Abstract
Objective
The aim of the study was to evaluate the effectiveness, safety, and cost associated with Wenxin keli in the treatment of cardiovascular diseases based on meta-analysis.
Methods
The terms “Wenxin keli” and “Wenxin” were used as the search terms in the PubMed, ProQuest, Springer, the Cochrane Library, CNKI (China National Knowledge Infrastructure), VIP (Chinese Scientific Journals Database), and Wan fang electronic databases (from January 2000 to October 2015). Relevant print journals and conference papers were also searched. Studies on randomized controlled trials (RCTs) of Wenxin keli used in the treatment of cardiovascular diseases were screened, and its indications were classified. Meta-analysis of these studies was conducted using the RevMan 5.2 software.
Results
A total of 49 RCTs (n=4,610) were included, 29 of which focused on arrhythmia, seven on angina, seven on heart failure, two on viral myocarditis, and four on menopausal syndrome. Analysis of the therapeutic indications of Wenxin keli showed that it was comparatively more curative and effective than other available treatments for cardiovascular diseases.
Conclusion
Wenxin keli showed better clinical efficacy in the treatment of arrhythmia, angina, and heart failure; however, more high-quality evidence is needed to support its use in the clinical setting.
Keywords: Wenxin keli, cardiovascular disease, meta-analysis, systematic review
Introduction
The number of patients affected by cardiovascular disease is steadily increasing because of socioeconomic development and modern lifestyles.1 A report from the World Health Organization reveals that chronic noncommunicable diseases have now become the leading cause of death worldwide. In 2008, 36 million individuals died of chronic noncommunicable diseases (63% of total deaths), of which 48% died of cardiovascular diseases.2 In recent years, there has been a shift in the medical paradigm, and cardiovascular and cerebrovascular diseases have now become a serious threat to public health.3 According to a report on Cardiovascular Diseases in China (2013), presented at the China Heart Congress, about one-fifth of all Chinese adults are currently affected with cardiovascular and cerebrovascular diseases.4 Furthermore, during the past five years, mortality due to cardiovascular diseases ranks first among all causes of death.4 Social and economic development has led to dramatic changes in lifestyles, including an increase in energy intake, less manual labor, accelerated pace of life, competitive pressures, and exposure to other risk factors associated with cardiovascular and other chronic noncommunicable diseases, which are causes for concern.5
Wenxin keli consists of several kinds of Chinese herbs including Huang Jing, Codonopsis, amber, Panax, and nard. Wenxin keli has been used clinically in the treatment of qi and yin deficiency, systolic blood stasis due to restless heart palpitations, shortness of breath, chest pain, premature ventricular contractions (PVC), and atrial premature beats. It is one of the main forms of treatment for cardiovascular disease in Chinese medicine. In recent years, many researchers have evaluated the use of Wenxin keli in the treatment of cardiovascular disease; however, further evaluation is necessary. Therefore, the present study aimed to conduct a comprehensive evaluation of the efficacy and safety of Wenxin keli, and provide the basis for its use as a medication for cardiovascular disease.
Materials and methods
Literature search
We performed systematic searches for randomized controlled trials (RCTs) designed to evaluate the clinical efficacy of Wenxin keli in CNKI (China National Knowledge Infrastructure), Wan fang, VIP (Chinese Scientific Journals Database), PubMed, the Cochrane Library, Springer, and ProQuest from January 1, 2000 to September 7, 2015 using “Wenxin keli” and “Wenxin” as the search terms.
Inclusion and exclusion criteria
Based on the Cochrane Collaboration Handbook standards, the following inclusion criteria were formulated for the selected literature: all published domestic and international RCTs on Wenxin keli; comparable baseline test data; interventions with individual drugs and Wenxin keli doses of 9 g, three times/day; any particular course of treatment; publications in Chinese and English. Diagnostic criteria used in the present study were based on authoritative Chinese and other countries diagnostic criteria. The exclusion criteria were as follows: duplicate publications, reports of combination therapy effects on treatment, descriptive studies, studies involving animal testing, conflicting before and after data (such as, the sum of the data not matching the total), and reports without statistical indicators.
Quality assessment
Study quality was evaluated with an improved version of the Jadad questionnaire, considering mainly four aspects: 1) random sequence generation (2 points); 2) randomized hiding (2 points); 3) blinding (2 points); 4) a withdrawal period (1 point). Two reviewers independently completed the assessment, and the mean score of the two reviewers was used as the final quality score of the selected studies. In the assessment of RCTs, 1–3 points were considered as low quality, and 4–7 points indicated high quality.
A unified data extraction sheet was derived, based on blinding characteristics in previously published medical literature, for use by the two reviewers. The information thereby extracted was then cross-checked. The extracted data included:
document specifications: first author, publication year, and title;
subjects: disease, diagnostic criteria, inclusion and exclusion criteria, sample size, etc;
interventions: medication, dosage, route of administration, duration of treatment, etc;
results: efficacy indicators.
