GLP-1 Receptor Agonists in HIV: Addressing Weight Gain Challenges

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Dr Srinivasa reported receiving research grant
funding from Gilead Sciences. (Updated November
13, 2023)
 
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On completion of this activity, learners will be able to:
Implement GLP-1 receptor antagonists (GLP-1RAs) as a
novel therapeutic class for weight loss
Summarize recent studies of GLP-1RA use among
people with HIV
Describe off-target effects of GLP-1RAs, which may be of
potential benefit to the HIV population
 
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Importance of body composition in weight loss
 
Studies of GLP-1RAs in HIV
 
Off target benefits of GLP-1RAs
 
 
 
 
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Weight gain has been associated with ART initiation and generally does not improve with switching ART regimens.
The NA-ACCORD study demonstrated that a
fter 3 yrs of ART: almost 1/5 of those who were normal weight became
overweight and 1/5 of those who were overweight became obese.
The ADVANCE study demonstrated that among ART-treated individuals, women with HIV gain more weight than men
with HIV.
Pooled analysis of 8 RCTs of treatment-naive PWH initiating ART reported a higher weight gain in those receiving INSTI
or TAF-containing regimens than in those receiving TDF, abacavir or zidovudine. 
Dolutegravir and bictegravir
 have been
most consistently implicated with INSTI-associated weight gain
Additional risk factors for weight gain include: low CD4 count, high viral load, black race
 
 
 
 
 
 
 
 
 
 
 
 
 
Godfrey, 
JID
 2019; Koethe, 
Nature Reviews 
2020; Koethe, 
AIDS Res Hum Retro 
2016; Koethe, 
HIV Med 
2015; Sax, 
CID
 2019; Bourgi, 
CID
 2020; Bares, 
J Women Health 
2018
 
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Bares, 
CID
 2023
 
Adjusted Cox Proportional Hazard Models of
Weight Change at Week 48 and Subsequent Clinical
Events Among Participants With 
>
10% Weight Gain
 
 
Participated were included were on any of
the following antiretrovirals:
                
tenofovir disoproxil fumarate
 
emtricitabine
 
lamivudine
 
abacavir
 
efavirenz
 
atazanavir
 
darunavir
 
raltegravir
 
Mean weight gain from 0–48 weeks:
       
 
3.6 kg (SD 7.3)
 
Participants who lost more than 5% of
their baseline weight had a lower risk of
incident metabolic syndrome:
       
 
HR 0.67, 95% CI [0.42, 1.07].
 
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Figure adapted from Cignarelli, 
Front Endo 
2022 and myendoconsult.com
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GLP-1 receptor
agonism
 
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Figure adapted from Cignarelli, 
Front Endo 
2022 and myendoconsult.com
 
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Rubino, 
JAMA
 2022
 
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overweight/obese without DM
(68 weeks)
 
Absolute Mean Weight Change (95% CI):
 
Semaglutide 2.4mg: -15.3 (-17.3 to -13.4)kg
Liraglutide 3.0mg: -6.8 (-8.8 to -4.9)kg
 
 
Participants Achieving >10%, >15%, >20% weight loss:
 
Semaglutide 2.4mg: 70.9%, 55.6%, 38.5%
Liraglutide 3.0mg: 25.6%, 12.0%, 6.0%
 
 
 
-
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Lincoff, 
NEJM
 2023
 
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BMI≥27, Pre-existing CVD, No known DM
 
Mean duration exposure to semaglutide: 34.2±13.7 months
Mean duration follow up: 39.8±9.4 months
 
Primary CV endpoint
(composite death from CV causes, nonfatal MI, or nonfatal
CVA)
 
6.5% in the semaglutide SQ group
    
 
8.0% in the placebo group
 
                *20% risk reduction with semaglutide SQ
 
 
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Mean weight change with semaglutide
50mg PO vs. placebo after 68 weeks:
       -15.1% vs. -2.4%
 
Increased GI adverse effects were
reported in the semaglutide vs. placebo
groups:
       80% vs. 45%
 
A trend towards a higher reduction in
hsCRP was seen in semaglutide vs.
placebo treated groups:
      -57% vs. -14%
 
 
 
 
 
 
Knop 
Lancet 
2023
 
*Semaglutide 50mg--currently 
under investigation
 
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BMI>30 or BMI>27 + weight related complications.
No known DM
 
