My Dashboard
Courses
Articles Evidence Reviews Practice Updates Cases News Presentations
About Us
My Dashboard
Drug Monograph

Oral Semaglutide (Rybelsus)

semaglutide tablets co-formulated with SNAC absorption enhancer

GLP-1 Receptor Agonist · Oral · FDA Approved September 2019
Pharmacokinetic Profile
Half-Life
~1 week
Metabolism
Proteolysis + fatty acid beta-oxidation (not CYP-dependent)
Protein Binding
>99% (albumin)
Bioavailability
~0.8% (SNAC-enhanced gastric absorption)
Steady State
4–5 weeks
Clinical Information
Drug Class
GLP-1 Receptor Agonist
Available Doses
R1: 3, 7, 14 mg; R2: 1.5, 4, 9 mg
Route
Oral, once daily (empty stomach, morning)
Renal Adjustment
None required
Hepatic Adjustment
None required
Pregnancy
Not recommended; discontinue ≥2 months before planned pregnancy
Lactation
Not recommended (SNAC in breast milk)
Schedule / Legal Status
Rx only (non-controlled)
Generic Available
No
Black Box Warning
Thyroid C-cell tumors (rodents)
Rx

Indications

IndicationApproved PopulationTherapy TypeStatus
Type 2 diabetes mellitus — glycemic controlAdults (≥18 years)Monotherapy or combinationFDA Approved
Cardiovascular risk reduction in T2DM — reduce MACE (CV death, nonfatal MI, nonfatal stroke) in adults at high CV riskAdults with T2DM + established ASCVD and/or CKDAdjunct to standard of careFDA Approved (Oct 2025)

Oral semaglutide is the first and only GLP-1 receptor agonist available in a pill form, approved as an adjunct to diet and exercise for glycemic management in adult type 2 diabetes. In October 2025, the FDA expanded the label to include cardiovascular risk reduction based on the SOUL trial, which demonstrated a 14% reduction in major adverse cardiovascular events among patients with type 2 diabetes and established atherosclerotic cardiovascular disease and/or chronic kidney disease. Oral semaglutide is not indicated for type 1 diabetes and is not a substitute for insulin in insulin-requiring patients.

Off-Label Uses

Weight management in overweight/obese patients with T2DM: Oral semaglutide consistently produces 3–5 kg weight loss in clinical trials. Although injectable semaglutide (Wegovy) carries the formal obesity indication, oral semaglutide may be used off-label when patients prefer an oral route. Evidence quality: High (consistent body weight secondary endpoints across PIONEER program).

Dose

Dosing

Two Formulations — Not Interchangeable on a mg-per-mg Basis

As of December 2024, Rybelsus is available in two formulations (R1 and R2) with different tablet strengths. They may not be used simultaneously, and switching between them requires following specific guidance (see below). Both formulations use a 30-day initiation dose that is not effective for glycemic control.

Formulation R1 (Original) — 3 mg, 7 mg, 14 mg

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
T2DM — glycemic control (new start)3 mg QD × 30 days7 mg QD14 mg QD3 mg is initiation only — not therapeutic
Uptitrate to 14 mg after day 61 if additional control needed
T2DM — add-on to metformin, SU, or insulin3 mg QD × 30 days7–14 mg QD14 mg QDConsider SU or insulin dose reduction to lower hypoglycemia risk
Same titration schedule regardless of background therapy
T2DM with high CV risk — MACE reduction3 mg QD × 30 days14 mg QD14 mg QDSOUL trial used 14 mg maintenance dose
Target 14 mg for CV indication; MACE reduction demonstrated at this dose

Formulation R2 (Newer) — 1.5 mg, 4 mg, 9 mg

Clinical ScenarioStarting DoseMaintenance DoseMaximum DoseNotes
T2DM — glycemic control (new start)1.5 mg QD × 30 days4 mg QD9 mg QD1.5 mg is initiation only — not therapeutic
Uptitrate to 9 mg after day 61 if additional control needed

Formulation Switching Equivalence

R1 DoseEquivalent R2 DoseNotes
7 mg QD4 mg QDDo not switch during initiation phase (days 1–30); start the new formulation the day after stopping the prior one
14 mg QD9 mg QDEquivalent exposure at steady state; switching permitted after completing the 30-day initiation phase
Clinical Pearl: Strict Administration Requirements

Oral semaglutide must be taken on an empty stomach in the morning with no more than 4 ounces (120 mL) of plain water. Patients must then wait at least 30 minutes before eating, drinking other beverages, or taking other oral medications. Tablets must be swallowed whole — never split, crushed, or chewed. Failure to follow these instructions dramatically reduces absorption (bioavailability drops from ~0.8% to essentially zero with food). If a dose is missed, skip it and resume the next morning.

