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TL;DR — Verdict

Zepbound (tirzepatide) remains the only obesity drug FDA-approved for obstructive sleep apnea. The approval came on December 20, 2024, based on SURMOUNT-OSA. Retatrutide remains investigational, but Lilly’s June 6, 2026 full-data release reported that the nested TRIUMPH-1 moderate-to-severe OSA basket reduced apnea-hypopnea index by up to 36.1 events per hour (60.6%). A separate dedicated Phase 3 OSA study remains active; these trial findings do not constitute an approved OSA indication.

Which Obesity Drugs Are Approved for Sleep Apnea? Is Ozempic One of Them?

One. As of May 23, 2026, Zepbound (tirzepatide) by Eli Lilly is the only obesity drug with an FDA-approved indication for obstructive sleep apnea. The FDA granted the approval on December 20, 2024, for the treatment of moderate-to-severe OSA in adults with obesity. This made Zepbound the first prescription medicine ever approved specifically for OSA.

Before this approval, the standard of care for OSA was continuous positive airway pressure (CPAP) therapy. No prescription drug had demonstrated sufficient efficacy in a controlled trial to earn an FDA indication. Zepbound changed that.

No other GLP-1 receptor agonist, dual agonist, or triple agonist has an FDA-approved OSA indication. Semaglutide (Wegovy/Ozempic) is not approved for sleep apnea. CagriSema and survodutide have no OSA-specific trial data. Retatrutide has reported a nested TRIUMPH-1 moderate-to-severe OSA basket, while a separate dedicated Phase 3 study continues; those findings remain investigational.

What Did the SURMOUNT-OSA Trial Show?

The SURMOUNT-OSA trial was a randomized, double-blind, placebo-controlled Phase 3 study evaluating tirzepatide in adults with moderate-to-severe obstructive sleep apnea and obesity, typically reflected in elevated body mass index. The trial had two arms: one with patients not using CPAP at baseline, and one with patients using CPAP.

The headline results were significant. Tirzepatide produced approximately 18% body weight loss and reduced the apnea-hypopnea index (AHI) by 51–52% versus baseline. AHI is the primary clinical measure of sleep apnea severity — it counts the number of apnea and hypopnea events per hour of sleep and is also used to track OSA severity over time.

Perhaps more notable: 42–50% of patients achieved disease remission, defined as an AHI below 5 events per hour. An AHI below 5 is clinically considered normal — meaning nearly half the patients in the trial no longer met the diagnostic threshold for sleep apnea, and reductions in AHI generally help improve symptoms.

These results were strong enough for the FDA to grant a new indication — the first time any drug had cleared that bar for OSA.

A pre-specified secondary analysis published in Nature Medicine on January 15, 2026 added a layer the original readout had only hinted at. Tirzepatide produced greater alleviation of cardiometabolic risk factors than placebo, and mediation analysis showed that improvements in OSA-specific metrics independently contributed to drops in hsCRP, HOMA-IR, and triglycerides over and above the weight-loss effect alone. The practical reading: treating the airway and the metabolic disease together is what captures the full cardiometabolic benefit — neither alone reproduces the combination. Source: Nature Medicine secondary analysis of SURMOUNT-OSA, PMID 41540105.

Lilly Approval Announcement Data
Endpoint Result
Breathing Interruptions At least 25 fewer per hour of sleep
Symptom Resolution Up to 50% no longer met OSA symptom criteria after 1 year
Detailed SURMOUNT-OSA Results
Endpoint Result
AHI Reduction Up to 62.8%
Disease Resolution Up to 51.5% of participants met criteria

Is Retatrutide Being Studied for Sleep Apnea?

Yes — on two tracks. The TRIUMPH-1 master trial included a nested moderate-to-severe OSA basket, and Lilly also lists an active dedicated Phase 3 study of retatrutide in moderate-to-severe obstructive sleep apnea as a standalone expanded-indication program.