Statistical analysis
The RevMan 5.2 software, provided by the Cochrane Collaboration, was used to conduct the meta-analysis. Count data were used to determine the odds ratio (OR) and 95% confidence interval (CI) for the efficacy analysis of effect size, whereas measurement data were used to determine the standardized mean difference. Heterogeneity of the included studies was expressed in terms of P and I2. If P>0.1 and I2<50%, the result of the test for heterogeneity was considered not statistically significant, and the fixed effects model was used for meta-analysis. For contrast, the random effects model was also applied to the data when P≤0.1 and I2≥50%.
Results
Retrieval results and quality assessment
We searched 2,970 potentially relevant articles in CNKI, 3,488 in Wan fang, 2,393 in VIP, and two each in PubMed, Springer, the Cochrane Library, and ProQuest. We retrieved 2,274 reports after reading the abstracts, and reports involving animal studies, pharmacological studies, and systems analyses were excluded. After screening the full texts of 663 documents that were selected following application of the inclusion and exclusion criteria, 29 studies on arrhythmia were included,6–34 of which nine were on PVC, seven on angina,35–41 seven on heart failure,42–48 two on viral disorders,49,50 and four on climacteric syndrome,51–54 as shown in Figure 1 and Table 1.
Figure 1.
Study selection steps.
Abbreviations: CNKI, China National Knowledge Infrastructure; VIP, Chinese Scientific Journals Database; WF, Wan fang.
Table 1.
Basic characteristics of included studies
| Study | Indications | Number of cases (test/control groups) | Treatment (days) | Interventions
|
Outcomes | Jadad score | |
|---|---|---|---|---|---|---|---|
| Drug test | Control drug | ||||||
| Gao6 | Arrhythmia | 48/48 | 28 | Wenxin keli | Propafenone | 1, 4 | 2 |
| Liu et al7 | Arrhythmia | 75/75 | 28 | Wenxin keli | Propafenone | 1 | 2 |
| Wang8 | Arrhythmia | 60/60 | 28 | Wenxin keli | Propafenone | 1, 4 | 2 |
| Cui9 | Arrhythmia | 60/60 | 28 | Wenxin keli | Propafenone | 1, 2 | 2 |
| Li et al10 | Arrhythmia | 48/35 | 28 | Wenxin keli | Propafenone | 1, 2, 3 | 1 |
| Xie11 | Arrhythmia | 34/32 | 28 | Wenxin keli | Propafenone | 1, 4 | 2 |
| Zou and Zhao12 | Arrhythmia | 102/101 | 28 | Wenxin keli | Propafenone | 1 | 2 |
| Wang13 | Arrhythmia | 75/75 | 28 | Wenxin keli | Propafenone | 1, 4 | 2 |
| Lou14 | Arrhythmia | 53/50 | 28 | Wenxin keli | Propafenone | 1 | 2 |
| Shi15 | Arrhythmia | 32/30 | 28 | Wenxin keli | Propafenone | 1, 4 | 2 |
| Wang16 | Arrhythmia | 58/64 | 28 | Wenxin keli | Propafenone | 2, 4 | 2 |
| Jin and Huang17 | Arrhythmia | 20/20 | 28 | Wenxin keli | Propafenone | 3 | 3 |
| Xue18 | Arrhythmia | 126/72 | 28 | Wenxin keli | Propafenone | 3 | 3 |
| Ren and Qiao19 | Arrhythmia | 43/21 | 28 | Wenxin keli | Propafenone | 3 | 3 |
| Wu and Yue20 | Arrhythmia | 48/33 | 28 | Wenxin keli | Propafenone | 3 | 2 |
| Li and Shen21 | Arrhythmia | 40/37 | 28 | Wenxin keli | Amiodarone | 1, 4 | 2 |
| Wang22 | Arrhythmia | 46/30 | 28 | Wenxin keli | Amiodarone | 1, 4 | 2 |
| Pang23 | Arrhythmia | 56/58 | 28 | Wenxin keli | Amiodarone | 1, 4 | 2 |
| Xu et al24 | Arrhythmia | 68/61 | 28 | Wenxin keli | Amiodarone | 1, 4 | 2 |
| Xia25 | Arrhythmia | 50/50 | 28 | Wenxin keli | Amiodarone | 1, 4 | 2 |
| Sun26 | PVC | 32/31 | 28 | Wenxin keli | Propafenone | 1, 2, 3 | 2 |
| Wu27 | PVC | 54/35 | 28 | Wenxin keli | Propafenone | 1, 2 | 2 |
| Wang28 | PVC | 60/30 | 28 | Wenxin keli | Propafenone | 1 | 2 |
| Guo29 | PVC | 53/53 | 28 | Wenxin keli | Propafenone | 1, 2, 3 | 2 |
| Jin30 | PVC | 60/30 | 28 | Wenxin keli | Propafenone | 1, 2, 3 | 2 |
| Zhang et al31 | PVC | 39/38 | 28 | Wenxin keli | Propafenone | 2, 3 | 2 |