PK

Pharmacology

Mechanism of Action

Semaglutide is a long-acting GLP-1 analog with 94% structural homology to native human GLP-1. It selectively binds to and activates the GLP-1 receptor, stimulating glucose-dependent insulin secretion from pancreatic beta cells while simultaneously suppressing inappropriately elevated glucagon release. This dual hormonal action lowers both fasting and postprandial blood glucose in an inherently glucose-dependent manner, conferring a low intrinsic hypoglycemia risk when used as monotherapy. Semaglutide also delays gastric emptying, promotes satiety, and reduces appetite and caloric intake, contributing to clinically meaningful weight loss. The oral formulation uses salcaprozate sodium (SNAC), a small fatty acid derivative that locally increases gastric pH beneath the tablet and transiently enhances transcellular permeability of the gastric epithelium to facilitate peptide absorption. Once absorbed, semaglutide behaves identically to the subcutaneous form.

ADME Profile

ParameterValueClinical Implication
AbsorptionGastric (SNAC-mediated); Tmax ~1 h oral; bioavailability ~0.8%; absorption nearly abolished by food or excess waterStrict fasting administration is essential; take with ≤120 mL water, wait 30 min before eating or other oral meds
DistributionExtensive albumin binding (>99%); apparent Vd ~12.5 L (primarily vascular compartment)Albumin binding prolongs half-life to ~1 week despite daily oral dosing; plasma levels steady-state in 4–5 weeks
MetabolismProteolytic cleavage of peptide backbone + sequential beta-oxidation of C18 fatty di-acid side chain; not organ-specific; no CYP450 involvementNo dose adjustments for hepatic or renal impairment; very low drug interaction potential via metabolic pathways
Eliminationt½ ~1 week; primary excretion via urine and feces; ~3% of absorbed dose excreted as intact semaglutide in urineLong half-life supports once-daily dosing despite low bioavailability; requires ≥2-month washout before planned pregnancy
SE

Side Effects

≥10% Very Common
Adverse EffectIncidenceClinical Note
Nausea11% (7 mg); 20% (14 mg)Dose-related (vs 6% placebo); most common during dose escalation; usually self-limiting over 4–8 weeks
Abdominal pain10% (7 mg); 11% (14 mg)Versus 4% placebo; typically epigastric; rarely requires discontinuation
1–10% Common
Adverse EffectIncidenceClinical Note
Diarrhea9% (7 mg); 10% (14 mg)Versus 4% placebo; related to GLP-1 effects on GI motility
Decreased appetite6% (7 mg); 9% (14 mg)Versus 1% placebo; pharmacological effect contributing to weight loss; may be beneficial
Vomiting6% (7 mg); 8% (14 mg)Versus 3% placebo; primarily during dose escalation; can contribute to dehydration and AKI
Constipation6% (7 mg); 5% (14 mg)Versus 2% placebo; related to delayed gastric emptying
Dyspepsia0.6–3%Abdominal distension, flatulence, eructation, and GERD each reported at 1–3%
Serious Serious (Regardless of Frequency)
Adverse EffectEstimated FrequencyTypical OnsetRequired Action
Acute pancreatitis0.1 events/100 pt-yearsAny time; may include necrotizing or hemorrhagic formsDiscontinue immediately; hospitalize; do not rechallenge; fatal cases reported (postmarketing)
Acute kidney injuryRare (postmarketing)Often during dose escalation with GI-related dehydrationRehydrate; monitor renal function; some cases required hemodialysis; counsel on adequate fluid intake
Diabetic retinopathy complications4.2% (vs 3.8% comparator)Early in treatment; associated with rapid HbA1c improvementMonitor patients with baseline retinopathy; particularly those with proliferative retinopathy or macular edema
Cholelithiasis / cholecystitis1.0–1.1%Months into therapy; GLP-1 class effectGallbladder imaging if symptoms develop; surgical referral if indicated; SOUL: cholecystitis 1.1% vs 0.7% placebo
Anaphylaxis / angioedemaVery rare (postmarketing)Any time during treatmentDiscontinue permanently; emergency management; contraindicated on rechallenge
Pulmonary aspiration (peri-procedural)Rare (postmarketing)During general anesthesia or deep sedationInstruct patients to inform anesthesia providers; GLP-1 class-wide warning added Nov 2024; residual gastric contents despite standard fasting
Ileus / intestinal obstructionVery rare (postmarketing)Any time during treatmentHospitalize; supportive management; discontinue semaglutide
Discontinuation Discontinuation Rates
Placebo-Controlled Trials (GI-related discontinuation)
4–8% vs 1% placebo
7 mg: 4%; 14 mg: 8% discontinued due to GI adverse reactions; nausea and vomiting most common causes
SOUL Trial (Median ~4 years)
15.5% vs 11.6% placebo
AE-related discontinuation; mainly gastrointestinal disorders and infections
Managing GI Side Effects

