Study design
This is a stratified randomized (random assignment), double-blind, single-dummy, parallel control of placebo, multicenter superiority test clinical study. The study will be conducted at the first Affiliated Hospital of Tianjin University of Traditional Chinese Medicine; Oriental Hospital of Beijing University of Chinese Medicine; the first Affiliated Hospital of Henan University of Traditional Chinese Medicine; the first Affiliated Hospital of Hunan University of Traditional Chinese Medicine; Affiliated Hospital of Shandong University of Traditional Chinese Medicine; Shanghai Hospital of Traditional Chinese Medicine; and Tianjin Children's Hospital. Ethical clearance for the trial was obtained from the respective ethics committees of the seven hospitals. Children with community-acquired pneumonia will undergo a standardized baseline evaluation before treatment, comprising detailed history taking, physical examination, and laboratory testing. All included patients are randomly divided into two groups: an experimental group and control group. The experimental group receives Anerning Granules plus ceftriaxone sodium; the control group receives AEN placebo plus ceftriaxone sodium. Each group will be treated for ten days, and a stage effect evaluation will be conducted on the sixth day.The trial is conducted in accordance with the World Medical Association Declaration of Helsinki and Good Clinical Practice of Pharmaceutical Products. 8 9 10 After a full explanation from the clinicians, written informed consent will be obtained from the participants before intervention.11 12 Strict data management and quality control will be conducted in this trial. 13 14 The study design is shown in Figure 1. The protocol follows the recommendations of the SPIRIT initiative (see additional file 1), 15 and the trial results will be reported according to the latest version of the CONSORT statement. 16
Patient and public involvement
Patients were not involved in the research question, design, conduct, outcome measures, or data analysis of the study. Only medically trained clinicians carried out patient recruitment and management in the study. The clinicians will describe the purpose, burden of the intervention, procedure, and potential risks of this trial to the participants themselves or their designated representatives before recruitment. We will disseminate the results of this study to participants through patient organizations and open lectures.
Participants and recruitment
Diagnostic criteria of Western medicine and traditional Chinese medicine
The Western medicine diagnostic criteria of community-acquired pneumonia in children will refer to the Guidelines for the Management of Children's Community-Acquired Pneumonia (2013 Revision)17 and will be formulated with reference to the 8th edition of "Zhufutang Practical Pediatrics".18 The traditional Chinese medicine (TCM) diagnostic criteria of community-acquired pneumonia in children will refer to the Guidelines for the Diagnosis and Treatment of Common Pediatric Diseases of the Chinese Medicine Society of China (2012) 19 and the "Twelfth Five-Year Plan" textbook "Pediatrics of Traditional Chinese Medicine".
Inclusion criteria
Inclusion criteria are as follows: (i) age > 1 and < 5 years; (ii) meet the Western diagnostic criterion of community-acquired pneumonia in children that the disease duration does not exceed 48 hours and consider bacterial infections; (iii) the syndrome differentiation of TCM is wind-heat closed lung and phlegm-heat closed lung; (iv) sign the written informed consent form for the clinical trial.
Exclusion criteria
Exclusion criteria are as follows: (i) chest X-ray film showed obvious lung tumors and tuberculosis; (ii) people with acute infectious diseases such as measles, whooping cough, or influenza; (iii) acute upper respiratory tract infection, wheezing bronchitis, bronchial asthma, bronchial foreign bodies or other respiratory diseases; (iv) children with severe malnutrition and immunodeficiency; (v) in combination with severe cardiopulmonary disease, liver and kidney disease, advanced tumors, and other serious or progressive diseases; (vi) those who meet the diagnostic criteria for CAP (severe) Western medicine for children; (vii) patients with clinical diagnosis or clinical consideration of viral pneumonia and mycoplasma pneumoniae pneumonia; (viii) people with an allergic constitution or allergy to penicillin, cephalosporin antibiotics, Anerning Granules and their components; (ix) researchers think it is inappropriate to join the group.
Exit criteria
Patients will leave the trial when one of the following criteria is met: (i) incorrectly included; (ii) are poorly compliant; (iii) no medication or any follow-up records; (iv) occurrence of allergic reactions or serious adverse events (AE); (v) participants have other complications or special physiological changes during the trial; (vi) patients have been treated with other medicines during the trial; (vii) not alleviated or the symptoms are aggravated; (viii) poor patient dependence; and (ix) breaking blind cases for various reasons. Participants may withdraw from the study at any time for any reason.
