Clinical Trial Details
— Status: Completed
Administrative data
NCT number |
NCT02621814 |
Other study ID # |
CJEBP-01 |
Secondary ID |
|
Status |
Completed |
Phase |
N/A
|
First received |
December 2, 2015 |
Last updated |
April 2, 2018 |
Start date |
May 6, 2016 |
Est. completion date |
October 30, 2016 |
Study information
Verified date |
April 2018 |
Source |
Children's Hospital of Fudan University |
Contact |
n/a |
Is FDA regulated |
No |
Health authority |
|
Study type |
Interventional
|
Clinical Trial Summary
Compared with breast milk and another commercially available formula, infants' growth rate
after 12 weeks' Friso formula with low glycation feeding will be assessed.
Description:
1. Sample size:Seventy two cases will be enrolled in breast milk group, 144 cases in
formula milk group, 72 cases each in commercially available formula subgroup and Friso
formula subgroup with 36 cases each in every hospital (18 males and 18 females).
2. Observation period:Observational period will maintain 12 weeks. Infants of breast milk
group are fed with breast milk before inclusion and during the trial process. In the
formula milk groups, if subjects were fed with other formula instead of commercially
available formula and Friso formula before inclusion, then a wash-out period of no more
than 2 weeks is necessary.
3. Random method: In commercially available formula subgroup and Friso formula subgroup,
infants will be included randomly. Random allocation sequence is generated in six trial
centers by the editorial department of Chinese Journal of Evidence-Based Pediatrics,
included infants are chosen and their information including name, gender, their parents'
name and telephone is reported to the editorial department of Chinese Journal of
Evidence-Based Pediatrics via WeChat. Then group division information is acquired, the
tested commercially available formula and Friso formula are given out to infants
accordingly.
4. Match of the breast milk group: Infants with purely breast milk-fed will be chosen.
Infants'gender and body weight (±5%) of breast matched with milk-fed group commercially
available formula subgroup and Friso formula subgroup.
5. Blinding method: Subjects, doctors and nurses know which formula is given. Personals in
charge of assessing stool character and ery secretion, and data analysis, are blind to
the information of group division.
6. Data records, monitoring and management 6.1 Data records 6.1.1 Original records:
Subjects' follow-up care cards are original files in this clinical trial which is in
duplicate copies. One copy should be saved in hospital. Original records shall be
traceable. Each researcher must strictly follow the principle of GCP and ensure that he
will record any observation and discovery in the follow-up care card and case report
form (CRF), all data are consistent, no optional changes are allowed. If any correction
is needed, the original record must not be changed, researchers can only add extra
descriptions and explain the reason, the correction needs to be signed and dated by
researchers who make it.
6.1.2 Case report form(CRF): Each in triplicate, it will be delivered to sponsors, main
institutions of clinical research and participating institutions of clinical research.
According to the principle of GCP, subjects' name should not appear in order to ensure
their privacy. Subjects' name must be filled in the initials.
All of the choices"□" will be marked"×". If some inspection items are not examined or
missed for some reason, it should be filled in: not examined. If the specific formula
dosage is unknown, it should be filled in: unknown. When filled in the numbers, it
should be filled in all □. If digits are not enough, it should be filled on right side.
If left side is empty, it should be filled by 0. No null terms or missing items are
allowed. Researchers must ensure that all data must be consistent with the original
record.
If modifying, researchers should draw a horizontal line in the middle of the original
record text, sidenote to modify, and then sign the modifier's name and the date. He must
not smear or cover the original record.
6.1.3 Data Record of subjects' guardian: It should be recorded according to the items
and their definitions in the designed CRF chart.
6.1.4 Extremum principles: The data, deviating significantly or outside the acceptable
range clinically, must be verified. Clinical doctors must make the necessary
instructions.
6.1.5 Data registration and preservation: Every time after the follow-up visit,
researchers should record the required information in the case report sheet timely.
After the end of each subjects' observed period, researchers should accurately record
relevant information from original records in the form of data in the CRF within 7 days.
CRF, informed consent and other documents should be examined and signed by the project
leader, then saved in the archive office of institution. If a problem is found, it
should be timely dealt with and recorded.
6.2 Data monitoring Editorial Board of Chinese Journal of Evidence-Based Pediatrics will
be in charge of data monitoring of the clinical trial. CJEBP will provide data
monitoring of the clinical trial to FrieslandCampina regularly in at middle experiment
stage and later experiment stage. During the trial, CJEBP will investigate 6 research
centers for their quality of practice at least one time, without any announcement in
advance. The monitoring subjects include child care doctors, nurses and guardians of
subjects enrolled in this trial.