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*Not for use in type 1 diabetes
 
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Injections site reactions
Risk of hypoglycemia is low (may occur when used in combo with sulfonylureas,
insulin, glinides)
Gastrointestinal: nausea, vomiting, diarrhea (most common, reported in 10-50%)
Symptoms may lessen with duration of therapy and dose titration
Pancreatitis
Use is contraindicated if prior history of pancreatitis
Biliary disease: cholelithiasis, cholecystitis
Acute renal insufficiency (infrequent, usually in setting of GI symptoms)
Medullary thyroid cancer (black box warning)
Use is contraindicated with personal/family history
 
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Several meta-analyses indicated that GLP-1RAs did not increase the risk of malignancy
 
In 2021, STEP 3 and STEP 4 trials reported the incidence of malignancy in obese adults as 1.1%
(6/535) in the semaglutide group and 0.4% (1/268) in the control group
 
Yang et al. explored the association of GLP1RA and neoplasms by mining the FDA Adverse
Event Reporting System (FAERS) database
 
 
GLP-1RA did not cause a disproportionate increase in all tumor cases.
 
 
Significant signals were detected between GLP-1RA and certain tumors--including thyroid
 
cancers, pancreatic neoplasms, and neuroendocrine tumors
 
 
 
Cao, 2019; Liu, 2019; Elashoff, 2011; Wadden,2021; Rubino, 2021; Yang, 
Frontiers Pharm
 2022
 
 
GLP-1 and glucose-dependent insulinotropic polypeptide
(GIP) agonist
Currently 
approved
 for 
use in 
typ
e 2 diabetes
Recently 
approved
 (11/2023) for use in 
obesity
Greater reduction in A1c than GLP-1RA alone, HbA1c dec 2-
2.5%
Mean body weight loss 7-11 kg
 
 
GLP-1, GIP, glucagon receptor agonist
Currently 
under investigation 
for use in 
typ
e 2 diabetes
Greater reduction in A1c than GLP-1RA alone, HbA1c dec
2%
Mean body weight loss 17.2 kg
 
 
Retatrutide
: Triple action agonist
Tirzepatide
: Dual action ‘twincretin’
 
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Brandt, 
J Int Med
 2018; Rosenstock, 
Lancet
 2023; Nogueiras, 
Nature Metab
 2023
 
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Adapted from Depres 2012; Godfrey 
JID
 2019
*Ideal Clinical
Strategy:
 
Reduce VAT
Preserve SAT
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*Ideal Clinical
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Reduce VAT
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Erlandson, 
Top Antiviral Med
 2020; Oliveria, 
Euro J Clinic Nut 2020;
 Wilding, JES 2021
 
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In the STEP 1 trial (semaglutide SQ weekly), an exploratory analysis showed:
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owever, the proportion of total lean body mass relative to total body mass increased by 3.0%-points.
I
ncreasing improvement in lean body mass:fat mass ratio was seen with semaglutide with increasing weight
loss.
 
*Ideal Clinical Strategy:
Preserve Lean Body Mass
 
 
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Retrospective study assessing GLP-1RA
initiation on weight and HbA1c among
persons with HIV, n=35 (LSU)
 
Baseline Characteristics
o
Mean BMI (SD): 35.7 (9.8) kg/m2
o
Mean HbA1c (SD): 9.5 (2.6) %
o
INSTI use: 89%
o
Concurrent use of metformin:
57%
 
 
 
 
 
 
 
Tauhid, 
OFID 
2022 Dec; 9(Suppl 2): ofac492.518/ ID Week 2022
 
66% lost weight (n=23)
 
9% stable weight (n=3)
 
26% gained weight (n=9)
 
Breakdown of weight changes with GLP-1RA use
 
 
Mean duration GLP-1RA use (SD): 20.6 (14.0) months
9/20 (45%) PWH with duration use >12 months lost >5% body weight
 
 
 
 
 
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Retrospective study assessing the impact of GLP-1RA initiation on weight, BMI and HbA1c, n=225 (UCSD)
Preparations included: semaglutide (60%--53% SQ/7% PO), liraglutide (3%), dulaglutide (31%), tirzepatide (6%)
41% achieved maximal dosing; mean duration on GLP-1RA :15.4 (4.5-26.4) months
 
 
 
 
 
 
 
 
 
 
Adapted from slides Nguyen, 
ID Week
 2023
 
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53 PWH (24%) had >5% weight loss
 
41 PWH (18%) transitioned from the obese to overweight category
 
 Factors associated with >5% weight loss
 
−Higher baseline BMI: OR 1.07 (1.02-1.3)
 
−Longer duration of treatment (months): OR 1.04 (1.01-1.07)
 
The use of dulaglutide was associated with decreased odds of achieving >5%
weight loss [OR 0.33 (0.17-0.66)] as compared to the other GLP-1 RAs.
 