Interventions
All researchers are clinical doctors and receive standardized training in diagnostic interviewing before the start of the trial. The 216 qualified subjects are divided into an experimental group of 144 cases and a control group of 72 cases. The experimental group was given oral Anerning Granules: 1 to 5 years old, 1 bag / time, 3 times / day; the control group was given oral Anerning Granules placebo: 1 to 5 years old, 1 bag / time, 3 times / day. Both groups were treated with intravenous ceftriaxone sodium (50mg / kg / time, 1 time / day, the total amount does not exceed 2 grams per day), and the experimental drug and its simulation agent are consistent in appearance, smell, and taste. The Anerning Granule Simulator is composed of sucrose, caramel color, lemon yellow, and bitter gourd extract. The drugs are provided by Jinxian Tibetan Medicine Co., Ltd. Ceftriaxone sodium is arranged by each clinical unit and is not provided uniformly. If clinical recovery is reached during this period, the treatment will be terminated.
Criteria for clinical cure and withdrawal
After treatment, the body temperature is normal, the signs of cough, sputum, and lungs basically disappear, and the symptoms and signs score and improvement are ≥90%; the body temperature (axillary temperature) is less than 37.3°C, and is maintained for 24 hours or more. Regarded as clinically cured, although the treatment period is less than 10 days, the drug can be discontinued. For details, please refer to the quantification standard table of TCM syndromes and signs on the CRF form (see additional file 2).
Drug allocation
The participant patients were randomly divided into 2 groups according to the 2:1 ratio. The divided test drugs are sent to each test center according to the random layered center number. Observation doctors should issue medicines according to the order of each patient's visit and the medicine number, and no medicines should be selected. The drug number remains unchanged throughout the trial. The distribution of medicines is conducted by nurses who have been professionally trained in standard operating procedure, one box at a time, containing 9 sachets (a 3-day dose). After the test, the drug administrator is responsible for the centralized destruction of the remaining drugs, according to procedures. If a blind bottom leak caused by any unspecified situation occurs and affects the objectivity of the test result, the test will be considered invalid. In the event of an emergency (such as a serious adverse event), or when the patient needs to be rescued and must know what treatment they received, the main investigator decides whether to unblind the blindness urgently according to the condition. Cases withdrawn due to efficacy reasons must not be broken. Once the blinding is urgently released, the numbered subjects will withdraw from the trial, and the investigator should record the reason for withdrawal on the case report form.
Test medication compliance
In clinical trials, the compliance of the subjects is mainly compliance with the test medication so that the subjects fully understand the importance of taking the medication on time and in quantity and avoiding adding other drugs or treatments. This test mainly uses the drug counting method, combined with the inquiry method when necessary, to judge the compliance of the test drug. Test medication compliance = (the amount of test drug taken / the amount of test drug that should be taken) × 100%.
Test process
Before conducting any experimental procedure, the subject and / or its agent must have read and signed the informed consent form approved by the ethics committee. The test procedure shall be carried out within the specified visit time window.The test process is shown in Table 1.
- Observation period: 10 days.
- Visiting points: observe every day.
- Safety follow-up: the patients were followed up to normal or pre-treatment levels.
Table 1:Overview of the test process
Phase
Project
|
The baseline period
|
Therapeutic observation period
|
follow-up(security)
|
-1~0day
|
Intermediate viewing point(Day 2 ~ day 9)
|
End point (day 10)
|
Sign the informed consent form
|
√
|
|
|
|
Cases to be included in the
|
√
|
|
|
|
Demographic data
|
√
|
|
|
|
Medical history
|
√
|
|
|
|
Always use
|
√
|
|
|
|
randomized
|
√
|
|
|
|
Distribution of experimental drugs
|
√
|
|
|
|
Distribute the subject diary card
|
√
|
|
|
|
Vital signs
|
√
|
√
|
√
|
|
The doctor of traditional Chinese medicine syndrome
|
√
|
√
|
√
|
|
Lung signs
|
√
|
√
|
√
|
|
Physical check
|
√
|
√
|
√
|
√*
|
X-ray chest radiograph
|
√
|
|
√
|
|
Blood, CRP, urine routine,stool routine
|
√
|
|
√
|
√*
|
Liver and kidney function
|
√
|
|
√
|
√*
|
Mycoplasma pneumoniae IgM
|
√
|
|
|
|
Electrocardiogram (ecg)
|
√
|
|
√
|
√*
|
Antibiotic use record
|
|
√
|
√
|
√*
|
Drug combination
|
|
√
|
√
|
√*
|
Adverse events
|
|
√
|
√
|
√*
|
Recall drug and subject log card
|
|
|
√
|
|
Note: * is the test when necessary.
