Orforglipron FDA Approval Status July 2026
Yes. Foundayo (orforglipron) was FDA approved on April 1, 2026. This page leads with the U.S. approval answer, then covers ATTAIN-1 data and the key facts behind the FDA decision.
Update History ▾
June 21, 2026: US-market SEO/AEO refresh — title, meta, H1, and freshness signals aligned to “orforglipron FDA approval status 2026” queries; no regulatory status change.
June 15, 2026: Re-checked FDA approval status against Lilly and FDA sources, updated freshness signals, and tightened the title/meta/subtitle around the U.S. approval answer that is driving current Search Console demand.
May 28, 2026: Added ATTAIN-MAINTAIN switch/maintenance evidence and refreshed answer surfaces after the first post-approval update cycle.
May 25, 2026: Reconciled approval language across verdict, takeaways, FAQ DOM, and schema; refreshed visible freshness signals.
May 17, 2026: Refreshed early post-approval status signals and aligned the page around the U.S. FDA answer.
May 10, 2026: Tightened title to Q&A format (~60 chars) and aligned H1/headline
April 14, 2026: Reframed as the canonical approval-answer page and refreshed freshness signals after the status-page rewrite
April 6, 2026: Updated — FDA approved April 1, 2026 as Foundayo
April 2, 2026: Latest data review and formatting update
Initial publication
Yes. Orforglipron (brand name Foundayo) was FDA approved on April 1, 2026 for chronic weight management in adults with obesity (BMI 30+) or overweight (BMI 27+) with at least one weight-related comorbidity. It is the first non-peptide oral GLP-1 receptor agonist approved for obesity. FDA said the decision landed 50 days after filing under the Commissioner's National Priority Voucher pilot program. For the broader label and program context, see the Foundayo FDA approval deep dive and the 2026 obesity approval tracker.
Scope note: This status page tracks the U.S. FDA answer, core trial evidence, and approval timing only. Prescription approval and RUO supply are separate lanes, and Remy Peptides does not supply Foundayo or prescription GLP-1 medicines.
- Orforglipron (Foundayo) was FDA approved on April 1, 2026, and that remains the current U.S. label status as of July 4, 2026.
- First non-peptide oral GLP-1 agonist approved for obesity — once daily, no food or water restrictions.
- ATTAIN-1: 12.4% weight loss at 72 weeks (17.2 mg dose) vs 2.1% placebo.
- ACHIEVE-3: Beat oral semaglutide on HbA1c and weight loss.
- Fastest NME approval since 2002 — 50 days, under the FDA’s CNPV pilot program.
- ATTAIN-MAINTAIN (Nature Medicine, May 12, 2026): after stopping injectables, oral orforglipron maintained a mean ~75% (post-tirzepatide) / ~79% (post-semaglutide) of prior weight loss at 52 weeks, vs 49%/38% on placebo.
| Item | Status (July 4, 2026) |
|---|---|
| FDA Approval | Approved — April 1, 2026 |
| Brand Name | Foundayo |
| Best Weight-Loss Figure | 12.4% at 72 weeks (17.2 mg approved-label cap); 14.3% at the 36 mg trial dose |
| Developer | Eli Lilly |
| Drug Type | Oral non-peptide GLP-1 receptor agonist |
| Dosing | Once daily, no food/water restrictions |
| Approval Speed | 50 days (fastest NME since 2002) |
| Approved Use | Chronic weight management in adults with obesity or overweight plus at least one weight-related comorbidity |
| FDA Priority Voucher | Granted (Commissioner’s National Priority Voucher) |
| Global Submissions | Filed in 40+ countries |
What Is Orforglipron FDA Approval Status in 2026?
Yes — orforglipron is FDA approved in 2026. Foundayo (orforglipron) received U.S. approval on April 1, 2026 for chronic weight management in adults with obesity or overweight plus at least one weight-related comorbidity. As of July 4, 2026, that remains the current label status; no new FDA action has been posted since approval.