| Li32 | PVC | 32/32 | 28 | Wenxin keli | Propafenone | 3 | 2 |
| Wang33 | PVC | 60/60 | 28 | Wenxin keli | Propafenone | 2, 3 | 2 |
| Yan34 | PVC | 60/60 | 28 | Wenxin keli | Propafenone | 2, 3 | 2 |
|
| |||||||
| Notes: 1, clinical efficacy; 2, ECG efficacy; 3, clinical symptoms of heart palpitations, shortness of breath, dizziness, insomnia, chest tightness, etc; 4, adverse reactions. | |||||||
|
| |||||||
| Yu et al35 | Angina | 40/35 | 28 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 2 | 2 |
| Shu and Li36 | Angina | 37/37 | 28 | Conventional treatment + Wenxin keli | Conventional treatment | 1 | 2 |
| Ye et al37 | Angina | 36/36 | 28 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 2 | 2 |
| Wei et al38 | Angina | 50/50 | 28 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 2 | 2 |
| Yuan39 | Unstable angina | 47/47 | 28 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 4 | 2 |
| Wei and Deng40 | Unstable angina | 50/50 | 28 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 3 | 2 |
| Yuan and Wei41 | Unstable angina | 80/80 | 28 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 3, 4 | 2 |
|
| |||||||
| Notes: 1, angina pectoris; 2, ECG efficacy; 3, changes in the indicator lipids; 4, adverse reactions. | |||||||
|
| |||||||
| Yu et al42 | Chronic heart failure | 37/35 | 56 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 2, 3 | 4 |
| Yang and Dong43 | Chronic heart failure | 40/40 | 56 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 3, 4 | 2 |
| Kong et al44 | Chronic heart failure | 30/30 | 56 | Conventional treatment + Wenxin keli | Conventional treatment | 2, 4, 6 | 2 |
| Xu45 | Chronic heart failure | 37/35 | 56 | Conventional treatment + Wenxin keli | Conventional treatment | 3 | 4 |
| Hu46 | Chronic heart failure | 50/48 | 56 | Conventional treatment + Wenxin keli | Conventional treatment | 4 | 2 |
| Yu47 | Congestive heart failure | 35/37 | 56 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 2, 3, 5 | 2 |
| Wang48 | Congestive heart failure | 35/35 | 56 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 2, 4, 6, 7 | 2 |
|
| |||||||
| Notes: 1, clinical efficacy; 2, TCM syndromes; 3, clinical echocardiography; 4, plasma BNP values; 5, heart rate; 6, 6-minute walking distance measurement; 7, adverse reactions. | |||||||
|
| |||||||
| Yang49 | Children with viral myocarditis | 34/34 | 14 | Conventional treatment + Wenxin keli | Conventional treatment | 1, 2 | 2 |
| Deng50 | Children with viral myocarditis | 30/28 | 14 | Conventional treatment + Wenxin keli | Conventional treatment | 1 | 2 |
|
| |||||||
| Notes: 1, clinical efficacy; 2, creatine kinase (CK-MB) change; 3, adverse reactions. | |||||||
|
| |||||||
| Liu and Ren51 | Climacteric syndrome | 60/58 | 84 | Conventional treatment + Wenxin keli | Conventional treatment + metoprolol | 1 | 2 |
| Lei52 | Climacteric syndrome | 42/38 | 84 | Conventional treatment + Wenxin keli | Conventional treatment + metoprolol | 1 | 2 |
| Li and Miao53 | Climacteric syndrome | 33/33 | 60 | Wenxin keli | Oryzanol + propranolol + vitamin B complex | 1 | 2 |
| Hu54 | Climacteric syndrome | 25/23 | 60 | Wenxin keli | Oryzanol + propranolol + vitamin B complex | 1 | 2 |
Notes: 1, clinical efficacy; 2, adverse reactions.
Abbreviations: BNP, brain natriuretic peptide; CK-MB, creatine kinase MB isoenzyme; ECG, electrocardiogram; PVC, premature ventricular contractions; TCM, traditional Chinese medicine.
The quality assessment of the studies was performed by two independent reviewers. Of the 49 studies included (Figure 1 and Table 1), only two studies were found to be of high quality (4 points).6–54 The results of specific assessment are presented in Table 1.
