Could a Dolutegravir-Based Antiretroviral Therapy Lead to Clinical Obesity? A Retrospective Cohort Study Conducted at Hawassa University Comprehensive Specialized Hospital in Hawassa, Sidama, Ethiopia

Background As of April 2019, the dolutegravir (DTG)-based regimen is replacing the efavirenz-based regimen in Ethiopia, mainly due to its superiority in viral load suppression. However, there is a growing concern about this medication-based regimen, the most serious of which is excessive weight gain. In this study, we looked at weight gain disparities among human immunodeficiency virus/acquired immunodeficiency syndrome (HIV/AIDS) patients on antiretroviral therapy (ART) who have been shifted to tenofovir/lamivudine/dolutegravir (TLD) from a tenofovir/lamivudine/efavirenz (TLE)-based regimen versus those who are maintained on a tenofovir/lamivudine/efavirenz-based regimen. Methods A facility-based retrospective observational cohort study was conducted in pursuit of weight change disparities between tenofovir/lamivudine/dolutegravir and tenofovir/lamivudine/efavirenz-based regimens among patients who have attained optimal viral suppression at Hawassa University Comprehensive Specialized Hospital antiretroviral clinic. Chi-square and logistic regression were used as appropriate using an SPSS version 21 program to test the association of specific variables to outcome variables, and a P value <0.05 was considered statistically significant. Results This study included 422 patients, 211 of whom were switched from tenofovir/lamivudine/efavirenz to tenofovir/lamivudine/dolutegravir and the remaining were who kept on a tenofovir/lamivudine/efavirenz-based regimen. Patients on a tenofovir/lamivudine/dolutegravir-based regimen had a mean weight gain of 3.88 ± 2.021 kg in one year compared to those on TLE (2.26 ± 2.39). In a bivariate analysis, being male was found to protect against unwanted weight gain at COR 0.531 (0.345, 0.816). A current CD4 count of more than 500 has been found to be strongly correlated with weight gain in multivariate analysis at an AOR of 0.315 (0.188, 0.527) at a P value ≤0.001. Conclusion According to this study, tenofovir/lamivudine/dolutegravir (TLD)-based antiretroviral medication (ART) users are more likely to gain weight, and clinicians should advise them of the risks of weight gain as well as cost-effective ways to prevent weight gain linked to poor health outcomes in these patients. Future investigations should confirm the findings of this study, and more research into the effects of weight gain in these people is required.


Introduction
Since the discovery of highly active antiretroviral therapy (HAART), the treatment of human immunodeficiency virus/acquired immunodeficiency syndrome (HIV/AIDS) has been revolutionized, as evidenced by a drastically reduced rate of death from HIV/AIDS and a decrease in the occurrence of opportunistic infections [1][2][3].
Dolutegravir, a recently added integrase inhibitor antiretroviral drug, impairs HIV integrase function and thus prevents HIV insertion into the host cell's DNA [1,[4][5][6]. It is not uncommon to see a short-term weight gain in HIV/ AIDS patients who begin ART, particularly in those with a pretreatment low body mass index (BMI) and significantly low CD4 at the time of treatment. [7][8][9]. To put it another way, the weight gain following ART initiation was once one of the tools used to assess ART success [7,10,11].
Given the significantly increased prevalence of noncommunicable diseases, weight gain reevaluation has exhibited a significant association of weight gain with metabolic syndrome, imperiling HIV/AIDS care yet further [12][13][14]. A multisite study conducted in the United States of America found that more than half of HIV/AIDS patients on ART for more than three years had clinical obesity, putting them at risk of developing noncommunicable diseases [4,9,15]. According to a 2019 WHO meta-analysis, an absolute increase in body weight of 3-5 kg has been ascertained among patients on a DTG-based regimen at about 48 weeks after ART initiation. As a result, individuals on a DTG-based regimen are strongly advised to abide by weight-loss specific suggestions, such as regular exercise [1-4, 9, 16].
Since the first ART, there has been a constant need for the development of better drugs in all areas of pharmacology [3,12]. As of April 2019, Ethiopia has begun to implement a new ART regimen as a preferred first-line ART based on WHO recommendations, which is a step in the right direction [13]. Instead of the well-known efavirenz-based ART regimen, a dolutegravir-based ART regimen is being used. e main reasons why this new medication was preferred over the existing medication were the good safety profile, rapid suppression of viral load, and high genetic variability for resistance, to mention a few [1,4,5]. Implementing the recommended regimen will be critical in the fight against HIV/AIDS, though, since evidence-based advice will dramatically improve coverage and achieve the desired treatment outcome. Despite these advantages, there is growing concern about this new regimen, with many patients complaining of unintended weight gain [1,3,6,14,17,18]. e decrease in morbidity and mortality among people living with the human immunodeficiency virus (PLWHA) has been linked to a rise in noncommunicable disease rates, notably metabolic disorders. In recent studies, virologically suppressed people living with HIV (PLWH) who transitioned from old antiretroviral medication (ART) to newer integrase strand transfer inhibitor (INSTI)-based regimens gained weight [1,19,20]. Given the potentially serious public health effects that could threaten the national widespread use of dolutegravir, it will be vital to follow the impact of the DTG-based ART regimen on clinical obesity. Because there are no data on these findings in the study area, we looked for significant weight change differences between patients who switched to a DTG-based regimen (TLD group) and those who stayed on an efavirenz-based regimen (TLE group).