Lilly’s June 6, 2026 release reported that the TRIUMPH-1 OSA basket reduced apnea-hypopnea index by up to 36.1 events per hour (60.6%) from a baseline of 58.6 events per hour. The dedicated OSA study has not yet reported. Given retatrutide’s triple-agonist mechanism (GLP-1 + GIP + glucagon receptor), researchers are watching whether the result is replicated across the broader OSA program. Retatrutide remains investigational and is not approved for OSA.

In Phase 2, retatrutide demonstrated up to 24.2% weight loss at 48 weeks. The December 2025 TRIUMPH-4 Phase 3 readout reported 28.7% at 12 mg over 68 weeks, and on May 21, 2026 the pivotal TRIUMPH-1 obesity trial reported 28.3% mean weight loss at 80 weeks on 12 mg (n=2,339) and up to 30.3% at 104 weeks in a BMI ≥35 extension. The reported TRIUMPH-1 OSA basket now provides a direct trial signal; the dedicated OSA study must still establish whether that result is replicated. For the trial schedules used in the TRIUMPH program, see the retatrutide dosage guide. For the published adverse-event data, see our retatrutide side effects profile.

Why Do Weight Loss Medications Improve Sleep Apnea?

Approximately 70% of patients with obstructive sleep apnea have excess weight or obesity, and obesity is the primary risk factor for sleep apnea, driving roughly 60% of cases. The connection is mechanical: excess adipose tissue around the upper airway increases pharyngeal collapsibility during sleep, leading to repeated airway obstruction — the hallmark of OSA.

Even a 10% weight gain can raise the risk of developing sleep apnea by about six-fold.

Clinical data consistently shows that 10–15% weight reduction can significantly reduce AHI scores, may lead to remission in some mild-to-moderate cases, and GLP-1 agonists are being studied as a way to help patients achieve it. The mechanism is straightforward: reducing fat deposits around the pharynx and tongue base decreases the mechanical load on the airway, reducing the frequency and severity of obstructive events and helping improve OSA symptoms. GLP-1 medications such as semaglutide and tirzepatide can also produce significant weight loss linked to lower AHI and symptom improvement.

This is why obesity drugs that produce meaningful weight loss are better understood as one treatment option for treating obstructive sleep apnea indirectly, rather than as direct cures, with possible benefit in some patients with metabolic disorders also extending through lower systemic inflammation. However, the relationship is not perfectly linear — some patients with significant weight loss still have residual OSA, which is why the FDA requires controlled trial evidence rather than extrapolating from weight-loss data alone. For a wider look at the obesity drug landscape, see our best obesity drug 2026 comparison.

PAP therapy, including continuous positive airway pressure (CPAP), remains the standard of care, but real-world adherence is approximately 50%. Many patients cannot tolerate the device, struggle with a CPAP machine, use it inconsistently, or abandon it entirely. Patients should not stop CPAP or other positive airway pressure treatment without medical supervision. Weight loss that reduces airway obstruction may lessen poor sleep and improve deep sleep. This adherence gap is what makes pharmacological alternatives like Zepbound clinically significant — not as a CPAP replacement, but as a complement or alternative for patients who cannot maintain CPAP therapy.

2026 Pooled Estimate — GLP-1 Class Effect on AHI

Beyond any single trial, an April 24, 2026 meta-analysis in Sleep & Breathing pooled 4 randomised controlled trials of GLP-1-based therapies in obstructive sleep apnea. The pooled estimate was a mean AHI reduction of −13.89 events/hour (95% CI −22.86 to −4.92, p<0.01), alongside 4–6 mmHg reductions in systolic blood pressure. This is the first class-level synthesis of the OSA-and-incretin literature, and it puts a number on the effect across studies rather than within a single program.