Results of meta-analysis
Meta-analysis of Wenxin keli in the treatment of arrhythmia
Clinical efficacy
There were 29 reports on the use of Wenxin keli in the treatment of arrhythmia, including nine on PVC. The results showed that Wenxin keli exhibited better clinical efficacy in the treatment of arrhythmia (OR =1.74, 95% CI [1.28, 2.35], P=0.0003; Figure 2) compared to propafenone. Also, in comparison to amiodarone, Wenxin keli again exhibited better clinical efficacy in the treatment of arrhythmia (OR =2.28, 95% CI [1.33, 3.89], P=0.003; Figure 3).
Figure 2.
Meta-analysis of Wenxin keli and propafenone in the treatment of arrhythmia.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Figure 3.
Meta-analysis of Wenxin keli and amiodarone in the treatment of arrhythmia.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Five studies considered the use of Wenxin keli in the treatment of PVC. The meta-analysis showed that it exhibited better clinical efficacy than propafenone (OR =2.92, 95% CI [1.72, 4.96], P<0.0001; Figure 4).
Figure 4.
Meta-analysis of Wenxin keli and propafenone in the treatment of PVC.
Abbreviations: CI, confidence interval; PVC, premature ventricular contractions; M–H, Mantel–Haenszel.
Efficacy of Wenxin keli on electrocardiogram
Three studies reported on the efficacy of Wenxin keli on electrocardiogram (ECG). Meta-analysis of the random effects model showed no significant difference between Wenxin keli and propafenone in the treatment of arrhythmia based on the ECG (OR =2.15, 95% CI [0.58, 7.97], P=0.25; Figure 5).
Figure 5.
Meta-analysis of Wenxin keli and propafenone in the treatment of arrhythmia.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Eight studies reported on the use of Wenxin keli in the treatment of PVC. The meta-analysis showed that Wenxin keli showed better efficacy than propafenone based on the ECG (OR =2.19, 95% CI [1.45, 3.30], P=0.0002; Figure 6).
Figure 6.
Meta-analysis of Wenxin keli and propafenone in the treatment of PVC.
Abbreviations: CI, confidence interval; PVC, premature ventricular contractions; M–H, Mantel–Haenszel.
Secondary outcomes
Five studies reported on the effect of Wenxin keli treatment on secondary efficacy variables in PVC. Heterogeneity was minimal; thus, the fixed effects model was applied to the study that reported on secondary efficacy variables, in addition to dizziness. The results showed that Wenxin keli exhibited better efficacy, in addition to dizziness (Table 2).
Table 2.
Meta-analysis of secondary efficacy variables in treatment of arrhythmia
| Outcomes | Number of included studies | Number of cases | Heterogeneity
|
Model | Meta-analysis
|
||
|---|---|---|---|---|---|---|---|
| I2 | P-value | OR (95% CI) | P-value | ||||
| Palpitations | 4 | 383 | 0% | 0.99 | Fixed | 3.29 (1.64, 6.61) | 0.0008 |
| Chest tightness | 5 | 451 | 0% | 0.70 | Fixed | 3.61 (2.22, 5.87) | <0.00001 |
| Restless sleep | 4 | 373 | 0% | 0.50 | Fixed | 2.49 (1.40, 4.43) | 0.002 |
| Dizziness | 4 | 379 | 55% | 0.09 | Random | 2.53 (0.87, 7.35) | 0.09 |
| Shortness of breath | 5 | 462 | 0% | 0.94 | Fixed | 3.00 (1.74, 5.19) | <0.0001 |
Abbreviations: CI, confidence interval; OR, odds ratio.
Adverse reactions
A total of eleven studies reported adverse reactions in the treatment of arrhythmia. Wenxin keli showed a lower incidence of adverse reactions, with reports of mild adverse reactions and favorable clinical application and safety, in comparison to both propafenone and amiodarone (Figures 7 and 8).
Figure 7.
Meta-analysis of Wenxin keli, propafenone, and associated adverse reactions on arrhythmia.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Figure 8.
Meta-analysis of Wenxin keli, amiodarone, and associated adverse reactions on arrhythmia.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Six studies reported on adverse reactions in the treatment of PVC. Meta-analysis of the fixed effects model showed that Wenxin keli exhibited a lower incidence of adverse reactions (OR =0.32, 95% CI [0.16, 0.64], P=0.001; Figure 9) compared to amiodarone.
Figure 9.
Meta-analysis of Wenxin keli, propafenone, and associated adverse reactions on PVC.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Publication bias
A funnel plot (Figure 10) showed that the studies reporting the use of Wenxin keli in the treatment of arrhythmia, included in the analysis, were substantially symmetric. This suggests less publication bias in these reports. According to the Cochrane Handbook, funnel plot analysis should not be performed for other indications if there are less than ten studies.
Figure 10.
Funnel plot of Wenxin keli and propafenone in the treatment of arrhythmia.
Abbreviations: SE, standard error of the mean; OR, odds ratio.