Study Design and Setting.
A retrospective observational cohort study was conducted at Hawassa University's comprehensive specialized hospital (HUCSH), which is located in Hawassa city, the capital of the SNNPR and Sidama region, 273 kilometers south of Addis Ababa. e boundaries of Hawassa city are defined by Lake Hawassa in the east, Oromia in the west, Wondogenet woreda in the north and east, and Shebadeno in the south. e city government covers a total of 157.2 square meters. Eight subcities and 32 kebeles make up the total area of km 2 . Two public hospitals and nine public health centers are also part of the city government. e Regional Health Bureau built Hawassa University's comprehensive specialized hospital (HUCSH) 16 years ago. e hospital was built with the intention of serving a population of 3.5-5 million people, but it currently serves the whole Sidama, SNNPR, and Oromia regions (HUSCH human recourse office). It is a tertiary hospital with more than 20 departments that provide both clinical and academic services. e ART clinic is one of the clinical services, and there are now roughly 2620 PLWHA on first-line ART, with nearly 55% of them on DTG-based regimens.
e research was carried out from January to March 2021, G.C.

Source Population.
e source population was all adult HIV patients who were on ART in HUCSH ART clinic.

Study Population.
All HIV patients who have been shifted from TLE to TLD and those who have been maintained on TLE have been on a specified regimen for at least one year.

Eligibility Criteria
2.3.1. Inclusion Criteria. All adult AIDS patients who have been on TLE-based regimen for at least 1 year and obtained optimal viral suppression and adult patients who had been shifted to TLD from TLE-based ART regimen, and stayed on TLD for at least 1 year and attained optimal viral load suppression in HURCSH ART clinic.

Exclusion
Criteria. AIDS patients who are on ART for less than one year, any patient with deliberate or unintended overdose, age less than 18, weight less than 26 kg, on secondline regimen, patients with unsuppressed viral load have been excluded from the study.

Sample Size.
e required sample size was estimated using Epi Info, version 7, statistical software, with the following assumptions: 95% confidence interval, 80% power, and a 1 : 1 ratio of exposed (DTG-based ART regimen) to nonexposed (TLE-based ART regimen). 422 was the final sample size.

Sampling Method.
e simple random sampling method was used to collect the data by reviewing the cards for bodyweight in kilograms (kg), body mass index (BMI), and other pertinent information based on the prepared tools.

Data Collection Procedure and Source of Data.
Standardized survey questionnaires were prepared to collect relevant data by reviewing the patient's charts. e charts of adults who were on ART in the HUCSH ART clinic were reviewed based on the prepared standardized questionnaires. Data collection was performed by trained general practitioners who were actively working at HUCSH ART clinic. Two medical doctors who were from another health facility were working as supervisors, and close supervision of the data collectors was being undertaken by the supervisors.