 
 
 
 
Adapted from slides Nguyen, ID Week 2023
 
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Retrospective study assessing the impact of GLP-1RAs on metabolic outcomes in individuals with type 2
diabetes mellitus and HIV (DM+HIV) compared to DM without HIV (DM), n=45 (University of Cincinnati)
 
 
 
 
 
 
 
 
 
Conclusion: PWH and DM had significantly greater weight loss compared to people with DM alone.
 
*significantly different
 
Lloyd, IAS 2023: https://programme.ias2023.org/Abstract/Abstract/?abstractid=3399
 
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Randomized, double-blind, placebo-controlled study of semaglutide SQ vs. placebo (full max dose 24 weeks) among
PWH with BMI≥25 and increased waist circumference, n=108 (Case Western/Medical University of South Carolina)
Primary Endpoint: VAT by CT; Other endpoints: weight, SAT by CT, DXA for total fat, limb fat, trunk fat, lean mass
 
 
 
 
 
 
 
 
 
Adapted from slides McComsey, ID Week 2023
 
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For every 1% lean mass reduction, the semaglutide group lost 2.4% fat mass and the placebo group gained 2.0% fat mass
No improvement in pericardial or liver fat
Overall excellent adherence, study-related AEs similar between groups; only 3 AEs lead to discontinuation
 
 
 
 
 
 
 
 
Adapted from slides McComsey, ID Week 2023
 
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Persons with BMI ≥30kg/m2 or BMI ≥27kg/m2 and hypertension, dyslipidemia or
type 2 diabetes mellitus randomized to semaglutide+diet/exercise vs.
diet/exercise (open label)
 
Outcome: 
Effect on total body weight
Other measures: 
immune function, inflammation, gut microbiome, glucose and
lipid metabolism
 
 
Clinicaltrials.gov
 
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GLP-1RAs are not expected to pose significant drug interactions via their metabolism (degraded
by endopeptidases)
 
GLP-1RAs are known to inhibit gastric acid secretion and to delay gastric emptying
Treatment with liraglutide reduced gastric acid secretion by 18.7% and prolonged gastric emptying time by 25 min
.
 
The dissolution and absorption of atazanavir and oral rilpivirine may be affected by elevated
gastric pH.
With such a small difference in gastric acid secretion and emptying time though, GLP-1RAs are thought to have a
minimal effect.
 
 A separated intake of orally administered GLP-1RA by 4 hrs before oral rilpivirine, and by 2–4 hrs
before atazanavir intake, has been recommended
 
Zino, 
HIV Med 
2023; Quast, 
Diabetes Care 
2020;
 
Cope,
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2019
 
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RCT conducted at 96 sites enrolling patients
with/without DM, BMI>25, and biopsy-
confirmed non-alcoholic steatohepatitis
(NASH) were treated with semaglutide 0.1-
0.4mg vs. placebo over 72 weeks. (n=320)
 
Treatment with semaglutide 0.4mg resulted in
a significantly higher percentage of patients
with NASH resolution vs placebo:
       59 vs. 17%
 
Mean percent weight loss was 13% in the
semaglutide 0.4-mg group and 1% in the
placebo group
 
 
 
Newsome, 
NEJM 
2021
 
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Semaglutide 2.4mg SQ vs. placebo over 52
wks
 
Among those with HFpEF and obesity,
semaglutide led to:
       -larger reductions in symptoms and
        physical limitations
       -greater improvements in exercise function
       -greater weight loss
 
Study was not powered to evaluate clinical
events, such as hospitalization from HF
 
 
 
 
Kosiborod, 
NEJM
 2023
 
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GLP-1 is also produced in the nucleus tractus solitarius of the brain stem and is released as a
neurotransmitter
 
GLP-1 receptors are expressed in brain regions involved in reward and addiction and its stimulation
modulates dopamine (decreases dopamine)
 
