Type 2 Diabetes Mellitus Clinical Trial
Official title:
Empowering Primary Care Providers and Patients to Improve Chronic Disease Outcomes: The EMPOWER Participatory Action Research (EMPOWER - PAR)
BACKGROUND
Chronic disease management (CDM) presents enormous challenges to the primary care workforce
due to the rising epidemic of cardiovascular risk factors. The Chronic Care Model (CCM) was
proven effective in improving chronic disease outcomes in developed countries. Evidence that
this model works in developing countries is still scarce. Therefore, the aim of this study
is to evaluate the effectiveness of the EMPOWER-PAR intervention (multifaceted CDM
strategies based on the CCM) in managing type 2 diabetes mellitus (T2DM) and hypertension
(HPT), using readily available resources in the Malaysian public primary care setting.
METHODS
This is a pragmatic cluster randomised controlled trial - participatory action research
which is currently being conducted in 10 public primary care clinics in Selangor and Kuala
Lumpur, Malaysia. Five clinics are randomly selected to provide the EMPOWER-PAR intervention
for 1 year, while the other 5 clinics continued with usual care. Each clinic recruits
consecutive T2DM and HPT patients who fulfil the inclusion and exclusion criteria over a
2-week period.
The EMPOWER-PAR intervention consists of creating/strengthening a multidisciplinary CDM
Team; and training the team to utilise the Global CV Risks Self-Management Booklet to
support patient care and reinforcing them to utilise relevant clinical practice guidelines
to aid management and prescribing.
For T2DM, primary outcome is the change in the proportion of patients achieving target HbA1c
of <6.5%. For HPT without T2DM, primary outcome is the change in the proportion of patients
achieving target blood pressure of <140/90 mmHg. Secondary outcomes include the proportion
of patients achieving targets serum lipid profile, body mass index and waist circumference.
Other outcome measures include medication adherence levels, process of care and prescribing
patterns. Patients' assessment of their chronic disease care, providers' perception,
attitude and perceived barriers in delivering the care and cost-effectiveness of the
intervention are also evaluated.
CONCLUSION
Results from this study will provide objective evidence of the effectiveness and
cost-effectiveness of a multifaceted intervention based on the CCM in resource constraint
public primary care setting. It is hoped that the evidence will instigate the much needed
primary care system change in Malaysia.
HYPOTHESES
The primary hypothesis for T2DM patients is that the proportion achieving target HbA1c of
<6.5% would improve with the EMPOWER-PAR intervention. The primary hypothesis for HPT
patients without T2DM is that the proportion achieving target BP of <140/90 mmHg would
improve with the EMPOWER-PAR intervention.
The secondary hypothesis for T2DM patients is that the proportion achieving target blood
pressure (BP) of <130/80 mmHg would improve with the EMPOWER-PAR intervention. The secondary
hypotheses for both groups of patients (T2DM and HPT without T2DM) are that the proportions
achieving target fasting serum lipid, body mass index (BMI) and waist circumference (WC)
would improve with the intervention. Medication adherence levels and patients' perceptions
of their experience in receiving chronic disease care are also expected to improve with the
intervention. Secondary hypotheses are also made at the primary care providers' level in
terms of the process of care and prescribing pattern which are expected to improve with the
intervention. Cost-effectiveness analysis and primary care providers' perception, attitude,
experience and perceived barriers in implementing the intervention are also explored.
METHODS
- Pragmatic cluster-randomised parallel controlled trial -participatory action research
conducted in 10 public primary care clinics from two states in Malaysia which are
Wilayah Persekutuan Kuala Lumpur (WPKL) and Selangor (SEL).
- The overall duration of the study is 2 years while the duration of intervention is 1
year.
- Blinding is not possible due to the nature and complexity of the intervention.
Site Recruitment
Site eligibility
All 34 clinics led by Family Medicine Specialists (FMS) in SEL and WPKL are invited to
participate in the study and are given the site feasibility assessment form.
To be eligible, the clinics must satisfy all of the following criteria:
i. have a minimum of 500 T2DM patients and 500 HPT patients in the registry. ii. have an FMS
who is keen to participate in the study and is willing to lead the implementation of the
intervention components in the clinic.
iii. Have the minimum capacity to implement the obligatory components of the EMPOWER-PAR
intervention.
iv. located within 70 km from the central laboratory as the blood samples are transported
back to the centre for analysis.