Outcome measures
Primary outcome measure
Antibiotic frequency at the clinical endpoint (DDDs): evaluation at the end of the test.
Secondary outcome measures
- The total effective rate of the disease: 5 and 7 days after the treatment and the record of the end point of the test, and the evaluation will be completed after the test.
- Clinical recovery time: evaluation after the end of the trial, calculated in days.
- Time for complete fever remission, time for onset of fever, cough, sputum, and sore throat; severity-time AUC of fever, cough, sputum, and sore throat symptoms, observed once every 24 hours (1 day) after treatment.
- The curative effect of TCM syndromes 5 or 7 days after treatment and recorded at the end of the trial, the evaluation of the end of the trial.
- Single symptoms (fever, daytime cough, nighttime cough, sputum quality, sputum volume, etc.) and the curative effect of lung signs are observed daily after treatment, and the trial is concluded.
- Effectiveness of chest X-ray is inspected and evaluated at the baseline and the end of the test.
- Incidence of conversion to CAP (severe) is evaluated at the end of the test.
Safety assessments
Safety measurements included laboratory indices and AEs. All patients will undergo laboratory examination before enrollment and at the end of the clinical trial. Changes in laboratory indices before and after the clinical trial will be compared to conducting a safety analysis. Laboratory indices are: (i) routine blood and urine testing; (ii) liver function (AST, ALT, TBIL, DBIL, γ-GT, ALP) and kidney function (Scr, BUN); and (iii) ECG. The occurrence of any AEs in trial participants such as subjective discomfort of patients or abnormal laboratory results will be recorded in the CRF during the whole trial process. We will withdraw patients who have severe AEs, as it will be unsafe for them to continue the trial. Meanwhile, we will give them relevant medical care and follow up with them until the reaction has terminated.
Informed consent
Before enrolling patients in the trial, the investigating doctor will completely and comprehensively describe the purpose, procedure, and potential risks of this trial in writing to the patients themselves or their designated representatives. Patients will be informed that they have the right to withdraw from the trial at any time. Each patient must provide written informed consent before participating in this study; this consent will be kept in the study file.
Quality control
Quality assessment will be conducted in terms of the following aspects: the progress of the trial; the qualifications of the investigators; the mastery of the program; the authenticity, accuracy, and completeness of the CRF; archival preservation; program implementation; AEs; drug preservation and storage; written informed consent; participant compliance; and laboratory examination data. In particular, the authenticity and accuracy of the CRF, program implementation, and determination of AEs will be strictly examined.
Data management
The patients in this trial will be recruited. Therefore, the original data will include the CRF, patient log card, original laboratory examination, and written informed consent. The inspector will regularly visit all centers to conduct a data quality inspection. The authenticity and accuracy of the data will be checked by original laboratory comparison, telephone follow-up with patients, and examination of the integrity, timeliness, and normalization of the data. The paper form of the data will be collected after approval and inspection. The researcher who is responsible for data entry will build a database with double-recorded data entry by two people, and consistency testing will be carried out to ensure accuracy.
Statistical analysis
Statistical analyses will be performed by professional statisticians using SPSS 22.0. Three datasets will be conducted: intention-to-treat; per-protocol set; and safety dataset. The intention-to-treat refers to the patients who have been randomized; an intentional analysis will be conducted for curative effect. The per-protocol set refers to all cases that do not violate the protocol and complete the trial; per-protocol set analysis will be conducted for curative effects. The safety dataset refers to the randomized cases that have taken a tested drug at least once with safety evaluation data after treatment. We use mean ± standard deviation (SD) for continuous variables and percentages for categorical variables. In measured indices, an independent t-test will be used for hypothesis testing of the normal variables, while the Wilcoxon rank sum test will be used for hypothesis testing of the skewed variables. The χ2 test will be used for hypothesis testing of the counted indices. The statistical analyses will use the two-sided hypothesis test. P ≤0.05 will be set as the significance level.