Factors Associated with Prolonged Poor Glycemic Control in Type 2 Diabetes Mellitus (T2DM) Patients Followed in the Department of Internal Medicine at the Yalgado Ouedraogo Teaching Hospital, Ouagadougou (Burkina Faso) ()
1. Background
The major interventional studies in diabetes mellitus unanimously recognize the benefit of glycemic control on the prevention of microvascular complications [1] [2] [3] [4]. Despite the controversies, this benefit also exists for macrovascular complications, but only becomes significant after a longer follow-up period, and gradually diminishes if glycemic control deteriorates [3].
Notwithstanding the variability of glycemic targets depending on patient characteristics, the recommended glycemic control for most patients with type 2 diabetes mellitus (T2DM) is defined by a hemoglobin A1c (HbA1c) target of 7% or less (53 mmol/mol) [5] [6] [7]. Studies in African research centers reported poor glycemic control of T2DM patients in proportions ranging from 68.3% to 83.3% [8] - [14]. These ranges were similar to those reported in Asia (81.6%) [15] but higher than those reported in Europe [16] (37.4%) and in the United States (38%) [17].
The factors associated with poor glycemic control are demographic, anthropometric and behavioral factors, as well as factors related to diabetes mellitus and the environment [8] [9] [10] [11] [13] [14] [18] - [22].
In 2001, a descriptive and analytical cross-sectional study with retrospective data collection over a 4-year-period assessing glycemic control in Burkina Faso (BF) reported that 57.5% of diabetes mellitus patients had poor glycemic control. The factors influencing glycemic control found in that study were similar to those found in the literature [23]. Twenty years after this aforementioned study, we initiated the present work, which, compared to the first one, involved a population exclusively restricted to T2DM patients. Indeed, the authors agree to promote the analysis of data from populations with the same type of diabetes mellitus. Heterogeneity in the typology of diabetes mellitus would be a confounding factor. For them, each type of diabetes mellitus has its own specific characteristics due to epidemiology, environment, heredity, mode of onset, and progression [24] [25]. In addition, the criteria for defining poor glycemic control in the present effort is a methodological difference from the previous study.
The objective of this work was to determine the prevalence of prolonged poor glycemic control in T2DM and to identify factors associated with this observed prolonged condition in the cohort of T2DM patients monitored and treated in the Department of Internal Medicine of the Yalgado OUEDRAOGO Teaching Hospital in Ouagadougou in order to optimize therapeutic education of these patients.
2. Methodology
2.1. Framework of the Study
The study took place in the Department of Internal Medicine of the Yalgado OUEDRAOGO Teaching Hospital. The internal medicine department within the hospital is a multidisciplinary department that mainly deals with metabolic and endocrine pathologies and Human Immunodeficiency Virus (HIV) infection.
2.2. Type and Population of the Study
This was a descriptive and analytical cross-sectional study combining retrospective data collection from previous years on patients’ follow-up and prospective data collection of missing information in their respective medical records. The study population consisted of a cohort of diabetes mellitus patients, at least 18 years of age, followed and treated in the Department of Internal Medicine of the Yalgado OUEDRAOGO Teaching Hospital between January 1, 2010 and December 31, 2018.
2.3. Criteria for Inclusion and Non-Inclusion
Included in this study were T2DM patients followed and treated for at least one year with at least two HbA1c measurements within the last year of follow-up. Not included in the study were patients who had made a change in diabetes therapy within the last 3 months and also those who did not respond to the call to complete the missing information in the medical record.
2.4. Sampling
This was a systematic random sampling from all the patients who were followed in the internal medicine department between January 1, 2010 and December 31, 2018, following a draw step of 10.
2.5. Questionnaire
The questionnaire was developed by the authors and their peers in the Department of Internal Medicine of the Yalgado OUEDRAOGO Teaching Hospital (Appendix 1). We also used Morisky’s assessment questionnaire [26] in order to appreciate the quality of the treatment’s compliance (Appendix 2).
2.6. Operational Definitions
Prolonged poor control of diabetes mellitus was reported in all patients with at least one of the outcomes of the various HbA1c measures in the last year of follow-up having a threshold above 7%. Alternatively, fructosamine was used to assess poor glycemic control when at least one of the outcomes of the various fructosamine measurements in the last year of follow-up had a threshold above 290 micromoles/L. Adherence was measured using Morisky’s questionnaire [26].