Site selection
Site feasibility assessment is conducted to identify eligible clinics. Out of the 34 sites,
only 20 fulfil the eligibility criteria to enter the study. These 20 clinics are then
matched into 10 pairs according to their geographical locations, staffing and workload.
Geographical location is divided into urban and sub-urban areas. Urban area is defined as an
area located within a major city, while sub-urban area is defined as an area located
surrounding and within commuting distance to a major city. Staffing is defined as the number
of doctors and allied health personnel (FMS, medical officers, assistant medical officers,
staff nurses, dieticians/nutritionists and pharmacists) working in the clinic. Workload is
defined as the average number of patients being seen in the clinic per day.
Multistage randomisation is performed using computer generated tables. The first stage is to
randomly select 5 out of the 10 pairs to be included into the study. The second stage is to
randomly allocate the clinics into intervention and control arms.
Patient Recruitment
This study recruits consecutive T2DM and/or HPT patients who attend the selected clinic
within the 2-week recruitment period. They are given the patient information sheet in the
waiting area. Informed consents are obtained from those who are willing to participate.
Screening is conducted to identify eligible participants based on the inclusion and
exclusion criteria. Eligible patients are then enrolled into the study.
Inclusion criteria
Males and females aged ≥ 18 years who are diagnosed with:
1. T2DM or HPT or both
2. Seen at least once in the last one year at the primary care clinic for the above
conditions
Exclusion criteria
1. Type 1 Diabetes Mellitus
2. Receiving renal dialysis
3. Presenting with severe HPT (Systolic BP >180mmHg and/or Diastolic BP >110 mmHg)
4. Diagnosed with conditions resulting in secondary hypertension
5. Diagnosed to have circulatory disorders needing referral to secondary care over the
last 1 year e.g. unstable angina, heart attack, stroke, transient ischaemic attacks
6. Receiving shared care between primary and secondary care for complications of T2DM
and/or HPT
7. Pregnancy
8. Enrolled in another study
All patients in the intervention arm are required to be seen at least twice by the CDM team
of each clinic during the 1-year intervention period. Those who do not comply are considered
as lost to follow-up. There is no limit to the number of clinic visits a patient is allowed
to make in either arm during the course of the study.
The EMPOWER-PAR INTERVENTION
The study intervention, referred to as the EMPOWER-PAR Intervention, is developed in
accordance with the Medical Research Council (MRC) guidance on developing and evaluating
complex interventions to improve health outcomes and is implemented at the primary care
clinics for a period of 1-year.
The underlying framework in developing the complex intervention for EMPOWER-PAR is based on
6 interrelated elements of the CCM. The 6 elements are 1) organisation of health care (i.e.
providing leadership and minimising barriers to care), 2) self-management support (i.e.
facilitating skills-based learning and patient empowerment), 3) decision support (i.e.
providing guidance for implementing evidence-based care), 4) delivery system design (i.e.
coordinating care processes), 5) clinical information systems (i.e. tracking progress
through reporting outcomes to patients and providers), and 6) community resources and
policies (i.e. sustaining care by using community-based resources).
Three obligatory components which define the EMPOWER-PAR intervention are developed based on
4 interrelated elements of CCM (organisation of health care, delivery system design,
self-management support and decision support). These intervention components utilise readily
available and existing resources in the Malaysian public primary care setting.
I. Creating/Strengthening a CDM Team-a multidisciplinary team lead by FMS to improve
coordination of care for T2DM and/or HPT and co-existing CV risk factors
II. Utilising the Global CV Risks Self-Management Booklet to support patients
self-management
III. Utilising the Clinical Practice Guidelines (CPG) for T2DM and HPT to aid management and
prescribing
Two optional components of the EMPOWER-PAR intervention are developed based on the other 2
CCM elements (clinical information system and community resources):
I. Utilising clinical information system and conducting clinical audits to track progress
through reporting outcomes to patients and providers
II. Utilising community resources to support and sustain care
SAMPLE SIZE CALCULATIONS
The sample size calculation was conducted based on the randomised clustered trial design
using PASS software (Copyright (c) 2009 by Dr Jerry L. Hintze, All Rights Reserved).