Gastrointestinal adverse effects are the hallmark tolerability limitation of oral semaglutide. In pooled placebo-controlled trials, any GI adverse reaction occurred in 41% of patients on 14 mg, 32% on 7 mg, and 21% on placebo. Severe GI events were reported in 2.0% (14 mg), 0.6% (7 mg), and 0.3% (placebo). The 30-day initiation dose (3 mg for R1, 1.5 mg for R2) exists solely to improve GI tolerability. Most nausea and vomiting occur during dose escalation and diminish as patients reach steady state. Counselling patients to eat smaller, more frequent meals, avoid high-fat foods, and stay well hydrated can reduce symptom burden. If GI effects are intolerable at 14 mg (R1) or 9 mg (R2), maintaining the lower maintenance dose (7 mg or 4 mg) is an appropriate strategy. Monitor for signs of dehydration, as GI-related volume depletion can precipitate acute kidney injury.

Laboratory Changes

Amylase: Mean increases of 10–13%. Lipase: Mean increases of 30–34%. These pancreatic enzyme elevations are commonly observed with GLP-1 receptor agonists and do not, by themselves, indicate pancreatitis. Clinical correlation is essential. Heart rate: Mean increase of 1–3 bpm; no change with placebo.

Int

Drug Interactions

Oral semaglutide is not metabolized by CYP450 enzymes, so it has no direct metabolic interactions with most drugs. However, its ability to delay gastric emptying can alter the absorption kinetics of co-administered oral medications. SNAC itself does not affect the pharmacokinetics of other oral drugs. The primary interaction concern is pharmacodynamic (additive hypoglycemia with insulin or secretagogues) and pharmacokinetic via altered GI transit.

MajorInsulin
MechanismAdditive glucose-lowering via complementary pathways
EffectIncreased hypoglycemia risk; plasma glucose <54 mg/dL in up to 30% when combined with insulin
ManagementConsider reducing insulin dose when initiating oral semaglutide; monitor blood glucose closely
FDA PI
MajorSulfonylureas (e.g., glimepiride, glipizide)
MechanismAdditive insulin secretion stimulation
EffectIncreased hypoglycemia risk including severe episodes
ManagementConsider reducing sulfonylurea dose at initiation; educate on hypoglycemia symptoms
FDA PI
ModerateLevothyroxine
MechanismDelayed gastric emptying increases levothyroxine absorption time and total exposure
Effect33% increase in levothyroxine exposure (AUC) in drug interaction study (90% CI: 1.25–1.42)
ManagementMonitor TSH more frequently when initiating or titrating oral semaglutide; adjust levothyroxine dose as needed; follow strict 30-min post-dose fasting rule
FDA PI
ModerateNarrow Therapeutic Index oral drugs (e.g., warfarin, digoxin)
MechanismAltered gastric emptying may modify absorption kinetics
EffectPotential changes in Cmax and AUC of narrow-TI drugs; clinical significance varies
ManagementIncrease clinical or laboratory monitoring (e.g., INR for warfarin); adhere to 30-min post-dose fasting
FDA PI
MinorOral contraceptives
MechanismDelayed gastric emptying may theoretically delay absorption
EffectNo clinically significant change in ethinylestradiol/levonorgestrel exposure in formal study
ManagementNo dose adjustment required
Drug Interaction Study
MinorMetformin, simvastatin, digoxin
MechanismPotential altered GI transit
EffectNo clinically relevant changes in exposure in formal drug interaction studies
ManagementNo dose adjustment required for any of these agents
FDA PI
Mon