Preclinical research 
has identified potent reductions in substance use and attenuation of drug-seeking
behavior with several different GLP-1RAs, mainly in rodent models
Suppresses motivation to consume alcohol, alcohol-seeking behaviors, relapse drinking and withdrawal symptoms
Suppresses nicotine intake and reward
Decreases some opioid seeking and withdrawal symptoms
Decrease cocaine and amphetamine reward, decrease cocaine intake
 
Preliminary clinical studies of alcohol use disorder suggest that GLP-1RAs reduce alcohol consumption in a
subset of individuals with obesity
 
**
Clinical studies are needed 
to assess the use of GLP-1RAs in addictive disorders.
 
 
Jerlhag
, Front Pharm 
2023; 
Hernandez,
 Neuropyschpharm 
2018; Hernandez, 
Addict Biol
, 2019; Egecioglu, 
PLOS one
, 2013; Egecioglu, 
Psychneuroendo
, 2013; Marty, 
Front
Neuro
, 2020; Vallof, 
Addict Biol, 
2015; Klausen 
JCI Inight, 
2022; Tuesta, 
Nat Neurosci 
2017; Douton, 
Behav Pharm
 2021; Zhang, 
Neuorpsychopharm,
 2020
 
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Are these chronic medications?
Is there reaccumulation of fat mass after GLP-1RA discontinuation?
Will the amount of lean mass lost have significant clinical contributions to frailty?
Will weight loss secondary to GLP-1RA use reduce metabolic risk among PWH?
Are there cardiovascular, kidney, and liver benefits associated with GLP-1RA use
among PWH?
Will GLPs demonstrate efficacy in addiction disorders in human studies?
Will there be increased insurance coverage for weight loss medications?
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GLP-1 receptor agonists offer a promising therapeutic approach for weight management in individuals with HIV. Weight gain is a common issue, exacerbated by antiretroviral therapy, and can lead to metabolic risks. This presentation by Dr. Suman Srinivasa discusses the potential of GLP-1 receptor agonists, recent studies on their use in HIV patients, and their off-target benefits. The session highlights the importance of addressing weight gain in the HIV population and explores the role of GLP-1RAs in managing body composition for weight loss.


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  1. Weighing in on GLP-1 Receptor Agonists for People With HIV Suman Srinivasa, MD, MS Massachusetts General Hospital Harvard Medical School Boston, MA

  2. Financial Relationships With Ineligible Companies (Formerly Described as Commercial Interests by the ACCME) Within the Last 2 Years Dr Srinivasa reported receiving research grant funding from Gilead Sciences. (Updated November 13, 2023) Slide 2

  3. Learning Objectives On completion of this activity, learners will be able to: Implement GLP-1 receptor antagonists (GLP-1RAs) as a novel therapeutic class for weight loss Summarize recent studies of GLP-1RA use among people with HIV Describe off-target effects of GLP-1RAs, which may be of potential benefit to the HIV population Slide 3

  4. Outline Weight gain among persons with HIV (PWH) Therapeutic potential of GLP-1 receptor agonists (GLP-1RAs) in diabetes and weight loss Importance of body composition in weight loss Studies of GLP-1RAs in HIV Off target benefits of GLP-1RAs Slide 4

  5. Weight gain in the era of contemporary ART Weight gain has been associated with ART initiation and generally does not improve with switching ART regimens. The NA-ACCORD study demonstrated that after 3 yrs of ART: almost 1/5 of those who were normal weight became overweight and 1/5 of those who were overweight became obese. The ADVANCE study demonstrated that among ART-treated individuals, women with HIV gain more weight than men with HIV. Pooled analysis of 8 RCTs of treatment-naive PWH initiating ART reported a higher weight gain in those receiving INSTI or TAF-containing regimens than in those receiving TDF, abacavir or zidovudine. Dolutegravir and bictegravir have been most consistently implicated with INSTI-associated weight gain Additional risk factors for weight gain include: low CD4 count, high viral load, black race Slide 5 Godfrey, JID 2019; Koethe, Nature Reviews 2020; Koethe, AIDS Res Hum Retro 2016; Koethe, HIV Med 2015; Sax, CID 2019; Bourgi, CID 2020; Bares, J Women Health 2018