Lipid fraction abnormalities have been defined by adopting the 2017 standards of the French National Authority for Health on lipid assessment [27] (Appendix 3). Microangiopathy was defined by the presence of either neuropathy and/or nephropathy and/or retinopathy. Neuropathy was defined by an abnormality of the filament test and/or an abnormality of the tuning fork test and/or reflex abnormalities. Nephropathy was defined by measurement of 24-hour proteinuria. The cut-off value for 24-hour proteinuria was 300 mg/24 h. Retinopathy was retained based on the results of fundus examinations with an ophthalmoscope. Macroangiopathy was defined by the presence of coronary artery disease, cerebrovascular disease and arteriopathy of the lower limbs. These findings were systematically searched for in the patients’ follow-up medical records. Arteriopathy was defined both on clinical criteria (intermittent claudication, decubitus pain, absence of both foot pulses, gangrene, ischemic ulcer) and imaging criteria (systolic pressure index less than 0.9, systolic pressure of the big toe greater than or equal to 1.3 accompanied by medicalcosis, calcifications, aneurysm and a perivascular environment appreciates hemodynamics for therapeutic purposes). The monthly gain consisted of the patient’s total income plus donations. Monthly expenses (direct cost of management) for diabetes mellitus included expenses for: travel, consultation, testing, and purchase of medication and capillary blood glucose strips.
2.7. Data Collection
Data collection covered the period from February 15, 2020 to May 15, 2020. The collection tool was an anonymous questionnaire. Data collection was done in conjunction with follow-up consultations by a physician based on a survey form. The use of medical records made it possible to extract clinical data (the conditions leading to the identification of diabetes mellitus, time since diabetes mellitus diagnoses, presence of micro- or macro-angiopathy) and paraclinical data (blood glucose and HbA1c results) of previous years follow-up. The individual interview allowed the completion of certain missing information, in particular drug compliance based on items from Morisky’s assessment questionnaire [26], certain sociodemographic and anthropometric characteristics and the financial status of the patients. Sociodemographic data (age, gender, level of education, average monthly income, marital status and residence), anthropometric data (weight, height, waist circumference and body mass index [weight divided by height squared]), and behavioral factors (alcohol and tobacco consumption) were collected.
2.8. Ethical Considerations
Confidentiality during the interview and respect for the anonymity of the questionnaire user were observed throughout this study. All personnel directly or indirectly involved in the data collection were health workers who were bound by strict professional secrecy. Free and informed verbal consent was obtained from patients prior to their inclusion in the study. Patients’ refusal to participate in the study did not preclude their diabetes management and follow-up at the center. Personal information about each patient was coded with a number that did not identify the patient when the study results were published.
2.9. Methods of Statistical Analysis
Statistical analyses were performed using Statistical Product and Service Solutions (SPSS) version 20. Quantitative variables were presented as means or medians with indicators of dispersion (standard deviation and percentile). Qualitative variables were described by the frequencies of the different modalities.
To determine the risk factors associated with poor glycemic control, we used a logistic regression model. A bivariate analysis was performed to analyze the relationship between each variable and poor glycemic control. A final model was then determined by multivariate logistic regression. All variables associated with poor glycemic control in bivariate logistic regression with a p-value less than 0.20 were included in the full model. Then, we used a stepwise descending method to obtain the final model, which was then tested by a Receiver Operating Characteristic (ROC) curve. The significance level was set at 5%. Raw and adjusted Odds-Ratio (OR) and 95% confidence interval (CI) were presented.
3. Results
3.1. General Characteristics of the Study Population
A total of 270 patients were included in this study. Poor glycemic control of diabetes mellitus was observed in 73.70% or approximately two-thirds of the patients in the cohort. The mean age of patients was 55.97 years (standard deviation [SD]: ±11.52 years) and the sex ratio (male/female) was 0.6 in favor of female. More than half of the population had a formal education (59.26%). One out of two patients (55.92%) was overweight. More than one out of two patients (67.04%) had at least one underlying health condition recorded in their medical history. History of arterial hypertension was the most represented (41.85%) condition. More than two thirds (85.19%) of participants were supported by their families in the management of their diabetes mellitus. The average expenditure for diabetes mellitus care was 55.82 USD (SD: 28.25) per month. Table 1 shows the distribution of patients in the study according to their general characteristics.