Monitoring

  • HbA1cBaseline, then every 3–6 months
    Routine    Primary efficacy marker. Consider uptitration if HbA1c target not met after 8+ weeks at maintenance dose. Expected reductions: 0.5–1.0% from 7 mg, 0.8–1.4% from 14 mg.
  • Renal FunctionBaseline, then during GI symptoms
    Trigger-based    Monitor eGFR and creatinine if patient develops significant nausea, vomiting, or diarrhea leading to dehydration. Postmarketing AKI cases have been reported, some requiring hemodialysis.
  • Diabetic RetinopathyBaseline, then per standard guidelines
    Routine    Patients with pre-existing retinopathy should be monitored more closely for progression, especially during periods of rapid glycemic improvement. Retinopathy complications were 4.2% vs 3.8% in pooled trials.
  • Body WeightEach visit
    Routine    Expected weight loss 2–5 kg. Weight is a secondary efficacy endpoint; can help with patient motivation and treatment adherence.
  • Pancreatitis SignsOngoing clinical vigilance
    Trigger-based    Educate patients on symptoms (severe persistent abdominal pain radiating to back, with or without vomiting). Amylase and lipase elevations of 10–34% are expected with GLP-1 agonists and do not alone indicate pancreatitis.
  • ThyroidClinical assessment; no routine calcitonin
    Trigger-based    Routine serum calcitonin or thyroid ultrasound is not recommended per FDA labeling (low specificity leading to unnecessary procedures). Evaluate neck mass, dysphagia, or persistent hoarseness if reported.
  • Blood GlucoseIncreased frequency with insulin/SU
    Trigger-based    Particularly important when combined with insulin or sulfonylureas. Monitor frequently during initiation and dose escalation. Severe hypoglycemia occurred in 0–1% as monotherapy.
  • TSH (with levothyroxine)4–6 weeks after initiation or titration
    Trigger-based    Levothyroxine exposure increases 33% with oral semaglutide. Check TSH 4–6 weeks after starting or changing semaglutide dose; adjust levothyroxine if needed.
CI

Contraindications & Cautions

Absolute Contraindications

  • Personal or family history of medullary thyroid carcinoma (MTC) — semaglutide causes thyroid C-cell tumors in rodents at clinically relevant exposures
  • Multiple Endocrine Neoplasia syndrome type 2 (MEN 2)
  • Prior serious hypersensitivity to semaglutide or any excipient — anaphylaxis and angioedema reported

Relative Contraindications (Specialist Input Recommended)

  • History of pancreatitis — GLP-1 agonists associated with acute pancreatitis including fatal cases; monitor closely and avoid in patients with active pancreatic disease
  • Severe gastroparesis — oral semaglutide further delays gastric emptying and is not recommended in this population
  • History of serious hypersensitivity to another GLP-1 RA — cross-reactivity unknown; use with caution
  • Pregnancy or planned pregnancy within 2 months — embryofetal toxicity in animals at sub-therapeutic exposures; discontinue at least 2 months before planned conception due to long washout

Use with Caution

  • Pre-existing diabetic retinopathy — monitor for progression; rapid glycemic improvement associated with worsening retinopathy (semaglutide injection SUSTAIN-6: 3% vs 1.8% placebo)
  • Patients on insulin or sulfonylureas — reduce secretagogue or insulin dose proactively to mitigate hypoglycemia
  • Renal impairment with GI symptoms — vomiting and diarrhea can precipitate volume depletion and AKI; counsel on hydration
  • Planned surgery requiring general anesthesia — GLP-1 class-wide concern for residual gastric contents and aspiration risk; inform anesthesia team
  • Breastfeeding — SNAC and/or its metabolites present in breast milk; breastfeeding not recommended with Rybelsus specifically (alternative injectable semaglutide formulations without SNAC may be considered)
FDA Boxed Warning Risk of Thyroid C-Cell Tumors

In rodent studies, semaglutide caused dose-dependent and treatment-duration-dependent thyroid C-cell tumors (adenomas and carcinomas) at clinically relevant exposures. It remains unknown whether oral semaglutide causes thyroid C-cell tumors, including medullary thyroid carcinoma (MTC), in humans. Rybelsus is contraindicated in patients with a personal or family history of MTC or MEN 2. Counsel all patients about the potential risk and symptoms of thyroid tumors (neck mass, dysphagia, dyspnea, persistent hoarseness). Routine calcitonin monitoring is not recommended.