  6. Weight gain after ART initiation and metabolic risk Participated were included were on any of the following antiretrovirals: tenofovir disoproxil fumarate emtricitabine lamivudine abacavir efavirenz atazanavir darunavir raltegravir Adjusted Cox Proportional Hazard Models of Weight Change at Week 48 and Subsequent Clinical Events Among Participants With 10% Weight Gain Clinical Event HR (95% CI) 2.01 (1.30, 3.08) 2.02 (1.55, 2.62) 1.54 (1.22, 1.95) Diabetes mellitus (n=130) Metabolic syndrome (n=360) Cardiometabolic event (n=424) Mean weight gain from 0 48 weeks: 3.6 kg (SD 7.3) Participants who lost more than 5% of their baseline weight had a lower risk of incident metabolic syndrome: HR 0.67, 95% CI [0.42, 1.07]. Slide 6 Bares, CID 2023

  7. GLP-1 receptor agonists (GLP-1RAs): Mechanism of Action Suppress appetite Slow gastric emptying Stimulate insulin secretion Inhibit glucagon release GLP-1 receptor agonism Decrease glucose production Slide 7 Figure adapted from Cignarelli, Front Endo 2022 and myendoconsult.com

  8. Broad Potential Benefits of GLP-1RAs Cardioprotection Increase cardiac output Improve endothelial function Increase glucose uptake Increase diuresis Increase natriuresis Decrease hepatic steatosis Increase glucose uptake Decrease lipogenesis Increase lipolysis Slide 8 Figure adapted from Cignarelli, Front Endo 2022 and myendoconsult.com

  9. GLP-1RAs: Preparations and FDA Indications Name Route Frequency Max Dosing FDA Indication Weight Loss SQ weekly 2.4mg Semaglutide (Wegovy) Semaglutide (Ozempic) Semaglutide (Rybelsus) Liraglutide (Saxenda) Liraglutide (Victoza) Dulaglutide (Trulicity) Exenatide ER (Bydureon) Exenatide (Byetta) Lixisenatide (Adylxin) SQ weekly 2.0mg Type 2 Diabetes GLP-1RA Long acting PO (30min before eating) SQ daily 14mg Type 2 Diabetes daily 3.0mg Weight Loss SQ daily 1.8mg Type 2 Diabetes SQ weekly 4.5mg Type 2 Diabetes SQ weekly 2.0mg Type 2 Diabetes SQ BID 10mcg Type 2 Diabetes GLP-1RA Short acting SQ daily 20mcg Type 2 Diabetes Slide 9

  10. GLP-1RAs: Efficacy on HbA1c/co-morbidities among individuals with DM Name Route Frequency Max Dosing Reduction in HbA1c% points Cardiovascular mortality benefit in existing/ high risk CVD Nephropathy benefit SQ weekly 2.0mg -1.5 to -2.0 Semaglutide (Ozempic) Semaglutide (Rybelsus) Liraglutide (Victoza) Dulaglutide (Trulicity) Exenatide ER (Bydureon) Exenatide (Byetta) Lixisenatide (Adylxin) PO daily 14mg -0.7 to -2.0 SQ daily 1.8mg -0.8 to -1.5 SQ weekly 4.5mg -1.0 to -1.5 SQ weekly 2.0mg -1.5 to -1.6 SQ BID 10mcg -1.0 SQ daily 20mcg -0.8 to -1.0 Slide 10

  11. STEP8 Trial: Efficacy on weight loss Results from the STEP 8 Trial (n=338) overweight/obese without DM (68 weeks) 0 Absolute Mean Weight Change (95% CI): -2 -1.9% Mean Weight Change (%) -4 Semaglutide 2.4mg: -15.3 (-17.3 to -13.4)kg Liraglutide 3.0mg: -6.8 (-8.8 to -4.9)kg -6 -6.4% -8 -10 Participants Achieving >10%, >15%, >20% weight loss: -12 -14 Semaglutide 2.4mg: 70.9%, 55.6%, 38.5% Liraglutide 3.0mg: 25.6%, 12.0%, 6.0% -16 -15.8% -18 Semaglutide (n=126) Liraglutide (n=127) Placebo (n=85) Slide 11 Rubino, JAMA 2022

