The goal of this single-arm, open label pilot study is to evaluate liraglutide at the recommended dosage administered subcutaneously + lifestyle counselling for the management of people living with HIV (PLWH) with obesity defined by a BMI ≥30 kg/m2 who are on dolutegravir-based ART. Following individual informed consent, all participants will undergo a series of basic cardiometabolic labs. They will then be initiated on liraglutide 0.6 mg administered subcutaneously, and this dose will be gradually increased over a period of 4 weeks to a dose of 3.0 mg daily. Alongside drug administration, participants will receive lifestyle counselling regarding diet and physical activity. Following completion of a 12-week "on treatment" period, liraglutide will be stopped and participants will be followed for an additional 12-weeks off treatment. Body weight, cardiometabolic risk parameters, and a suite of patient-reported outcomes regarding diet, physical activity, sleep, and quality of life will be assessed periodically over the course of the study.
South Africa has the largest population of PLWH globally, with a prevalence of 17% in adults or 7.2 million PLWH. The rapid scale-up of ART programs has resulted in \>6 million PLWH on treatment, significant gains in life expectancy, and a large population of aging PLWH. With increasing life expectancy, obesity and type 2 diabetes have become growing threats for PLWH in South Africa and globally. One recent study found that 63% of PLWH are overweight or obese, and 6% have diabetes in this setting. This elevated risk of obesity in PLWH in South Africa is likely due to a confluence of both general considerations and HIV-specific factors. First, South Africa has experienced an accelerated background epidemic of metabolic disease in the general population with a prevalence of overweight and obesity that is nearly equal to that of high-income countries. Additionally, the International Diabetes Federation estimates that approximately 15.5 million adults are living with diabetes in the African Region, and projects it to grow to 41 million by 2045. As part of this background epidemic of metabolic disease, South Africa is also experiencing a nutrition transition, with widespread availability of processed and refined foods as well as sugar-sweetened beverages. Regarding HIV-specific issues, in 2019 the first-line ART regimen for the South African national HIV treatment program transitioned to TLD. TLD is generally very safe and well-tolerated and has a high barrier to HIV resistance but this transition to this regimen has been associated with risk of excess weight gain at the population level. Both clinical trials and observational studies conducted in South Africa have shown substantial increases in body weight in those who are initiating this ART regimen newly and among those who are suppressed and switched, especially women. Given this, there is a growing risk of obesity in PLWH in this context and a need for management strategies to address this increasingly prevalent comorbidity. Preventing the metabolic complications of HIV in South Africa and worldwide requires urgent solutions. To date, obesity management and diabetes prevention have largely consisted of behavioural interventions such as the Diabetes Prevention Program and related lifestyle modification efforts, focused on improving diet and increasing physical activity. However, in the past several years, novel anti-obesity pharmacologic agents such as the glucagon-like peptide-1 receptor agonists (GLP-1 RAs) have shown enormous promise for obesity management and diabetes prevention in people who are HIV-negative (8-10). However, this drug class has a very limited evidence base in PLWH and relatively scant data from sub-Saharan African populations. Currently, liraglutide is the only GLP-1 RA approved for obesity management in South Africa and this protocol proposes to use the drug for its labelled indication of "weight loss in addition to diet and exercise in adults aged 18 and above who have: (1) a BMI of 30 or greater (obese) or (2) a BMI of greater than 27 and less than 30 (overweight) and weight related health problems (such as diabetes, high blood pressure, hypercholesterolemia, or obstructive sleep apnoea). This evidence gap motivates further inquiry into GLP-1 RAs such as liraglutide as one potential approach to obesity management and prevention of diabetes in PLWH who have comorbid obesity in South Africa, with implications for PLWH in other contexts. In this proposal, the investigators seek to further this important area of inquiry by evaluating the acceptability of liraglutide along with lifestyle counselling in PLWH who have obesity and are stable on dolutegravir-based ART in South Africa.
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
TREATMENT
Masking
NONE
Enrollment
40
Dosing regimen: In this study protocol, liraglutide dosing will be implemented as follows: Liraglutide will be started at a dose of 0.6 mg per day. Participants will be taught to use the injection pen and will be observed giving the first injection. The dose will then be increased by 0.6 mg each week to a maximum dosage of 3.0 mg per day at the end of 4 weeks. This corresponds to the following dosing schedule: Week 1: 0.6 mg per day for one week Week 2: 1.2 mg per day for one week Week 3: 1.8 mg per day for one week Week 4: 2.4 mg per day for one week Week 5-12: 3.0 mg per day for 8 weeks Week 13-24: No drug administration
Africa Health Research Institute Clinical Trials Unit
Mtubatuba, South Africa
RECRUITINGProportion of participants who screen and enroll among those approached
This will be expressed in terms of the proportion of participants who attend screening and enrolment visits among the total number who are approached regarding interest in study participation.
