when entered into the case report form. Only de-identified data will be collected and removed from the premises. We plan to publish the results of this study in peer-reviewed journals or academic conference proceedings.