Diabetes Mellitus Clinical Trial
Official title:
Improving Access to HbA1c Measurement in Sub-Saharan Africa
Glycated haemoglobin (HbA1c) is the best surrogate of average blood glucose control in diabetic patients. Large-scale studies in the USA and UK have demonstrated that lowering HbA1c significantly reduces diabetes complications. Moreover, immediate feedback of HbA1c measurement to patients improves control. However, HbA1c is unavailable in most parts of Africa, a continent with one of the highest burden of diabetes. To translate these evidences, the investigators will provide affordable access to HbA1c measurement and relevant education in 2 African countries aiming significant improvement of diabetes control. The investigators will develop with local health authorities, training and cost-recovery scheme for long-term sustainability.
The objective is to determine whether the introduction of routine affordable HbA1c
determination with immediate feedback to patients and relevant education in an underserved
population without any further intervention on drug supply would significantly improve
diabetes control. As this will be an after-versus-before type study, each patient will be
his own control.
Study setting The study will be undertaken in 10 existing diabetes care centre in two
countries, including 4 regional centers in Guinea, a West African country of 10 millions
inhabitants, and 6 regional centers in Cameroon, a Central African country of 18 million
inhabitants.
The health districts covered in Guinea are Conakry, Labe, Kankan and Boke each being
situated in a different ecological and cultural areas. In Cameroon, the health districts
covered are Biyem Assi in Yaoundé, Garoua, Limbe, Ebolowa, Bamenda, Bafoussam also covering
the 4 ecological zone of Cameroon.
All these health districts have existing diabetes care centre with trained personnel run in
public hospital with prices and medicine affordable to most of the population covered.
However, none of these centers have an HbA1c machine, and diabetes control is mainly
evaluated using blood glucose, most often fasting.
Target population The aim is to provide the service to all patients followed in the selected
centers at low cost however the first eligible 1000 patients will be included in the formal
intervention free of charge.
Eligibility All patients with a physician-confirmed diagnosis of diabetes and who have been
followed in the diabetes centre for at least one year are eligible Sample size In order to
detect a difference of 1 unit (1% glycated haemoglobin) between to samples with a standard
deviation of 1.2%, alpha coefficient of 0.001 and 0.8 power using a two-sided test, a
minimum population of 80 subjects is required. The minimum sample size if alpha is 0.01 is
55 subjects. We therefore decided a sample size of 100 patients per centre in order to be
able to analyze data taking into account center or physician effect. It thus give an overall
sample size of 1000 subjects.
Sampling method We will use a systematic sampling, enrolling consecutive eligible patients
volunteering to participate until completion of the sample size in each individual centre.
Inclusion All eligible patients, not intending to migrate from the study site within 1 year,
and volunteering to participate will be enrolled. At inclusion the following will record of
demographic characteristics, past medical history, characteristics of diabetes, evaluation
of patient knowledge, and measurement of anthropometric characteristics, blood pressure,
haematocrit, HbA1c, and urinary albumin excretion at baseline.
Intervention and follow up:
Data will be collected using a clinical record form designated to this effect. The
intervention will consist of the measurement of HbA1c at baseline, 3, and 6 months with
immediate feedback to patients and provision of targeted education after each determination,
on level, significance, and targets.
Treatment will follow usual guidelines with no additional intervention. Adjustment of
treatment will be done by the health care personnel in a treat-to-target fashion. No change
in drug supply will be introduced. No specific recommendation will be given concerning the
frequency of hospital visit between the study visits at baseline, month 3, 6, and 12. Each
centre will continue with usual follow up frequency.
At month 12, we will repeat the evaluation of patient knowledge, and the measurement of
anthropometric characteristics, blood pressure, haematocrit, HbA1c, and urinary albumin
excretion for comparison to baseline.
Timeframe
- Start date: Month 7
- End of enrollment: Month 12
- End of follow-up of last patient enrolled: Month 24
Outcome measures
Primary outcome: Change in HbA1c from baseline to 12 months
Secondary outcomes:
- Change in percentage of patients at HbA1c target from baseline to 12 months
- Change in urinary albumin excretion from baseline to 12 months The other measures will
serve for the interpretation of data Deliverables
- Dataset for each centre between Month 24 and Month 26
;
Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label
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