3.2. Characteristics of Diabetes Mellitus
The average time period since diagnostic of diabetes mellitus was 5.85 years (SD: ±5.15 years). At least one complication of diabetes mellitus was found in more than half (68.15%) of the population. Almost all (94.81%) the patients in the study were receiving a pharmacological treatment for T2DM. The mean number of tablets taken was 2.94 (SD: ±1.56) per patient. Table 2 shows the distribution of study patients by their clinical status of diabetes mellitus.
3.3. Factors Associated with Prolonged Poor Type 2 Diabetes Mellitus Control Univariate Analysis
3.3.1. Relationship between General Characteristics of the Study Population and Prolonged Poor Diabetes Mellitus Control
The level of education (p = 0.02) and the presence of abdominal obesity (p = 0.04) were associated with prolonged poor diabetes mellitus control. Patients with low formal education had prolonged poor control of their diabetes mellitus. The same was true for those with abdominal obesity. There were no factors studied that were associated with prolonged poor diabetes mellitus control with respect to gender, age, medical history, lifestyle (tobacco, alcohol, physical activity), family status, place of residence and income level. In terms of family support, this variable was also associated with prolonged poor diabetes mellitus control (p = 0.03). The increase in monthly expenditures on diabetes mellitus care was correlated with prolonged poor diabetes mellitus control (p < 0.01). Expenditures on diabetes mellitus care were higher in patients with prolonged poor glycemic control.
3.3.2. Relationship between Diabetes Mellitus and Prolonged Poor Control
Dietary intake measures alone (p < 0.01), insulin use alone (p < 0.01) or in combination with an oral antidiabetic drugs (p < 0.01), combination of oral
Table 1. Distribution of study patients by general characteristics (N = 270).
HIV: Human Immunodeficiency Virus; USD: United States Dollar.
Table 2. Distribution of study patients by diabetes mellitus characteristics (N = 270).
T2DM: Type 2 Diabetes Mellitus.
antidiabetic drugs (p < 0.01), and poor adherence to Morisky’s scale diabetes mellitus medication (p < 0.01) were factors associated with prolonged diabetes mellitus imbalance. These patients had prolonged poor glycemic control except for those on dietary measures alone, who were at lower risk of prolonged imbalance (OR = 0.08, 95% CI [0.02 - 0.30]; p < 0.01).
3.4. Multivariate Analysis
In multivariate analysis with bivariate logistic regression, six factors were independently associated with prolonged poor diabetes mellitus control. These were no formal education (OR = 8.34, 95% CI [1.97 - 35.22]; p < 0.01); family support for diabetes mellitus management (OR = 0.65, 95% CI [0.45 - 0.94]; p = 0.02); presence of abdominal obesity (OR = 2.27, 95% CI [1.08 - 4.77]; p = 0.03); a history of hospitalization (OR = 7.39, 95% CI [2.97 - 18.39]; p < 0.01); poor adherence to antidiabetic treatment (OR = 2.97, 95% CI [1.42 - 6.18]; p < 0.01); presence of microangiopathy (OR = 5.05, 95% CI [2.36 - 10.81]; p < 0.01).
Table 3 and Table 4 show respectively the relationship between the general characteristics of the study population and prolonged poor diabetes mellitus control and the relationship between diabetes mellitus characteristics and prolonged poor control.
The model specification was verified using the Roc statistical method. Figure 1 shows sensitivity and specificity of factors associated with prolonged poor control of T2DM.
The area under the curve was 0.88, which reflects a very good sensitivity and specificity of these factors associated with poor long-term control of T2DM.
4. Discussion
4.1. Prevalence of Prolonged Poor Control of Diabetes Mellitus
Approximately two-thirds (73.70%) of the patients in our study had prolonged poor diabetes mellitus control. This proportion was similar to that reported by Kibirige in Uganda (73.5%) [28] and Omar in Sudan (71.9%) [29]. It was lower in the studies by Tapsoba in Burkina Faso (57.5%) [23], Souliotis in Greece (57.1%) [30] and Cai in China (31.5%) [31]. In contrast to studies by Tekalegn in Ethiopia (80%) [32], Hai in Pakistan (81.6%) [15] and Rahman in Bangladesh (82%) [33] which found a higher prevalence.