Data Processing, Analysis, and Data Quality
Assurance. e collected data were being cross-checked daily for the accuracy of the information. Chi-square and relatives logistic regression were used as appropriate using an SPSS version 21 program to test the association of specific variables to outcome variables, and a P value <0.05 was considered statistically significant. Results were presented using texts, tables, pie charts, and bar graphs were interpreted by looking at the proportion in percent and odds ratios with 95% confidence interval. A weight change greater than 5% was taken as a significant weight gain (clinical obesity) [1,[21][22][23]. A properly designed data collection instrument was used and pretested on 21 patients who were enrolled at the Adare General Hospital ART clinic. A few amendments were made to the flow of the questionnaire. For analysis, the collected data were entered, cleaned, and managed with SPSS version 22.

Results
In this study, we evaluated 422 HIV/AIDS patients, equally divided into TLD-and TLE-based groups, with a 100% response rate. Across both study groups, the proportions of age, gender, marital status, and educational status were virtually identical (see Table 1). e majority of the TLD-based groups with more than 5% weight gain were in WHO stage 2 when they started ART, whereas the TLE groups were in WHO stage 3. Lower CD4 counts at the start of ART were found to be associated with significant weight gain in both groups when compared to high CD4 counts, whereas viral load has the opposite relationship (Table 2). e majority of same-day ART initiations were reported in those with a weight gain greater than 5%, particularly in the TLD group, and the least weight gain was observed in those who began ART within one month of knowing their status (see Table 3).
Despite the fact that a higher proportion of the TLD group is on TB treatment, the median provision of CPT and INH remained nearly comparable between the two groups. Metformin was the most commonly prescribed medication for illnesses other than HIV/AIDS in both groups, followed by combinations of Lasix plus digoxin plus spironolactone. Patients on a TLD-based regimen had a mean weight gain of 3.88 ± 2.021 kg in one year compared to those on TLE (2.26 ± 2.39) (see Table 4).
e TLD group that gained significant weight gain of 5% or more experienced the longest duration of weight gain within 48 weeks of ART initiation (67.0 percent). However, between the two groups, the least weight change was observed within 12 weeks of ART initiation. Diabetes mellitus was the most commonly diagnosed medical disease in both groups, with a higher prevalence in the TLE group (28.6 percent vs. 15.9 percent, respectively). e majority of the study groups experienced adverse drug reactions (ADRs) during treatment, with peripheral neuropathy symptoms such as numbness, tingling, and pain being the most common (in about 21.1 percent of TLD and 10.2 percent of TLE). e advancement of ADR was reported mostly within 12 weeks and above in the TLD group, but within 4 weeks in the TLE analog.
In a bivariate analysis, being male was found to protect against unwanted weight gain at COR 0.531 (0.345, 0.816), whereas having an initial viral load of more than 1000 at the start of ART and starting on TLD were found to be risk factors for unwanted weight gain at COR 3.258 (1.943, 5.466), and COR 2.055 (1.390, 3.039), respectively, at a P value less than or equal to 0.2. e multivariate analysis in this study revealed that a current CD4 count greater than 500 is significantly associated with weight gain with an AOR of 0.315 (0.188, 0.527) at a P value of ≤0.001 (see Table 5).