Meta-analysis of Wenxin keli in the treatment of angina
Angina pectoris
Six reports, included in the analysis, reported on the use of Wenxin keli in the treatment of angina pectoris, of which three specifically focused on angina and three on unstable angina. Meta-analysis of the fixed effects model showed that the clinical efficacy of Wenxin keli combined with conventional therapy in the treatment of angina was significantly better than conventional therapy alone (OR =3.12, 95% CI [1.77, 5.52], P<0.0001; Figure 11). The clinical efficacy of Wenxin keli combined with conventional therapy in the treatment of unstable angina was also significantly better than conventional therapy alone (OR =3.97, 95% CI [1.92, 8.22], P=0.0002; Figure 12).
Figure 11.
Meta-analysis of Wenxin keli and propafenone in the treatment of angina.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Figure 12.
Meta-analysis of Wenxin keli and propafenone in the treatment of unstable angina.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
ECG efficacy
Two studies reported on the efficacy of Wenxin keli in the treatment of angina based on the ECG. Meta-analysis of the fixed effects model showed that the efficacy of Wenxin keli combined with conventional therapy was not significantly different from that of the conventional therapy alone (OR =2.02, 95% CI [0.65, 6.24], P=0.22; Figure 13).
Figure 13.
Meta-analysis of Wenxin keli combined with conventional therapy in the treatment of angina.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Adverse reactions
Three studies mentioned the development of adverse reactions to Wenxin keli in the treatment of angina, two of which could not be compared because the experimental and control groups were not described separately. The latter test group and six cases (15%) in the control group exhibited no adverse reactions.
Meta-analysis of Wenxin keli in the treatment of heart failure
Clinical efficacy
Two studies reported on the clinical efficacy of Wenxin keli in the treatment of chronic heart failure. Meta-analysis showed that Wenxin keli combined with conventional treatment showed no greater clinical efficacy (OR =2.62, 95% CI [0.91, 7.56], P=0.07; Figure 14) compared to the conventional treatment group.
Figure 14.
Meta-analysis of Wenxin keli combined with conventional treatment for chronic heart failure.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Secondary efficacy variables
Analysis of secondary efficacy end points showed that Wenxin keli combined with conventional treatment showed better efficacy in left ventricular ejection fraction (LVEF) values, plasma brain natriuretic peptide (BNP) levels, and stroke volume (Table 3).
Table 3.
Meta-analysis of secondary efficacy variables in treatment of heart failure
| Outcomes | Number of included studies | Number of cases | Heterogeneity
|
Model | Meta-analysis
|
||
|---|---|---|---|---|---|---|---|
| I2 | P-value | MD (95% CI) | P-value | ||||
| LVEF values | 4 | 310 | 57% | 0.08 | Random | 0.76 (0.41, 1.12) | <0.0001 |
| Plasma BNP levels | 3 | 238 | 99% | <0.00001 | Random | −5.92 (−9.70, −2.14) | 0.002 |
| Stroke volume | 3 | 212 | 29% | 0.24 | Fixed | 0.50 (0.18, 0.83) | 0.002 |
Abbreviations: BNP, brain natriuretic peptide; CI, confidence interval; LVEF, left ventricular ejection fraction; MD, mean difference.
Meta-analysis of Wenxin keli in the treatment of viral infections
Clinical efficacy
Two studies reported on the clinical efficacy of Wenxin keli in the treatment of viral infections. Meta-analysis showed that Wenxin keli combined with conventional treatment exhibited better clinical efficacy (OR =4.89, 95% CI [1.30, 18.38], P=0.02; Figure 15) compared to conventional treatment.
Figure 15.
Meta-analysis of Wenxin keli combined with conventional treatment for viral infections.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Adverse reactions
Two studies investigated adverse reactions associated with Wenxin keli in the treatment of viral infections. No adverse reactions were reported in either study, suggesting the safety of Wenxin keli.
Meta-analysis of Wenxin keli in the treatment of climacteric syndrome
Clinical efficacy
Four studies reported on the clinical efficacy of Wenxin keli in the treatment of climacteric syndrome, of which two compared Wenxin keli combined with conventional therapy to conventional therapy alone, and the other two compared Wenxin keli to a combination of oryzanol, propranolol, and vitamin B complex. Meta-analysis showed that in comparison to conventional treatment alone, Wenxin keli combined with conventional treatment exhibited better clinical efficacy in the treatment of climacteric syndrome (OR =3.67, 95% CI 1.88, 7.18, P=0.0001; Figure 16). In comparison to the control drug (propranolol + oryzanol + vitamin B), Wenxin keli showed better clinical efficacy (OR =7.82, 95% CI [2.92, 20.95], P<0.0001; Figure 17).
Figure 16.
Meta-analysis of Wenxin keli combined with conventional treatment for climacteric syndrome.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Figure 17.