Figure 1. Sensitivity and specificity of factors associated with prolonged poor control of T2DM.
Table 3. Relationship between general characteristics of the study population and prolonged poor diabetes mellitus control (N = 270).
Abbreviations: OR: odds ratio; CI: confidence interval; HIV: Human Immunodeficiency Virus; USD: United States Dollar.
Table 4. Relationship between characteristics of diabetes mellitus and prolonged poor control (N = 270).
Abbreviations: OR: odds ratio; CI: confidence interval; T2DM: type 2 diabetes mellitus.
Several factors could explain these differences in proportion. For example, in Cai’s study in China, where the prevalence of poor diabetes mellitus control was lower than in our patients, the assessment of diabetes mellitus control was done in patients at the beginning of their therapeutic education [31]. It has been documented that the profile of diabetes mellitus control tends to deteriorate overtime [8] [13] [15] [18] [33].
Similarly, in the Da Vico study, where the proportion of poor diabetes mellitus control was 36.7% at 12 months after the diagnostic of diabetes mellitus, all patients had received therapeutic education [34]. Our high proportion of poor diabetes mellitus control could be explained by the low completion rate of therapeutic education in the patient population, 24.3% [35] versus 100% [34]. Indeed, therapeutics education creates conditions for improved patient compliance and follow-up.
Compared to the study that was conducted in Burkina Faso [23], the endpoints for diabetes control differed: mean HbA1c versus normal HbA1c on a continuous basis. The greater difficulty in maintaining normal HbA1c on a continuous basis may explain why there were fewer patients in control than in the previous study in which HbA1c could vary over time.
4.2. Factors Associated with Prolonged Poor Control of Diabetes
4.2.1. Sociodemographic Characteristics
Gender was not associated with prolonged poor diabetes mellitus control in our study (OR = 0.74, 95% CI [0.42 - 1.31]; p = 0.30), which were similar to findings by some authors [23] [36]. Others found different results: poor prolonged control associated with the female gender [8] [18] [19] [20] and poor prolonged control associated with the male gender [21] [33].
This result may raise questions. Indeed, since women attend health facilities more often than men [37], one would be tempted to think that they would have better results in terms of treatment effectiveness. However, a systematic review concluded that the reduction in HbA1c levels obtained during regular diabetes mellitus follow-up visits persisted for up to 6 months, and tended to diminish after 12 or 24 months [38].
Age was not a factor associated with prolonged poor diabetes mellitus control in our study (OR = 0.74, 95% CI [0.4 - 1.37]; p = 0.34). This result was similar to some studies [11] [22] [30] [39]. For other authors, age less than 40 years was associated with poor glycemic control [18] [21] [40] [41].
These results could be explained by methodological differences. Age being a continuous variable, to better appreciate the influence of age on poor diabetes mellitus control a better stratification was indicated than dichotomization into <65 years old and ≥65 years old in our study.
Low educational level was associated with diabetes imbalance in our study, (OR = 8.34, 95% CI [1.97 - 35.22]; p < 0.01). Such an observation has also been reported by some authors [14] [19] [21] [42] [43] [44]. However, Demoz in a recent study found opposite results [18].
This negative influence of low formal education on glycemic control could be explained by the difficulty that health workers may have in conducting therapeutic education based on approaches or strategies adapted to the socio-cultural and educational level of our patients. It is therefore necessary to take this into account in the awareness and education directed at different sub-populations.
4.2.2. Economic Characteristics
Low income was not associated with prolonged poor diabetes mellitus control in our study (OR = 0.83, 95% CI [0.20 - 3.39]; p = 0.80).
This result seems paradoxical, as access to care is more difficult for low-income people, especially in a context where there is no health insurance. Several studies of T2DM patients have shown that poor glycemic control is associated with low income [14] [19] [30] [33].
Our study showed that patients who had a high financial burden for diabetes mellitus care were more likely to have poor diabetes mellitus control (OR = 2.55, 95% CI [1.21 - 5.39]; p = 0.01).
This result could be explained by the financial burden of patients, which in the long run may have an impact on compliance and regularity of follow-up.