Time frame: Measured at screening
Time to reach study enrollment target
Time frame: Measured at enrollment
Study retention rate at 12 weeks
This will be expressed as a proportion of participants who remain in the study after the 12 week "on treatment" period among those enrolled.
Time frame: Measured at Visit 4 at 12 weeks
Study retention rate at 24 weeks
This will be expressed as a proportion of participants who remain in the study after the full 24 weeks of study procedures are completed among those enrolled.
Time frame: Measured at End of Study at 24 weeks
Rate of adherence to treatment over 12 weeks
The investigators will assess volume remaining in the injector pens and provide a percentage of doses per participant that remained unused at the end of the 12-week period on treatment.
Time frame: Measured at Visit 4 at 12 weeks
Embedded qualitative interviews regarding the acceptability of liraglutide for obesity management
This will be open-ended responses to a brief exit interview about acceptability and feasibility.
Time frame: Measured at End of Study at 24 weeks
Incidence of treatment-emergent adverse events as defined in this protocol
The investigators will report incidence of TEAEs up to 24 weeks (12 weeks on + 12 weeks off treatment)
Time frame: From the initiation of treatment until the date of a treatment-emergent adverse event, assessed up to 24 weeks.
Incidence of serious adverse events (SAEs), as defined in this protocol
The investigators will report incidence of SAEs up to 24 weeks (12 weeks on + 12 weeks off treatment)
Time frame: From the initiation of treatment until the date of a serious adverse event, assessed up to 24 weeks.
Change in body weight following 12 weeks on treatment
Body weight will be measured in the study at both enrolment and after 12 weeks on treatment (Visit 4); these will be used to calculate a continuous change in kg.
Time frame: Measured at Visit 4 at 12 weeks
Change in body weight over 24 weeks (12 weeks on + 12 weeks off treatment)
Body weight will be measured in the study at both enrolment and after 24 weeks on treatment (EOS); these will be used to calculate a continuous change in kg.
Time frame: Measured at End of Study at 24 weeks
Change in HbA1c following 12 weeks on treatment
HbA1c will be measured at enrolment and at Visit 4; here investigators will calculate the difference between these measures (in %).
Time frame: Measured at Visit 4 at 12 weeks
Change in HbA1c over 24 weeks (12 weeks on + 12 weeks off treatment)
HbA1c will be measured at enrolment and at EOS; here investigators will calculate the difference between these measures (in %).
Time frame: Measured at End of Study at 24 weeks
Change in fasting plasma glucose following 12 weeks on treatment
Fasting glucose will be measured at enrolment and at Visit 4; investigators will calculate the difference between these measures (in mmol/L).
Time frame: Measured at Visit 4 at 12 weeks
Change in fasting plasma glucose over 24 weeks (12 weeks on + 12 weeks off treatment)
Fasting glucose will be measured at enrolment and at EOS; investigators will calculate the difference between these measures (in mmol/L).
Time frame: Measured at End of Study at 24 weeks
Change in depressive symptoms following 12 weeks on treatment
This will be defined as the difference in depression score per the Patient Health Questionnaire (PHQ-9) at enrolment and Visit 4. The minimum value is 1 and the maximum is 27, where the greater the total score, the greater severity of depression.
Time frame: Measured at Visit 4 at 12 weeks
Change in depressive symptoms over 24 weeks (12 weeks on + 12 weeks off treatment)
This will be defined as the difference in depression score per the Patient Health Questionnaire (PHQ-9) at enrolment and EOS. The minimum value is 1 and the maximum is 27, where the greater the total score, the greater severity of depression.
Time frame: Measured at End of Study at 24 weeks
Change in physical activity level following 12 weeks on treatment
This will be defined as the difference in physical activity expressed in MET-minutes per week, where MET minutes represent the amount of energy expended carrying out physical activity, per the International Physical Activity Questionnaire (IPAQ) at enrolment and Visit 4.
Time frame: Measured at Visit 4 at 12 weeks
Change in physical activity level over 24 weeks (12 weeks on + 12 weeks off treatment)
This will be defined as the difference in physical activity expressed in MET-minutes, where MET minutes represent the amount of energy expended carrying out physical activity, per week per the International Physical Activity Questionnaire (IPAQ) at enrolment and EOS.
Time frame: Measured at End of Study at 24 weeks
Change in dietary habits following 12 weeks on treatment
This will be defined as the difference in total servings of fruits and vegetables, change in frequency of sugar-sweetened beverage intake, and change frequency of fast food intake from enrolment to Visit 4.
Time frame: Measured at Visit 4 at 12 weeks
Change in dietary habits over 24 weeks (12 weeks on + 12 weeks off treatment)
This will be defined as the difference in total servings of fruits and vegetables, change in frequency of sugar-sweetened beverage intake, and change frequency of fast food intake from enrolment to EOS.
Time frame: Measured at End of Study at 24 weeks
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