  12. SELECT Trial: CV outcomes in obesity without DM Results from the SELECT Trial (n=17,604) BMI 27, Pre-existing CVD, No known DM Mean duration exposure to semaglutide: 34.2 13.7 months Mean duration follow up: 39.8 9.4 months Primary CV endpoint (composite death from CV causes, nonfatal MI, or nonfatal CVA) 6.5% in the semaglutide SQ group 8.0% in the placebo group *20% risk reduction with semaglutide SQ Slide 12 Lincoff, NEJM 2023

  13. OASIS-1 Trial: Oral Semaglutide 50mg for weight loss Results from the OASIS-1 Trial (n=338) BMI>30 or BMI>27 + weight related complications. No known DM Mean weight change with semaglutide 50mg PO vs. placebo after 68 weeks: -15.1% vs. -2.4% Increased GI adverse effects were reported in the semaglutide vs. placebo groups: 80% vs. 45% A trend towards a higher reduction in hsCRP was seen in semaglutide vs. placebo treated groups: -57% vs. -14% *Semaglutide 50mg--currently under investigation Slide 13 Knop Lancet 2023

  14. GLP-1RA: Current Clinical Indications for Patients Clinical Indications for GLP-1RAs With established atherosclerotic CVD (ASCVD) or kidney disease Type 2 Diabetes Mellitus* Without established ASCVD or kidney disease and HbA1c>9% Without established ASCVD or kidney disease and HbA1c 9%, but weight gain is a concern Obesity BMI 30 kg/m2 BMI of 27 to 29.9 kg/m2with weight-related comorbidities + not met weight-loss goals (5% loss of total body weight over 3-6 months) with comprehensive lifestyle intervention alone *Not for use in type 1 diabetes Slide 14

  15. GLP-1RA: Potential Adverse Side Effects Injections site reactions Risk of hypoglycemia is low (may occur when used in combo with sulfonylureas, insulin, glinides) Gastrointestinal: nausea, vomiting, diarrhea (most common, reported in 10-50%) Symptoms may lessen with duration of therapy and dose titration Pancreatitis Use is contraindicated if prior history of pancreatitis Biliary disease: cholelithiasis, cholecystitis Acute renal insufficiency (infrequent, usually in setting of GI symptoms) Medullary thyroid cancer (black box warning) Use is contraindicated with personal/family history Slide 15

  16. GLP-1RAs: More about Potential Malignancy Risk Several meta-analyses indicated that GLP-1RAs did not increase the risk of malignancy In 2021, STEP 3 and STEP 4 trials reported the incidence of malignancy in obese adults as 1.1% (6/535) in the semaglutide group and 0.4% (1/268) in the control group Yang et al. explored the association of GLP1RA and neoplasms by mining the FDA Adverse Event Reporting System (FAERS) database GLP-1RA did not cause a disproportionate increase in all tumor cases. Significant signals were detected between GLP-1RA and certain tumors--including thyroid cancers, pancreatic neoplasms, and neuroendocrine tumors Slide 16 Cao, 2019; Liu, 2019; Elashoff, 2011; Wadden,2021; Rubino, 2021; Yang, Frontiers Pharm 2022

  17. Combination GLP-1RAs: Twincretins and beyond Role of Gut Hormone Co-agonists and Potential Synergistic Effects GIP Glucagon increase appetite yes Appetite Suppression Slow Gastric Emptying Stimulate Insulin Secretion Glucagon Inhibition Decrease Glucose Production Other no effect yes yes yes Increase glucagon Indirect effects through glucagon -- -- Increase glucose production Lipolysis, increased energy expenditure, may activate GLP-1R Slide 17 Brandt, J Int Med 2018; Rosenstock, Lancet 2023; Nogueiras, Nature Metab 2023

  18. Discerning Phenotypes with Excess Adiposity in HIV SAT VAT *Ideal Clinical Strategy: *Ideal Clinical Strategy: Reduce VAT Preserve SAT Reduce VAT Reduce SAT Growth hormone releasing hormone analogue (tesamorelin) ? GLP1 receptor agonism Slide 18 Adapted from Depres 2012; Godfrey JID 2019