4.2.3. Anthropometric Characteristics
Patients with abdominal obesity had prolonged poor glycemic control in our study (OR = 1.76, 95% CI [1.00 - 3.84]; p = 0.04). This observation has been made by several authors [10] [11] [18] [39].
Indeed, abdominal obesity is associated with insulin resistance. However, patients with insulin resistance are more difficult to treat because they require, for example, higher doses of insulin for insulin therapy.
4.3. Lifestyle
Smoking was not a factor associated with prolonged poor diabetes mellitus control in our study (OR = 2.08, 95% CI [0.69 - 6.26]; p = 0.71). Some studies found contrary results [19] [43] [45] [46]. According to Ohkuma, HbA1c levels increase proportionally with the daily amount and duration of tobacco exposure [47].
In our study, alcohol consumption was not a factor associated with prolonged poor diabetes mellitus control (OR = 0.89, 95% CI [0.51 - 1.58]; p = 0.71). Achila found opposite results [10]. Wiss in his study reported that alcohol reduced the HbA1c level, which may indicate a beneficial effect on glycemic control [48]. This study concluded that moderate and/or heavy alcohol consumption led to a significant reduction in the HbA1c level, highlighting the correlation between the amount of alcohol and the HbA1c level [31].
4.4. Adherence to Treatment
In our study, poor medication adherence was associated with prolonged poor diabetes mellitus control (OR = 2.97, 95% CI [1.42 - 6.18]; p < 0.01). This observation was found in many other studies [18] [33].
A study conducted in Burkina Faso reported that the main reasons for non-compliance with diabetes mellitus medication treatment were oversight and the geographical and financial inaccessibility of patients [49]. To these, we can add:
Frequent interruptions in therapy due to denial of the chronicity of the illness,
Work overload leading to a communication problem and having a negative impact on the doctor-patient relationship and trust. One meta-analysis found that physician consultation time in developing countries was less than 5 minutes in 18 of the 67 countries included in the study [50]. The patient’s needs and concerns cannot be addressed in this amount of consultation time.
Physical activity practice was not a factor associated with prolonged poor diabetes mellitus control in our study (OR = 0.67, 95% CI [0.38 - 1.17]; p = 0.16). Studies have found similar results [16] [18]. Others, however, found contrary results [33] [39] [43] [51].
This result seems unexpected. Indeed, several meta-analyses and systematic reviews have clearly demonstrated the benefits of physical activity practice in terms of glycemic control.
In our study, neither the possession of a glucometer (OR = 0.86, IC 95% [0.5 - 1.5]; p = 0.61), nor the practice of self-monitoring of blood glucose (OR = 0.93, 95% CI [0.54 - 1.60]; p = 0.81) were factors associated with diabetes mellitus imbalance. These data were contrary to those in the literature [19] [33].
Our result could be explained by the lack of optimization of the self-monitoring of blood glucose device (difficult access to strips, inefficient use, less reactivity or inability of our patients to self-manage) in our context.
Patients who were supported by their families were protected from prolonged poor diabetes mellitus control in our study (OR = 0.65, 95% CI [0.45 - 0.94]; p = 0.02). Similar results have been reported by some authors [15] [19].
This support from the family would help the patient to have a less contemptuous view of the disease. The family could also be a source of motivation for the patient through a personalized and often negotiated self-monitoring of blood glucose.
4.5. Clinical Aspects of Diabetes
Time since diabetes mellitus diagnostic was not associated with prolonged poor diabetes mellitus control in our study (OR = 1.05, 95% CI [0.52 - 2.15]; p = 0.88). Some authors found similar results [23] [30]. Other studies found opposite results [8] [13] [15] [19] [33] [40] [43] [50] [52].
From a pathophysiological perspective, one would expect poor control of diabetes mellitus due to the continuous decline in β cell functioning characteristic of T2DM and the difficulty in balancing diabetes mellitus over time. However, data modeling of large intervention studies has not been able to hypothesize a threshold value for the age of diabetes mellitus [1] [2] [3] [4].