The pooled figure sits below SURMOUNT-OSA's headline 51–52% relative AHI reduction because it averages across trials, doses, and baseline severities — and an absolute events/hour change is a different metric from a relative percentage. Read together, the single-trial and pooled data both point in the same direction: meaningful AHI reduction tracking weight loss, plus a blood-pressure co-benefit. These are research findings on prescription medicines, reported here as scientific context — Remy Peptides supplies research-grade peptides for in-vitro laboratory use only.

Obesity Drugs & Sleep Apnea — Pipeline Comparison
Drug OSA Indication Trial AHI Reduction Weight Loss Status
Zepbound (tirzepatide) FDA approved (Dec 2024) SURMOUNT-OSA 51–52% vs baseline ~18% Approved & available
Retatrutide Pre-specified endpoint + dedicated OSA Phase 3 TRIUMPH-1 OSA basket + dedicated OSA Phase 3 Up to −36.1 events/hour (−60.6%) in TRIUMPH-1 OSA basket 28.3% at 80wk in TRIUMPH-1 obesity pivotal (May 21, 2026); up to 30.3% at 104wk BMI ≥35 ext Investigational; dedicated study ongoing
Semaglutide (Wegovy) Not approved for OSA No OSA trial No controlled data ~16% (STEP trials) Approved for obesity only
CagriSema No OSA indication No OSA trial No data ~22.7% (REDEFINE 2) No OSA program
Survodutide No OSA indication No OSA trial No data ~18.7% (Phase 2) No OSA program

Do GLP-1 Drugs Improve Sleep Apnea Without an OSA Approval?

Some observational and retrospective data suggest that GLP-1 receptor agonists may improve sleep apnea markers secondary to weight loss. This is mechanistically plausible — any drug that produces 10–15%+ weight loss should reduce AHI in obese patients with OSA.

However, observational data is not the same as a controlled trial with an OSA-specific primary endpoint. The FDA approved Zepbound for OSA based on SURMOUNT-OSA — a purpose-designed, randomized, placebo-controlled study that measured AHI reduction as a primary outcome. No other GLP-1 agonist has this level of evidence for OSA.

Semaglutide (Wegovy/Ozempic) is one of the most commonly prescribed weight loss medications for obesity, but Novo Nordisk has not announced an OSA-specific clinical trial. Without controlled data, any claims about semaglutide treating sleep apnea are extrapolation, not evidence. It does not have FDA approval for treating OSA specifically and should not be presented as an approved OSA treatment. Healthcare providers may observe improvement in some OSA patients taking semaglutide, but this does not constitute an approved indication. For a comparison of adverse event profiles across these compounds, see our Ozempic vs Mounjaro vs Wegovy side effects review.

What Should Researchers Watch Next?

Three developments will shape the OSA treatment landscape in 2026 and beyond:

1. Dedicated OSA Phase 3 readout for retatrutide. The nested TRIUMPH-1 OSA basket has reported an AHI reduction of up to 36.1 events per hour (60.6%). Lilly’s separate Phase 3 study in moderate-to-severe OSA remains active and will show whether that signal is replicated. Retatrutide remains investigational; no approval outcome should be inferred before regulatory review.

2. Real-world Zepbound OSA data. Post-approval studies and real-world evidence will clarify how Zepbound performs outside controlled trial conditions — particularly on CPAP discontinuation rates, long-term AHI durability, and changes in OSA severity over time.

3. Whether competitors pursue OSA indications. Novo Nordisk (semaglutide), Amgen, and Zealand/Roche have not announced OSA-focused trials, but semaglutide and peers can be viewed more broadly as anti-obesity medications being evaluated for possible future OSA programs. If retatrutide’s dedicated OSA study confirms the TRIUMPH-1 basket signal, competitive pressure may drive additional OSA programs. Until then, Zepbound remains the only approved pharmacological option. Explore the full landscape of anti-obesity medications in our best obesity drug 2026 guide.

Weight management will remain central to future OSA research even as more drugs are studied.