Sample size calculation for T2DM patients
A sample size of 626 (313 in each arm) is obtained by sampling 10 clusters (5 intervention
vs 5 control) with 63 subjects from each cluster to achieve 91% power to detect 25%
difference in the proportion of subjects achieving target HbA1c <6.5% from baseline and
between the intervention and control groups. The test statistic used is the two-sided Z test
(unpooled). The significance level of the test is 0.05. Therefore, after allowing for 25%
dropout rate, this study aims to recruit a total sample of 836 T2DM patients at baseline
i.e. 418 in each arm and 84 from each clinic.
Sample size calculation for HPT patients without T2DM
A sample size of 438 (219 in each arm) is obtained by sampling 10 clusters (5 intervention
vs 5 control) with 44 subjects from each cluster to achieve 88% power to detect 25%
difference in the proportion of subjects achieving target BP <140/90 mmHg from baseline and
between the intervention and control groups. The test statistic used is the two-sided Z test
(unpooled). The significance level of the test is 0.05. Therefore, after allowing for 25%
dropout rate, this study aims to recruit a total sample of 584 HPT patients at baseline i.e.
292 in each arm and 58 from each clinic.
STATISTICAL ANALYSIS
The statistical analysis plan to test the primary hypotheses of the study is described.
Continuous variables will be described by summary statistics (means and standard deviations)
for normally distributed variables. If the distribution is not normal, median with
inter-quartile range will be reported instead. Other descriptive statistics, such as minimum
and maximum values will be reported when necessary. Categorical (nominal/ordinal) variables
will be described by frequencies with percentages. All outcomes are treated as categorical
variables (e.g. proportions of patients achieving targets for HbA1c and BP). To assess the
differences in the proportions of patients who are able to reach the treatment goals by
their intervention strategy, a generalized estimation equation model that adjusts for
clustering effects will be used. The model will be an independent working model. Treatment
effects will be obtained using the estimated marginal means and differences will be tested
using the Wald chi-square tests. The power of the study will be recalculated based on the
effect size and after taking into account the clustering effect of the study design. An
intention-to-treat analysis will be conducted, and P-values of less than 0.05 will be
considered significant. All analyses will be carried out using SPSS (IBM Corp. Released 2011
IBM SPSS Statistics for Windows, Version 20.0. Armonk, NY: IBM Corp.).
ETHICAL CONSIDERATIONS
The Ethics Committee of UiTM and Medical Research Ethics Committee (MREC) of the Ministry of
Health (MOH) approves the study protocol. Permission from the Family Health Development
Division (FHDD) of the MOH and the respective Health District Offices are also obtained
prior to the conduct of the study. The study is conducted in accordance to the Declaration
of Helsinki and Good Clinical Practice (GCP) requirements. Patient information sheet are
given and informed consent are obtained from all participants prior to their study
enrolment. For participants who are unable to read, the content of the consent form is read
aloud to them and a copy of the patient information sheet is given to their next of kin with
additional explanation given if needed. Confidentiality of personal information is ensured
at all times. Subject enrolment is done by the investigators and not their attending doctors
to reduce subject's vulnerability to participate in the study. Subjects are informed of any
immediate results obtained from the study that may affect their care or health.
DISCUSSION
The EMPOWER-PAR is the first pragmatic, randomised controlled trial of multifaceted chronic
disease management strategies being conducted in the Malaysian public primary care setting.
It is expected to yield important new evidence on the improvements of T2DM and HPT clinical
outcomes, the two most prevalent chronic diseases being managed in the public primary care
sector.
Ultimately, results from this study will provide objective evidence of the effectiveness and
cost-effectiveness of a multifaceted intervention based on the CCM in a resource-constrained
public primary care setting. If proven effective, the results may be generalisable to other
Malaysian public primary clinics which share the same characteristics and would probably be
inexpensive to replicate. It is hoped that the objective evidence from EMPOWER-PAR would
provide a platform to instigate the much needed primary health care system change in
Malaysia.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Health Services Research
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