Patients with a hospitalization history for an acute diabetes mellitus-related event had a higher risk of prolonged poor diabetes control (OR = 14.79, 95% CI [6.44 - 33.96]; p < 0.01). In fact, according to one study, these hospitalizations occurred in patients who were generally unobservant, with already complicated diabetes mellitus showing HbA1c levels greater than 10.61% vs. 9.07% respectively before and after hospitalization [53].
Microangiopathy (OR = 8.85, 95% CI [4.64 - 16.90]; p < 0.01) or macroangiopathy (OR = 2.47, 95% CI [1.40 - 4.34]; p < 0.01) were factors associated with prolonged poor diabetes mellitus control. Authors found similar results [1] [2] [3] [4]. Demoz, on the other hand, reported opposite results [18]. In the literature, poor control of diabetes mellitus is thought to be associated with the progression of the disease to complications. However, the association of microangiopathy with poor glycemic control in our study seems unexpected. Perhaps it was necessary to correlate fasting blood glucose measurements to better appreciate this association rather than normal HbA1c on a continuous basis.
4.6. Diabetes Mellitus Treatment
The use of oral antidiabetic drugs alone was not associated with prolonged poor diabetes mellitus control in our study (OR = 0.93, 95% CI [0.5 - 1.71]; p = 0.82). Our results were contrary to those of a study from Algerian [13]. On the other hand, the use of combination oral antidiabetic drugs was associated with prolonged poor diabetes mellitus control (OR = 11.33, 95% CI [2.89 - 44.33]; p < 0.01). Our results were similar to those of the Algerian study [13]. The explanation may stem from therapeutic inertia related to the patient and/or the practitioner. Indeed, in practice, many dual therapy patients remain unbalanced but are reluctant to prescribe insulin; oral triple therapy is an option that is very often inaccessible in our context.
It is important to note that the use of combination of oral antidiabetic drugs is associated with poorer compliance due to the number of tablets and the number of doses to be taken. This could lead to a move towards prescribing a single antidiabetic drug.
Insulin use alone (OR = 24.29, 95% CI [5.54 - 106]; p < 0.01) or in combination with oral antidiabetic drugs (OR = 14.66, 95% CI [2.43 - 88.48]; p < 0.01) was a factor associated with prolonged poor diabetes mellitus control in our study. These results were similar to those of other studies [13] [16] [19] [30].
This result could be explained by the insulin recovery, in a context of prolonged diabetes mellitus condition that is therefore difficult to balance. In addition to this would be the problem of adherence to insulin therapy, its cost and the difficulties of conservation (disruptions of the cold chain). It is also known that the balance of diabetes mellitus tends to deteriorate with the duration of follow-up [8] [13] [15] [18].
Patients on dietary intake measures alone were protected against prolonged poor diabetes mellitus control in our study (OR = 0.08, 95% CI [0.02 - 0.3]; p < 0.01). Such an observation was made by Tapsoba in Burkina Faso [23]. On the other hand, our results were contrary to those of an Algerian study [13].
Our result can be explained by the following treatment approach: when a patient in his last year of follow-up is still on hygienic dietary measures alone, this diabetes mellitus condition is most often balanced and there would be no need to prescribe medication.
5. Limitations and Constraints of the Study
This study assessed prolonged poor glycemic control and developed a score associated with the likelihood of poor glycemic control in T2DM patients in their final year of follow-up in the internal medicine department. However, there were limitations and biases that needed to be considered in interpreting the results. These were related to:
An overestimation bias due to the HbA1c target greater than or equal to 7 to retain the diabetes mellitus imbalance, which is usually only the minimum value for judging the diabetes mellitus imbalance. The retrospective nature of the study did not provide all the data to individualize the targets.
A reporting bias related to the declarative nature of the answers given to the questionnaire, particularly in the area of assessing compliance with Morisky’s drug treatment [26].
Despite these limitations and biases, the observed results are in agreement with many studies in the literature as discussed above.
6. Conclusion
About two-thirds of the study population had prolonged poor control of diabetes. Factors associated with prolonged poor glycemic control were the educational level, the nature of family support for the management of diabetes mellitus, hospitalization for a diabetes-related event, the presence of abdominal obesity, poor adherence to medication, and the presence of microangiopathy. Lifestyle, environment (family support), and adherence to treatment seem to be key to good glycemic control. The practitioner should take these elements into account in his or her daily practice. In the context of developing countries, and in the absence of health insurance, a predictive score would be a tool to help in the identification of patients at risk of diabetes imbalance and would contribute to improving management of these patients.