Zepbound (tirzepatide) by Eli Lilly is the only obesity drug FDA-approved for obstructive sleep apnea. The approval was granted on December 20, 2024, for moderate-to-severe OSA in adults with obesity. It is the first prescription medicine ever approved specifically for OSA.
Zepbound does not cure sleep apnea in most patients, but it can produce disease remission. In SURMOUNT-OSA, 42–50% of patients achieved an AHI below 5 events per hour — the clinical threshold for remission. Results depend on continued treatment and individual response.
Wegovy (semaglutide) is not FDA-approved for obstructive sleep apnea. Semaglutide may help improve symptoms indirectly through weight loss, but no controlled trial has established semaglutide as an OSA treatment. Zepbound is the only obesity drug with an approved OSA indication.
Yes. TRIUMPH-1 included a nested moderate-to-severe OSA basket and reported an apnea-hypopnea-index reduction of up to 36.1 events per hour (60.6%) in June 2026. Lilly also lists a dedicated Phase 3 OSA study. Retatrutide remains investigational and is not approved for OSA.
Clinical data indicates that 10–15% body weight loss can significantly reduce AHI scores. In SURMOUNT-OSA, tirzepatide produced ~18% weight loss and reduced AHI by 51–52% versus baseline. A 2026 pooled meta-analysis of 4 RCTs (Sleep & Breathing, April 24, 2026) put the class-level effect at a mean AHI reduction of −13.89 events/hour (95% CI −22.86 to −4.92, p<0.01), with 4–6 mmHg systolic blood-pressure reductions. The degree of improvement generally correlates with the magnitude of weight loss.
Yes. Zepbound is approved as a treatment for OSA, not as a replacement for CPAP. The SURMOUNT-OSA trial included an arm with patients using CPAP alongside tirzepatide. Clinicians may prescribe Zepbound as an adjunct to CPAP or as an alternative for patients who cannot tolerate CPAP therapy, but any change should be guided by a sleep medicine specialist.

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The Remy Peptides Editorial Board reviews research articles covering GLP-1 receptor agonists, triple agonists, and the obesity drug pipeline. Its review spans peptide analytical chemistry, HPLC purity validation, and clinical trial data interpretation.

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References & Citations
  1. U.S. Food & Drug Administration. FDA approves first medication for obstructive sleep apnea. December 20, 2024. fda.gov
  2. Eli Lilly. Zepbound (tirzepatide) approved for moderate-to-severe obstructive sleep apnea in adults with obesity. December 2024. investor.lilly.com
  3. Eli Lilly. Lilly’s tirzepatide reduced obstructive sleep apnea severity — detailed SURMOUNT-OSA results. investor.lilly.com
  4. Zepbound. Sleep apnea information page. zepbound.lilly.com
  5. Malhotra A, et al. Tirzepatide for the treatment of obstructive sleep apnea and obesity (SURMOUNT-OSA). N Engl J Med. 2024. nejm.org
  6. Eli Lilly. Retatrutide Phase 3 clinical program — TRIUMPH trials. clinicaltrials.gov
  7. Eli Lilly. Full TRIUMPH-1 and TRANSCEND-T2D-1 Phase 3 results, including the TRIUMPH-1 OSA basket. June 6, 2026. investor.lilly.com
  8. Jastreboff AM, et al. Triple-hormone-receptor agonist retatrutide for obesity — a Phase 2 trial. N Engl J Med. 2023;389(6):514–526. nejm.org
  9. American Academy of Sleep Medicine. Obstructive Sleep Apnea — Overview. aasm.org
  10. GLP-1 receptor agonists for obstructive sleep apnea: a meta-analysis of 4 RCTs (mean AHI reduction −13.89 events/hour, 95% CI −22.86 to −4.92, p<0.01; 4–6 mmHg systolic BP reduction). Sleep & Breathing. April 24, 2026. doi:10.1007/s11325-026-03681-4. link.springer.com