Meta-analysis of Wenxin keli in the treatment of climacteric syndrome.
Abbreviations: CI, confidence interval; M–H, Mantel–Haenszel.
Adverse reactions
No adverse reactions were reported in the literature regarding the use of Wenxin keli in the treatment of climacteric syndrome. Thus, comparisons between any control and corresponding experimental groups were not possible.
Discussion
Wenxin keli consists primarily of Codonopsis, Huang Jing, Panax, amber, nard, and other traditional Chinese herbs. It represents the first broad-spectrum treatment capable of affecting multiple ion channels (Na+, K+, and Ca2+) that can also significantly improve heart function (without causing arrhythmias), heart palpitations, chest tightness, and other associated symptoms. Modern pharmacological studies have confirmed that Codonopsis contains inulin and amino acids, and that it exerts anti-platelet aggregation, enhances immunity, and improves myocardial contractile effects.55 Huang Jing exhibits lipid-lowering and anti-atherosclerotic effect, reduces blood pressure, and increases coronary blood flow.56 Panax can increase coronary blood flow, inhibit self-discipline of the ectopic pacemaker sinus node, reduce myocardial oxygen consumption, improve microcirculation, and regulate myocardial ischemia and hypoxia.56 Nard plays a role in relieving depression, and pharmacological experiments show that it contains valerian ketones. These compounds can combine with specific proteins via ion channels in the myocardial cell membrane to reduce myocardial cell automaticity, extend the atrial action potential of ventricular muscle and conduction system time, interrupt reentry, and eliminate arrhythmias.57 The therapeutic index of Wenxin keli on the heart, kidneys, and liver was within normal limits. Wenxin keli can enhance immune function, without causing significant adverse reactions, and shows no evidence of the side effects of myocardial ischemia and arrhythmia. It is therefore considered to be safe and effective.3
Limitations
Among the studies included in the meta-analysis, only two of them that had higher scores on the Jadad questionnaire were used to evaluate the quality, thereby potentially affecting the strength of the results. There were fewer documents available for some of the indications analyzed, and some studies had smaller sample sizes. Both of these factors represent limitations of the present study. No standards for RCTs have been published in People’s Republic of China; therefore, allocation concealment and blinding were rarely mentioned in the studies included in the analysis. Thus, it is possible that most of the original reports were inconclusive and the results were of low quality, thereby increasing bias. To address the aforementioned limitations and verify the results of the present study, additional high-quality RCT studies that employ larger sample sizes are required.
Conclusion
Based on the available evidence, meta-analysis is an effective method to prove the safety and efficacy of a particular treatment. The results of meta-analysis allow physicians and patients to choose the most effective treatment.
For systematic reviews of Wenxin keli in the treatment of cardiovascular disease, we used the indicators of angina pectoris total efficiency, ECG total efficiency, and adverse outcomes for comparison with the control groups that were treated with propafenone and amiodarone. The findings observed in the treatment of arrhythmia, PVC, angina pectoris, heart failure, viral myocarditis, and climacteric syndrome, among others, were derived from 49 studies. Overall, these studies reported favorable effects of Wenxin keli, regardless of whether it was used directly or as an adjuvant therapy. Furthermore, a low incidence of adverse reactions was evident among the studies analyzed.
Footnotes
Disclosure
The authors report no conflicts of interest in this work.
References
- 1.Go AS, Mozaffarian D, Roger VL, et al. Heart disease and stroke statistics – 2014 update: a report from the American Heart Association. Circulation. 2014;129(3):399–410. doi: 10.1161/01.cir.0000442015.53336.12. [DOI] [PubMed] [Google Scholar]
- 2.World Health Organization . Global Status Report on Noncommunicable Diseases 2010. Geneva: WHO; 2011. [Google Scholar]