Discussions
In this study, we evaluated 422 HIV/AIDS patients, equally divided into TLD-and TLE-based groups, with a 100% response rate. Across both study groups, the proportions of age, gender, marital status, and educational status were virtually identical. e majority of the TLD-based group was at WHO stage 2 when they began ART, whereas the TLE group was at WHO stage 3. One of the criteria for switching patients from the TLE to the TLD regimen is long-term viral suppression, which has something to do with the WHO clinical stage [3,18]. e TLE group reported the majority of same-day ART initiation (20.6 percent), while the TLD group had a higher proportion of those who started ART within one week of learning their status. Meticulous workup is required prior to initiating ART, despite the fact that early initiation is the AIDS Research and Treatment avocation at the moment, particularly as the regimen shifts from TLE-based to TLD-based [1,3,18].
Patients on a TLD-based regimen had a mean weight gain of 3.88 ± 2.02 kg in one year compared to those on TLE (2.26 ± 2.39). Because TLD has a faster viral suppression rate than TLE, the former group will gain more weight, in addition to the class-specific weight gain of integrase inhibitors [24][25][26][27][28][29][30][31]. is is almost identical to the study conducted by

AIDS Research and Treatment
Kassem et al. [6], Phillips et al. [16], Jamison et al. [32], and Phillips et al. [33]. e WHO recommendation in its latest update, 2019, also warns of the possibility of excessive weight gain of about 3-5 kg in DTG-based regimens. erefore, our study's findings will be supported further by the WHO recommendation in its latest update [3,4]. One of the possible mechanisms for DTG-associated weight gain has been proposed as a decrease in energy expenditure following the rapid reduction of viral load following the initiation of a DTG-based regimen [1,2,16].
In both groups, diabetes mellitus was the most commonly diagnosed medical condition, particularly in the TLE group (28.6 percent and 15.9 percent, respectively). is could be due to the alarmingly high prevalence of diabetes mellitus in the general population [13,34]. Metformin was the most commonly prescribed medication for non-AIDS medical indications in this study. is is most likely due to current trends of rising noncommunicable disease prevalence, such as diabetes mellitus, among HIV/AIDS patients in particular, and the general population in general. As a result, it is critical to strictly monitor the patient's serum blood glucose as DTG is reported [3,18,35].
e multivariate analysis in this study revealed that a current CD4 count greater than 500 is significantly associated with weight gain with an AOR of 0.315 (0.188, 0.527) at a P value of ≤0.001. e literature indicates a short-term weight gain in HIV/AIDS patients who begin ART, particularly those with a low pretreatment BMI and significantly low CD4 at the time of ART initiation [7][8][9]. As a result, we recommend this population's careful interpretation of weight gain, as not all weight gain is harmful to one's health.

AIDS Research and Treatment
In general, DTG-based ART has been shown to increase HIV/AIDS patients' morbidity and mortality by increasing the likelihood of clinical obesity, and as a consequence, metabolic syndrome. As a result, keeping a watch out for clinical obesity and intervening early is advised.

The Strength and Limitations
5.1. Strength. As far as we know, this is the first study of its kind (there is no single study conducted in our country on this specific topic). It also compares two groups of patients, with the results aiding clinicians in alerting their patients as early as possible before the onset of metabolic syndrome as a consequence of clinical obesity.

Limitations.
ere are limitations to this research. e fact that this is a retrospective study has its own set of drawbacks, as does the fact that it is limited to a particular hospital. Other individuals on non-efavirenz-based regimens were not included in the study. We believe that more research should be conducted, and that the study findings presented in this report should be considered with care.

Conclusions
According to this study, tenofovir/lamivudine/dolutegravir (TLD)-based antiretroviral medication (ART) users are more likely to gain weight, and clinicians should advise them on the risks of weight gain as well as cost-effective ways to prevent weight gain linked to poor health outcomes in these patients. Future investigations should confirm the findings of this study, and more research into the effects of weight gain in these people is required.

Data Availability
Additional data can be available from the correspondent author up on reasonable request.

Ethical Approval
A letter of cooperation for approval to conduct the study was obtained from the Hawassa University Comprehensive Specialized Hospital (HUCSH) Institutional Review Board (IRB). e information was then collected secretly to protect the patients' privacy. Consent e information was gathered by reviewing the patient's chart; obtaining written consent from the patient is not required. However, they are routinely informed on admission or at the initial visit to the hospital, as the hospital is a tertiary hospital, whose role is research and development, to name a few.

Conflicts of Interest
e authors declare that there are no conflicts of interest regarding the publication of this paper.