  19. Weight Loss with GLP-1As: fat vs. lean mass With the use of contemporary ART, the HIV population is aging and the prevalence of frailty is increased. Sarcopenia risk may be 6-fold higher among PWH when compared to matched individuals without HIV. In addition, sarcopenia may occur at a younger age among PWH. In the STEP 1 trial (semaglutide SQ weekly), an exploratory analysis showed: %change body weight from baseline to week 68 was: -15.0% with semaglutide vs -3.6% with placebo. In the semaglutide group: Relative total fat mass decreased -19.3% Relative regional visceral fat mass decreased -27.4% However, the proportion of total lean body mass relative to total body mass increased by 3.0%-points. Increasing improvement in lean body mass:fat mass ratio was seen with semaglutide with increasing weight loss. Relative total lean body mass decreased -9.7% *Ideal Clinical Strategy: Preserve Lean Body Mass Slide 19 Erlandson, Top Antiviral Med 2020; Oliveria, Euro J Clinic Nut 2020; Wilding, JES 2021

  20. Do people living with HIV lose weight on GLP-1RA therapy? Breakdown of weight changes with GLP-1RA use Retrospective study assessing GLP-1RA initiation on weight and HbA1c among persons with HIV, n=35 (LSU) 100% 26% gained weight (n=9) 90% 80% 9% stable weight (n=3) Baseline Characteristics Mean BMI (SD): 35.7 (9.8) kg/m2 Mean HbA1c (SD): 9.5 (2.6) % INSTI use: 89% Concurrent use of metformin: 57% 70% o 60% 50% o 66% lost weight (n=23) 40% o 30% o 20% 10% 0% Mean duration GLP-1RA use (SD): 20.6 (14.0) months 9/20 (45%) PWH with duration use >12 months lost >5% body weight Slide 20 Tauhid, OFID 2022 Dec; 9(Suppl 2): ofac492.518/ ID Week 2022

  21. GLP-1 RAs Promote Weight Loss Among People With HIV Retrospective study assessing the impact of GLP-1RA initiation on weight, BMI and HbA1c, n=225 (UCSD) Preparations included: semaglutide (60%--53% SQ/7% PO), liraglutide (3%), dulaglutide (31%), tirzepatide (6%) 41% achieved maximal dosing; mean duration on GLP-1RA :15.4 (4.5-26.4) months Slide 21 Adapted from slides Nguyen, ID Week 2023

  22. GLP-1 RAs Promote Weight Loss Among People With HIV 53 PWH (24%) had >5% weight loss 41 PWH (18%) transitioned from the obese to overweight category Factors associated with >5% weight loss Higher baseline BMI: OR 1.07 (1.02-1.3) Longer duration of treatment (months): OR 1.04 (1.01-1.07) The use of dulaglutide was associated with decreased odds of achieving >5% weight loss [OR 0.33 (0.17-0.66)] as compared to the other GLP-1 RAs. Slide 22 Adapted from slides Nguyen, ID Week 2023

  23. Impact of GLP-1RAs on body weight in patients with type 2 diabetes and HIV Retrospective study assessing the impact of GLP-1RAs on metabolic outcomes in individuals with type 2 diabetes mellitus and HIV (DM+HIV) compared to DM without HIV (DM), n=45 (University of Cincinnati) DM+HIV (n=15) -10.4 (12.5) kg -8.0 (10.0) % 60% -1.3 (2.4) DM (n=30) -1.7 (8.5) kg -1.5 (6.8) % 33% -0.5 (2.0) Mean Change Weight (SD) * Mean %Change Weight (SD) * Achieved >5% weight loss Mean Change HbA1c (SD) *significantly different Conclusion: PWH and DM had significantly greater weight loss compared to people with DM alone. Slide 23 Lloyd, IAS 2023: https://programme.ias2023.org/Abstract/Abstract/?abstractid=3399

  24. Effects of Semaglutide in HIV-Associated Lipohypertrophy Randomized, double-blind, placebo-controlled study of semaglutide SQ vs. placebo (full max dose 24 weeks) among PWH with BMI 25 and increased waist circumference, n=108 (Case Western/Medical University of South Carolina) Primary Endpoint: VAT by CT; Other endpoints: weight, SAT by CT, DXA for total fat, limb fat, trunk fat, lean mass Slide 24 Adapted from slides McComsey, ID Week 2023

  25. Effects of Semaglutide in HIV-Associated Lipohypertrophy For every 1% lean mass reduction, the semaglutide group lost 2.4% fat mass and the placebo group gained 2.0% fat mass No improvement in pericardial or liver fat Overall excellent adherence, study-related AEs similar between groups; only 3 AEs lead to discontinuation Slide 25 Adapted from slides McComsey, ID Week 2023