- 3.Wang J, Shui LM. 1991–2003 Ningbo City Jiangdong district residents cardiovascular disease mortality dynamic analysis. Chin J Prevent Control Chronic Dis. 2005;13(5):251–252. [Google Scholar]
- 4.Hu XL, Zhou JM, Chen XP. Role of AGXT2 in ADMA metabolism and the development of cardiovascular and cerebrovascular diseases. Chin Pharmacol Bull. 2015;05:601–605. [Google Scholar]
- 5.Li YH, Zhou JM, Yang C, et al. Study on cardiovaseular and cerebrovaseular diseases and its influencing factors among 5 kinds of occupational populations in 6 provinces in China. Chin J Health Education. 2012;01:3–7. [Google Scholar]
- 6.Gao P. Clinical analysis of 52 cases buchang Wenxin keli in treatment of arrhythmia. Chin Comm Doc. 2010;13:144. [Google Scholar]
- 7.Liu JF, Cao PL, Ge YZ, et al. Curative effect analysis of Wenxin keli in treatment of cardiac arrhythmia. Acta Acad Med Jiangxi. 2009;09:52–54. [Google Scholar]
- 8.Wang YM. Clinical study of Wenxin keli in treatment of cardiac arrhythmia. Chin Prac Med. 2007;23:3–5. [Google Scholar]
- 9.Cui YX. Clinical analysis of buchang Wenxin keli in treatment of arrhythmia. Chin Prac Med. 2010;26:165–166. [Google Scholar]
- 10.Li YB, Sun CY, et al. Clinical observation of 48 cases on Wenxin keli in treatment of arrhythmia. Chin Comm Doc. 2006;22(09):43. [Google Scholar]
- 11.Xie HQ. Clinical analysis of 34 cases on Wenxin keli in treatment of arrhythmia. J Kunming Med Coll. 2009;(3B):386–387. [Google Scholar]
- 12.Zou GX, Zhao BC. 102 cases of Wenxin keli in treatment of arrhythmia. J Tradit Chin Med. 2002;09:689–690. [Google Scholar]
- 13.Wang CY. 150 cases of Wenxin keli in treatment of arrhythmia. Clin J Rational Drug Use. 2012;28:65–66. [Google Scholar]
- 14.Lou MP. 53 cases of Wenxin keli in treatment of arrhythmia. Modern Medicine. 2008;17:2627–2628. [Google Scholar]
- 15.Shi H. The efficacy of Wenxin keli in treatment of arrhythmia. Chemists (Academic Edition) 2012;10(12):174–175. [Google Scholar]
- 16.Wang MS. Clinical observation on treatment of 58 cases with cardiac arrhythmia by buchang wenxin granule. Henan Coll of Sci and Tech (Med Science) 2009;02:119–120. [Google Scholar]
- 17.Jin HX, Huang T. 20 cases of clinical observation on Wenxin keli treating arrhythmia. Chin Comm Doc. 2007;(15):94. [Google Scholar]
- 18.Xue JZ. 126 cases of clinical observation on Wenxin keli treating arrhythmia. Chin J Integr Med Cardio. 2008;3(Suppl):103–104. [Google Scholar]
- 19.Ren YH, Qiao HF. 46 cases of clinical observation on Wenxin keli treating arrhythmia. Chin J Integr Med Cardio. 2005;3(3):256–257. [Google Scholar]
- 20.Wu XW, Yue L. 48 cases of clinical observation on Wenxin keli treating arrhythmia. Chin J Integr Med Cardio. 2004;2(8):487–488. [Google Scholar]
- 21.Li ZY, Shen JX. 40 cases of clinical observation on Wenxin keli treating arrhythmia. Zhejiang J Tradit Chin Med. 2011;09:698. [Google Scholar]
- 22.Wang DQ. 40 cases of clinical observation on buchang Wenxin keli treating arrhythmia. J Tradit Chin Med. 2010;51(7):624. [Google Scholar]
- 23.Pang YL. 56 cases of clinical observation on buchang Wenxin keli treating arrhythmia. Yunnan J Tradit Chin Med Mater Medica. 2010;31(12):33. [Google Scholar]
- 24.Xu ZM, He YP, et al. 68 cases of clinical observation on buchang Wenxin keli treating arrhythmia. J Chin Physician. 2006;(Suppl):562–563. [Google Scholar]
- 25.Xia DM. Clinical efficacy obseravation on buchang Wenxin particles treating arrhythmias. Modern Diagn Treat. 2010;21(6):344–345. [Google Scholar]
- 26.Sun XJ. 68 cases of clinical observation on buchang Wenxin keli treating ventricular contraction. Liaoning J Tradit Chin Med. 2009;09:1530–1531. [Google Scholar]
- 27.Wu Y. Clinical observation on Wenxin keli improving premature patient’s symptoms and ECG. Chin J Exp Med Formul. 2009;8(15):92–93. [Google Scholar]
- 28.Wang HQ. Clinical observation on the safety and efficacy of Wenxin keli treating ventricular contraction. Clin Focus. 2009;12:1082–1083. [Google Scholar]
- 29.Guo YH. 112 cases of clinical observation on buchang Wenxin keli treating premature ventricular contractions. Med Inf. 2013;1(26):163. [Google Scholar]
- 30.Jin RS. Clinical observation on buchang Wenxin keli treating ventricular contractions. Chin Prac Med. 2011;17(6):164–165. [Google Scholar]