The approval made Foundayo the first non-peptide oral GLP-1 receptor agonist cleared for obesity. FDA said the decision arrived 50 days after filing under the Commissioner’s National Priority Voucher pilot program. For label details and launch context, see the Foundayo FDA approval deep dive.
What Is Orforglipron (Foundayo)?
Orforglipron is Eli Lilly’s once-daily oral non-peptide GLP-1 receptor agonist, now approved for obesity in the United States under the brand name Foundayo. The non-peptide structure is the key differentiator — unlike peptide-based oral GLP-1 drugs such as oral semaglutide, orforglipron does not require fasting before dosing or restrictions on food and water intake after administration. For a detailed comparison of oral GLP-1 compounds, see Oral Obesity Drugs in 2026.
Eli Lilly has already secured the U.S. obesity approval and continues development work in type 2 diabetes. The current U.S. status answer now turns less on launch commentary and more on label scope, post-approval evidence, and how the obesity and diabetes programs continue across the broader development plan. For the label and program specifics, see our Foundayo (orforglipron) FDA approval details.
Lilly positions orforglipron as an oral GLP-1 that eliminates the formulation constraints that have historically limited peptide-based oral drugs. This practical advantage is distinct from mechanism of action — orforglipron activates the same GLP-1 receptor as semaglutide, but delivers it in a structurally different oral format.
What Did the ATTAIN-1 Phase 3 Trial Show?
In August 2025, Eli Lilly reported positive Phase 3 obesity data from the ATTAIN-1 trial. The FDA-approved Foundayo label caps maintenance dosing at 17.2 mg, which delivered approximately 12.4% mean weight loss at 72 weeks; the higher 36 mg trial dose produced approximately 14.3%. The FDA approved orforglipron on April 1, 2026 as Foundayo. It is a once-daily small molecule oral glucagon-like peptide-1 receptor agonist designed to mimic the GLP-1 hormone and activate its receptors throughout the body.
The ATTAIN-1 trial also showed improvements in cardiometabolic risk factors alongside weight reduction. Notably, orforglipron can be taken any time of the day without restrictions on food and water intake, unlike oral semaglutide which requires fasting. With the U.S. obesity approval now secured, the remaining near-term watch points are launch execution, global registrations, and separate type 2 diabetes label expansion.
| Feature | Orforglipron | Wegovy Pill |
|---|---|---|
| Status (April 2026) | Approved as Foundayo (April 1, 2026) | FDA approved; US launched |
| Drug Type | Non-peptide GLP-1 agonist | Peptide-based oral semaglutide |
| Mechanism | GLP-1 receptor agonist | GLP-1 receptor agonist |
| Developer | Eli Lilly | Novo Nordisk |
| Best Weight-Loss Figure | 12.4% at 72 weeks (ATTAIN-1) | 16.6% (OASIS 4, adherence estimand) |
| Dosing Restrictions | None — no food/water restrictions | Empty stomach, limited water, 30-min fast |
ACHIEVE-3: Orforglipron vs Oral Semaglutide
A pivotal head-to-head clinical trial, ACHIEVE-3, compared orforglipron and oral semaglutide in 1,698 participants with type 2 diabetes over 52 weeks, using four treatment arms: orforglipron 12 mg, orforglipron 36 mg, oral semaglutide 7 mg, and oral semaglutide 14 mg. Orforglipron delivered superior blood sugar control compared to oral semaglutide, lowering A1C by 2.2% versus 1.4%. Participants on orforglipron 36 mg lost 19.7 lbs (9.2%) compared to 11.0 lbs (5.3%) with oral semaglutide 14 mg, representing a 73.6% greater relative weight loss.