6.2.1 Child care doctors: monitor the quality of explaining the research to subjects'
guardians and the informed consent signing; Random of distribution; The accurate
measurement of body length, weight and head-circumference; judgement of gut intolerance;
record of stool frequency, pictures of stools and eye secretions.
6.2.2 Nurses: motor the accuracy of the measuring equipment; the correctness of the
measuring method; the rightness of data recording (mean value of 2 measurements); the
management of trial formula (reception time, check-up, distribution subjects, date and
signature, recycling subjects, date, quantity of the rest formula and signature).
6.2.3 Guardians of subjects enrolled in this trial: randomly inspect 1-2 guardians,
investigate whether mixed feeding or mixed with other brand formula feeding exists; the
usage of trial formula; regularity of follow-up visits; taking photos of fresh stools
and eye secretions.
6.3 Data management 6.3.1 Buildup, test and data entry of WeChat client: According to
the project of the CRF,administrators will establish WeChat client, test and modify this
client, and enter data after ensuring the accuracy of this client. Every researcher in
each hospital uploads the measured data to administrators by WeChat client on the day he
completes one case observation and measurement. In order to ensure the accuracy of the
data, administrators should compare data uploaded by WeChat client with the original
CRF. Subjects' guardians will upload photos of stool character and eye secretion to
administrators by WeChat client at 3 points of follow-up time.
6.3.2 Generation and correction of doubt, quality control(QC) and database shutdown:
After completing data input and comparison, data administrators will verify the
reliability, integrity and accuracy of data according to requirements of clinical trial
scheme. If he finds loss of content or logic contradiction or filling in wrong or
uncertain data, clinical monitors will send it to clinical trial centers in the form of
data question table (DQF). Researchers will give answers to questions as soon as
possible and reply. Data administrators will modify, confirm and correct data according
to researchers' answers. After solving all of problems, quality control personnels will
check the quality of database according to QC plan. Then he will close the database
after check.
6.3.3 Data check, lock and transmit blindly: Data administrators submit data management
reports, and require a meeting about data-check blindly attended by principal
investigator, statistical analyst, data administrators, monitors, and sponsors. Check
data blindly, sign blindly data-check resolution after meeting, lock in the database;
locked data will be analyzed by personnels of statistical analysis.
7. Statistic analysis 7.1 General principles: All of the statistical tests must be
two-sided tests, P<0.05 is considered to be statistically significant difference for all
tests. Mean, median, standard deviation, maximum, minimum, 25% and 75% quintile are used
for statistical description of measurement data. Count data or level data is described
by frequency ( percentage).
SAS9.1.3 statistical software is used for statistical analysis. 7.2 Analysis of missing
cases: List cases number of inclusion, completion and falling off. Loss rate and
comparison between groups should be analyzed by Chi-square test and Fisher's exact
probability method.
7.3 Evaluation of effectiveness: Measurement data of indexes(Growth rate of height,
weight and head circumference at 4,8,12 week, defication frequency) should be analyzed
by normality test firstly. If data conforms to normal distribution, the comparation
between formula milk group (commercially available formula subgroup and Friso formula
subgroup) and breast milk group should be analysed by One-Way ANOVA method. LSD method
is used for multiple comparisons. If data does not conform to normal distribution, then
Wilcoxon Rank-Sum test is used. A level of significance is α=0.05 (two-tailed).
Frequency data of indexes ( incidence of constipation at 4,8,12 week, eyes secretion) is
recorded as cases or percentage. If theoretical frequency <5 or total observed frequency
<30, Fisher's exact probability method is used; otherwise Chi-square test is used. A
level of significance is α=0.05 (two-tailed).
8. Quality control Standardized operation procedures should be established in all of
research process.
8.1 Qualification of research institution: Research institution must be community health
service centers qualified for baby healthy check-up.
8.2 Qualification of researchers: The researchers need GCP training and work under the
guidance of senior professionals.
8.3 Trial quality control measures: ①Before the start of clinical trials, researchers
(including nurses) must receive training for measurement of height, weight and head
circumference; ②check measurement bed before measurement everyday. Researchers must
compare scale on plastic flexible rule with that on standard steel rule and change
plastic flexible if error >0.1cm. ③The pictures of the feces and eyes will be
independently scored by 2 specialists under the condition of unknowing the group. ④The
specialist must be responsible for experimental formula, counter locked, storage at room
temperature away from light. The remaining experimental formula will be stored
separately, registering number. At the end of trial, the remaining experimental formula
will be sent back to sponsor.⑤Monitor: Monitor will be appointed by sponsor, ensuring
subjects' interests during period of trial. Trial record and data report must be true,
accurate, complete and correct, ensuring that trial must comply with both approved plan
and Relevant laws.