- 31.Zhang B, Liu F, Duan XX. Clinical observation on buchang Wenxin keli treating premature ventricular contractions. Chin J Mod Drug Appl. 2010;01:103–104. [Google Scholar]
- 32.Li ZM. 64 cases of clinical observation on buchang Wenxin keli treating premature ventricular contractions. Chin Hth Nutrition. 2012;12:243–244. [Google Scholar]
- 33.Wang YJ. 60 cases of clinical observation on buchang Wenxin keli treating premature ventricular contractions. Chin Prac Med. 2011;16:158–159. [Google Scholar]
- 34.Yan GF. Clinical observation on treatment of 60 cases of premature ventricular vontraction with Wenxin granules. Guid J Tradit Chin Med Pharm. 2007;13(4):24–25. [Google Scholar]
- 35.Yu YH, Li BH, et al. Clinical observation on buchang Wenxin keli treating angina. Xinjiang J Tradit Chin Med Pharm. 2004;04:14–15. [Google Scholar]
- 36.Shu B, Li Y. Wenxin granules for treating 37 cases of angina pectoris of coronary atherosclerosis heart disease. Chin Pharm. 2013;22(16):102–103. [Google Scholar]
- 37.Ye GF, Shi YF, et al. Clinical study of Wenxin granule on coronary heart disease with angina pectoris. Jilin Med J. 2008;29(5):362–363. [Google Scholar]
- 38.Wei YQ, Zhang XW, et al. Clinical study of Wenxin keli treating unstable angina. Pract J Cardiac Cereb Pneum Vasc Dis. 2010;03:370–371. [Google Scholar]
- 39.Yuan KY. Clinical analysis of Wenxin keli treating unstable angina. Chin Prac Med. 2011;22:141–142. [Google Scholar]
- 40.Wei YQ, Deng GY. Clinical study of Wenxin keli treating angina. Liaoning J Tradit Chin Med. 2010;08:1516. [Google Scholar]
- 41.Yuan JQ, Wei YY. Clinical study of Wenxin keli treating unstable angina. Clin Med. 2005;03:43–44. [Google Scholar]
- 42.Yu T, Li DH, et al. 37 cases of clinical observation on Wenxin keli treating chronic heart failure. Jilin J Tradit Chin Med. 2006;11:9–10. [Google Scholar]
- 43.Yang F, Dong ZH. Effect of Wenxin keli on chronic heart failure, plasma brain natriuretic peptide and cardiac function in patients. Zhejiang J Tradit Chin Med. 2009;01:72. [Google Scholar]
- 44.Kong YH, Deng CJ, Cheng W, et al. Effect of Wenxin keli on cardiac function and plasma brain natrium peptide in patients with chronic heart failure. J Clin Cardiol. 2009;25(6):428–430. [Google Scholar]
- 45.Xu KH. Clinical observation on Wenxin keli treating chronic heart failure. Health for Everybody (Medical Guide) 2008;04:128. [Google Scholar]
- 46.Hu JH. Effect of Wenxin granuleon chronic heart failure. Chin Tradit Patent Med. 2010;32(12):2035–2037. [Google Scholar]
- 47.Yu XF. 37 cases of clinical observation on Wenxin keli treating heart failure. Chin Prac Med. 2008;05:95–96. [Google Scholar]
- 48.Wang H. Clinical observation on Wenxin keli treating chronic congestive heart failure. Liaoning J Tradit Chin Med. 2012;11:2229–2230. [Google Scholar]
- 49.Yang LL. Clinical observation of Wenxin granule in the treatment of children with viral myocarditis. Modern Diagn Treat. 2014;20:4634–4635. [Google Scholar]
- 50.Deng XC. Clinical analysis of Wenxin keli in treatment of children with viral myocarditis by assisting. Yunnan J Tradit Chin Med Mater Medica. 2012;07:86. [Google Scholar]
- 51.Liu PX, Ren FX. 118 cases of clinical observation on Wenxin keli treating palpitations in patients with climacteric syndrome. China Med. 2008;8(3):493–494. [Google Scholar]
- 52.Lei DF. 42 cases of clinical observation on Wenxin keli treating palpitations in patients with climacteric syndrome. Shaanxi J Tradit Chin Med. 2009;07:791–792. [Google Scholar]
- 53.Li L, Miao F. Clinical observation on Wenxin keli treating climacteric syndrome. J Changzhi Med Coll. 2010;05:343–344. [Google Scholar]
- 54.Hu XP. 35 cases of clinical observation on Wenxin keli treating climacteric syndrome. Clin Res. 2013;2:161. [Google Scholar]
- 55.Qi P. 32 cases of clinical observation on Wenxin keli treating arrhythmia. Yunnan J Tradit Chin Med Mater Medica. 2010;08:49. [Google Scholar]
- 56.Liu CL, Dong ZS. 32 cases of clinical observation on Wenxin keli treating tachyarrhythmias. Chin J Integr Med Cardio. 2005;3(1):68–69. [Google Scholar]
- 57.Ye F. 63 cases of clinical observation on Wenxin keli treating arrhythmia. The Chin and Forgn Hth Abs. 2013;10(10):204. [Google Scholar]