Appendix 1: Data Collection Sheet
File number: ........................... File number: ..............................
1) GENERAL INFORMATION
Surname and First Names (Initials): .............................................
Age in the last year of follow-up (in years): .................................
Sex: Male /__/ Female /__/
Patient’s area of residence (hospital’s implantation area): Yes /__/ No /__/
Level of education: Not Educated /__/ Primary level /__/ Secondary level /__/
University level /__/
Family status: Lives as a couple (married, surrounded by family) No (single, divorced, widowed, separated/divorced)
Average monthly income in USD:
❏ <92.62 [92.62 - 277.86[ [277.86 - 463.1[ >463.1
How much do you estimate the different monthly expenses to care for your diabetes (in USD)?
❏ ≤27.79 ]27.79 - 55.57] >55.57
Do you feel that your family is an important help in the management of your diabetes?
/__/ never /__/ a little /__/ often /__/ always
2) MEDICAL HISTORIES
Lifestyle:
Alcohol: Drinking Alcohol No-drinking
NB: 3 glasses per day for men and 2 glasses per day for women:
Tobacco: Current smoker (have smoked in the last 30 days)
❏ Non-smoker Former smoker
If former smoker: <3 years >3 years
Do you practice sports (jogging, walking, indoors, ...)? Yes No
If yes, how many times a week?
❏ Less than 3 times More than 3 times
Are there diabetics in your family?
❏ Yes No
Medical ATCD:
❏ Arterial hypertension HIV infection Viral hepatitis
❏ Pulmonary tuberculosis Stroke Kidney failure Solid cancers
❏ Osteoarthritis Depression
3) HISTORY OF DIABETES
How long have you been aware of your diabetes (in years):
❏ <5 [5 - 10[ ≥10
Circumstance of Discovery of Diabetes:
Incidental /__/ Functional Signs /__/ Complication /__/
Type of treatment during the last year of follow-up:
MHD alone /__/; Insulin /__/; ADO /__/
Have you ever been hospitalized: Yes /__/ No /__/
Do you have a glucometer?: Yes /__/ No /__/
If yes, do you monitor your blood glucose at home at least once a month?
Yes /__/ No /__/
4) CLINICAL EXAMINATION
a) Vitals during the last year of follow-up:
Weight (kg):.................... Size (m).................. Height (cm)..................
TAS (mmHg)............................. TAD (mmHg).............................
b) Search for complications during the last year of follow-up
Nephropathy: yes /__/ no /__/ Retinopathy: yes /__/ no /__/
Glaucoma: yes /__/ no /__/ Cataract: yes /__/ no /__/
Neuropathy: yes /__/ no /__/ Arteriopathy: yes /__/ no /__/
Diabetic foot: yes /__/ no /__/ Stroke: yes /__/ no /__/
Coronary insufficiency (Angina, MDI, ...): yes /__/ no /__/
Dyslipidemia: yes /__/ no /__/
c) PARACLINIC
Q: Quarter.
Lipid fraction abnormalities (mmol/l)
Triglycerides:................ Total cholesterol.................. HDLc..........................
LDLc..................... MDRD (kidney function): .........................
Appendix 2: Morisky Compliance Assessment
Interpretation: Each answer “no” is considered as “1” and each “yes” is classified as “0”.
The exception is made in question 5, where each “Yes” answer is considered as “1” and each “No” is classified as “0”.
For question 8, if a patient chooses an answer “never/rarely” the score is “1” and if he chooses the answer “all the time” the score is “0”.
The answers “occasionally, sometimes, regularly” are respectively evaluated as “0.25, 0.5, 0.75”.
Appendix 3: Lipid Fraction Abnormalities Defined by 2017 Standards of the French National Authority for Health on Lipid Assessment
Cholestérol total: 4.10 - 5.20 mmol/l ou 1.6 - 2.0 g/l
Triglycéride: 0.40 - 1.70 mmol/l ou 0.35 - 1.50 g/l
HDL-cholestérol: superior a 1.0 mmol/l ou suprior a 0.40 g/l
LDL-cholestérol: inferior a 4.1 mmol/l ou inferior a 1.60 g/l