9. Definition and management of adverse events 9.1 Definition of adverse events: adverse
events are defined as those occur after a patient or a subject in a clinical study
receives a tested product, the event does not necessarily have a causal relationship
with the test products. Adverse events are the diseases or signs or symptoms that occur
during the course of the study (including abnormal laboratory findings). Adverse events
can be serious or not serious, may or may not cause the subjects to withdraw from the
study. All adverse events must be recorded, and the relationship between the product and
the product is evaluated.
9.2 Information collection of adverse events: researchers must know and record the following
information concerning adverse events: subjects and date, description of the event, source of
report, the suspected products, continuous time, frequency, extent, severity, measures taken,
results and complications, the relationship with tested products.
9.3 Extent of adverse events: Mild: symptoms were not obvious, only slightly harmful to
health. Middle: the symptoms are obvious, but can be tolerated, without immediate treatment.
Serious: it is hard to bear.
9.4 Severity of adverse events: Serious adverse events refer to the follwing adverse events
which appear at any of the dosage: leading to death, threatening life , need to be
hospitalized or hospitalization has been prolonged, resulting in permanent or significant
disability and loss of function, congenital anomalies or birth defects, or other significant
medical events. Not serious: Those events can not be defined as serious adverse events are
not serious events.
9.5 Unexpected or expected serious adverse events: Researchers must assess whether the
adverse events be expected to occur or not. Expectation is evaluated by Safety Officer
Medical which base on the current knowledge and existing product information. An unexpected
adverse event is one that the nature, severity, frequency are inconsistent with conditions of
the study and ( or) product information.
All suspected adverse events related to the tested products, as well as serious adverse
events that are not expected to be serious are considered to be SUSARs (suspicious unexpected
serious adverse event). SUSAR need to be reported to the management authority or independent
ethics committee in a very short time.
According to the Chinese food and Drug Administration report of adverse reactions and and
regulations of drug supervision, any new or serious adverse reactions of any drug must be
reported within 15 days, any deaths must be reported immediately. Fax: +86-10-67184591,
Email: report@adr.gov.cn.
9.6 Relationship with the tested product: Medical institutions will evaluate the relationship
between adverse events and the tested product according to the following standards. ①
unrelevant: there is evidence proving that adverse events are caused by other reasons. For
example, adverse events are obviously caused by the disease, adverse events are consistant
with effects or adverse reactions of the drugs, or adverse events had already existed before
using the tested product research. ② Not likely to be relevant: it seems to have a
time-relationship with the use of tested product, but the occurrence of adverse events can be
explained by other reasons. ③Probably relevant: it seems to have a time-relationship with the
use of tested product, and adverse events seem to have a causal relationship with the
product. ④ Surely relevant: it seems to have a time-relationship with the use of tested
product, and no other reasons can explain the occurrence of adverse events. Adverse events
diminish or disappear after stopping using tested products, and symptoms occur once again
with the use of tested products.
9.7 report and record: ①serious adverse events: clinical safety management must be informed
by fax or scaning within 24 hours, regardless of whether the event is related to the tested
product. When it's the first time to report, or each time when SAE needs modification,
researchers need to complete serious adverse events spreadsheet in the eCRF, The spreadsheet
will be automaticly sent to clinical safety manager xt211311@aliyun.com in the form of email.
All serious adverse events are also required in the eCRF spreadsheet severity column to
choose "serious". ②Not serious adverse events: all not serious adverse events must be
recorded on the eCRF's adverse events page.
9.8 follow-up visits: All serious adverse events should be followed up until the outcome of
the event. The researchers need to inform the clinical safety manager of any follow-up
information within 24 hours, such as changes in diagnosis, results, the date of remission,
the termination of treatment, and so on.
If serious adverse events persist after discontinuation of the study, follow-up is required.
In addition, when adverse events occur, if it's necessary to further evaluate the causal
relationship between adverse events and the tested product, then all the examinations and
laboratory results must be recorded in the case report form or attached document. Within 30
days after the last use of the study product, the SAE also needs to be reported in the same
way within 24 hours.
9.9 Inform: The sponsor is responsible for the safety evaluation of the tested product. The
sponsor must promptly inform all researchers, observational hospitals and regulatory
authorities of any discoveries that are likely to affect subjects' safety, influence study
process, change the ethics committee's attitude to approve or agree that research continues.
9.10 Report: The sponsor must accelerate reporting to all investigators, observational
hospitals, IRB (S) /IEC (s) and management authorities (if necessary) about all serious and
suspicious unexpected serious adverse reactions (SUSAR).
This accelerated report needs to comply with applicable regulatory requirements, and ICH
guidelines on the management of clinical safety data: standards of accelerated reporting.
The sponsor should submit all latest progress and staged reports of security to management
authorities, according to applicable regulatory requirements