  26. Other Ongoing Studies of GLP-1RAs in HIV Semaglutide's Efficacy in Achieving Weight Loss for Those With HIV (SWIFT) University College Dublin Persons with BMI 30kg/m2 or BMI 27kg/m2 and hypertension, dyslipidemia or type 2 diabetes mellitus randomized to semaglutide+diet/exercise vs. diet/exercise (open label) Outcome: Effect on total body weight Other measures: immune function, inflammation, gut microbiome, glucose and lipid metabolism Slide 26 Clinicaltrials.gov

  27. Potential Interactions between GLP-1RAs and ARTs GLP-1RAs are not expected to pose significant drug interactions via their metabolism (degraded by endopeptidases) GLP-1RAs are known to inhibit gastric acid secretion and to delay gastric emptying Treatment with liraglutide reduced gastric acid secretion by 18.7% and prolonged gastric emptying time by 25 min. The dissolution and absorption of atazanavir and oral rilpivirine may be affected by elevated gastric pH. With such a small difference in gastric acid secretion and emptying time though, GLP-1RAs are thought to have a minimal effect. A separated intake of orally administered GLP-1RA by 4 hrs before oral rilpivirine, and by 2 4 hrs before atazanavir intake, has been recommended Slide 27 Zino, HIV Med 2023; Quast, Diabetes Care 2020;Cope, Pharmacotherapy 2019

  28. Semaglutide in NASH RCT conducted at 96 sites enrolling patients with/without DM, BMI>25, and biopsy- confirmed non-alcoholic steatohepatitis (NASH) were treated with semaglutide 0.1- 0.4mg vs. placebo over 72 weeks. (n=320) Treatment with semaglutide 0.4mg resulted in a significantly higher percentage of patients with NASH resolution vs placebo: 59 vs. 17% Mean percent weight loss was 13% in the semaglutide 0.4-mg group and 1% in the placebo group Slide 28 Newsome, NEJM 2021

  29. Step-HFpEF: Semaglutide in HFpEF and Obesity Results from the Step-HFpEF Trial (n=338) Heart failure with preserved ejection fraction (HFpEF), BMI 30 Semaglutide 2.4mg SQ vs. placebo over 52 wks Among those with HFpEF and obesity, semaglutide led to: -larger reductions in symptoms and physical limitations -greater improvements in exercise function -greater weight loss Study was not powered to evaluate clinical events, such as hospitalization from HF Slide 29 Kosiborod, NEJM 2023

  30. The role GLP-1RA in addictive disorders GLP-1 is also produced in the nucleus tractus solitarius of the brain stem and is released as a neurotransmitter GLP-1 receptors are expressed in brain regions involved in reward and addiction and its stimulation modulates dopamine (decreases dopamine) Preclinical research has identified potent reductions in substance use and attenuation of drug-seeking behavior with several different GLP-1RAs, mainly in rodent models Suppresses motivation to consume alcohol, alcohol-seeking behaviors, relapse drinking and withdrawal symptoms Suppresses nicotine intake and reward Decreases some opioid seeking and withdrawal symptoms Decrease cocaine and amphetamine reward, decrease cocaine intake Preliminary clinical studies of alcohol use disorder suggest that GLP-1RAs reduce alcohol consumption in a subset of individuals with obesity **Clinical studies are needed to assess the use of GLP-1RAs in addictive disorders. Jerlhag, Front Pharm 2023; Hernandez, Neuropyschpharm 2018; Hernandez, Addict Biol, 2019; Egecioglu, PLOS one, 2013; Egecioglu, Psychneuroendo, 2013; Marty, Front Neuro, 2020; Vallof, Addict Biol, 2015; Klausen JCI Inight, 2022; Tuesta, Nat Neurosci 2017; Douton, Behav Pharm 2021; Zhang, Neuorpsychopharm, 2020 Slide 30

  31. Clinical Questions with GLP-1RAs Are these chronic medications? Is there reaccumulation of fat mass after GLP-1RA discontinuation? Will the amount of lean mass lost have significant clinical contributions to frailty? Will weight loss secondary to GLP-1RA use reduce metabolic risk among PWH? Are there cardiovascular, kidney, and liver benefits associated with GLP-1RA use among PWH? Will GLPs demonstrate efficacy in addiction disorders in human studies? Will there be increased insurance coverage for weight loss medications? Slide 31

  32. Q and A Session

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