Orforglipron showed clinically meaningful improvements from baseline across key cardiovascular risk factors, including non-HDL cholesterol, HDL cholesterol, VLDL cholesterol, total cholesterol, systolic blood pressure, and triglycerides. Discontinuation rates due to adverse events were higher for orforglipron (about 9–10%) compared to oral semaglutide (4–5%), mainly due to gastrointestinal symptoms. The most common adverse events included nausea, diarrhea, vomiting, dyspepsia, and decreased appetite. Orforglipron is also being investigated for treating hypertension and obstructive sleep apnea.
The ACHIEVE Phase 3 global clinical development program for orforglipron has enrolled more than 6,000 people with type 2 diabetes. Research suggests tirzepatide may be more effective than orforglipron for both weight loss and blood sugar control. Retatrutide, the triple-receptor agonist, posts among the highest weight-loss figures reported in current obesity trials — see the retatrutide research profile for its mechanism and trial data. The lead investigator for the ACHIEVE-3 trial is based at Texas Southwestern Medical Center.
ATTAIN-MAINTAIN: Maintaining Weight Loss After Injectables
A Phase 3b switch/maintenance trial, ATTAIN-MAINTAIN, was published in Nature Medicine on May 12, 2026. It tested whether patients who stopped an injectable GLP-1 could hold onto their results by switching to oral orforglipron. After discontinuing injectables, orforglipron preserved a mean of approximately 75% of prior weight loss in post-tirzepatide patients and 79% in post-semaglutide patients at 52 weeks, versus 49% and 38% respectively on placebo.
This is the first peer-reviewed evidence that an oral GLP-1 receptor agonist can maintain weight loss after injectable therapy is withdrawn — a key practical question given the documented weight regain seen after stopping injectables. For more on that pattern, see GLP-1 discontinuation and weight regain data.
What Happens Next?
Three developments define the near-term path for orforglipron:
1. U.S. label implementation. The obesity approval is already secured, so the next practical milestone is how the approved label, payer decisions, and prescriber uptake evolve in the United States.
2. Additional label expansion data. The ATTAIN and ACHIEVE programs continue to generate obesity and type 2 diabetes data. Those readouts matter less for the base obesity approval answer now, and more for label expansion, payer positioning, and cross-indication strategy.
3. Competitive positioning. The key research question is now how Foundayo stacks up against oral semaglutide and injectable leaders. Its non-peptide format and no-fasting routine are the clearest differentiators. For a direct efficacy comparison, see Retatrutide vs Orforglipron, and for broader pipeline context use the obesity drug approval tracker.
Why Does This Matter Now?
Orforglipron is the first non-peptide oral GLP-1 agonist approved for obesity — a meaningful distinction from the peptide-based Wegovy pill. The development of orforglipron is the result of extensive drug research, including preclinical pharmacology studies and Phase 3 clinical trials, highlighting the scientific innovation behind its creation.
The practical implications are significant. Small-molecule drug design is reshaping the landscape of obesity and diabetes research. Peptide-based oral drugs require specific dosing conditions — empty stomach, small amounts of water, waiting periods before eating — that affect real-world adherence. A non-peptide oral GLP-1 without those restrictions changes the convenience profile and gives researchers a cleaner comparison point for oral obesity therapies.
Further reading
Our Research Standards
This article cites peer-reviewed studies, FDA filings, and ClinicalTrials.gov data. All claims are cross-referenced against primary sources. We update articles when new trial data or regulatory decisions are published. Read our editorial policy →
- Eli Lilly. Orforglipron Phase 3 obesity results — ATTAIN-1. August 2025. investor.lilly.com
- Eli Lilly. What to know about orforglipron. lilly.com
- Novo Nordisk. FDA approves Wegovy pill (oral semaglutide 25 mg). December 2025. novonordisk.com
- Novo Nordisk. Annual Report 2025: Innovation and therapeutic focus. annualreport.novonordisk.com
- Nature Medicine. ATTAIN-MAINTAIN: oral orforglipron for weight-loss maintenance after injectable GLP-1. May 12, 2026. nature.com