Pt

Patient Counselling

Purpose of Therapy

Oral semaglutide works by mimicking a natural gut hormone (GLP-1) that helps the body release insulin when blood sugar is high, reduces appetite, and slows digestion. It is taken once daily as a pill and is used to improve blood sugar control in type 2 diabetes, with an added benefit of reducing the risk of heart attacks, strokes, and cardiovascular death in patients at high risk.

How to Take

Take one tablet first thing in the morning on a completely empty stomach. Swallow it whole with no more than a half-glass (4 ounces) of plain water. Then wait at least 30 minutes before eating breakfast, drinking any other beverage (including coffee or juice), or taking any other pills. Do not crush, split, or chew the tablet. If you miss a dose, skip it and take the next dose the following morning.

Nausea and GI Symptoms
Tell patientNausea is the most common side effect and usually improves over the first few weeks as the body adjusts. Eating smaller, lighter meals, avoiding greasy or very rich foods, and staying hydrated can help. The starting dose is intentionally low to ease the stomach into the medication.
Call prescriberIf nausea, vomiting, or diarrhea is severe or persistent, or if unable to keep fluids down, as dehydration can harm the kidneys.
Thyroid Cancer Warning
Tell patientIn animal studies, this class of medication caused thyroid tumors. It is not known if this occurs in humans. Report any lump or swelling in the neck, trouble swallowing, hoarseness, or shortness of breath.
Call prescriberImmediately if noticing a lump in the neck or difficulty swallowing or breathing.
Pancreatitis Warning Signs
Tell patientSevere or persistent stomach pain (especially in the upper abdomen radiating to the back) with or without vomiting could be a sign of pancreatitis, a serious condition requiring emergency care.
Call prescriberStop the medication and seek emergency care immediately if experiencing these symptoms.
Low Blood Sugar (with Insulin or SU)
Tell patientIf also taking insulin or a sulfonylurea, the risk of low blood sugar is higher. Symptoms include shakiness, sweating, confusion, rapid heartbeat, and hunger. Always carry a fast-acting glucose source.
Call prescriberIf experiencing frequent or severe low blood sugar episodes so that the other diabetes medication dose can be adjusted.
Pregnancy Planning
Tell patientOral semaglutide may harm an unborn baby based on animal studies. It must be stopped at least 2 months before trying to conceive because the drug stays in the body for weeks after the last dose. Alternative injectable semaglutide formulations (without SNAC) may be considered during breastfeeding under clinician guidance.
Call prescriberImmediately if becoming pregnant or planning to become pregnant.
Surgery and Procedures
Tell patientThis medication slows stomach emptying, which could increase the risk of food remaining in the stomach during anesthesia. Always tell the surgical or anesthesia team about this medication before any planned procedure.
Call prescriberWell in advance of any planned surgery or procedure to discuss whether and when to stop the medication.
Ref

Sources

Regulatory (PI / SmPC)
  1. Rybelsus (semaglutide) tablets, for oral use. Full Prescribing Information. Revised October 2025. Novo Nordisk Inc. FDA LabelPrimary source for all dosing (R1 and R2 formulations), indications (including Oct 2025 MACE indication), adverse reaction incidence rates, warnings, and drug interaction data.
  2. Rybelsus (semaglutide) tablets. Summary of Product Characteristics. European Medicines Agency. EMAEuropean regulatory summary; approved April 2020 for type 2 diabetes in the EU.
Key Clinical Trials
  1. McGuire DK, Busui RP, Deanfield J, et al. Oral semaglutide and cardiovascular outcomes in high-risk type 2 diabetes. N Engl J Med. 2025. Published March 29, 2025. doi:10.1056/NEJMoa2501006SOUL trial (N=9,650): demonstrated 14% MACE reduction (HR 0.86; 95% CI 0.77–0.96; P=0.006) over median 49.5-month follow-up; basis for the Oct 2025 CV risk reduction label expansion.
  2. Aroda VR, Rosenstock J, Terauchi Y, et al. PIONEER 1: randomized clinical trial of the efficacy and safety of oral semaglutide monotherapy in comparison with placebo in patients with type 2 diabetes. Diabetes Care. 2019;42(9):1724–1732. doi:10.2337/dc19-0749Pivotal monotherapy trial demonstrating HbA1c reductions of 0.6% (3 mg), 0.9% (7 mg), and 1.1% (14 mg) vs placebo at 26 weeks.
  3. Husain M, Birkenfeld AL, Donsmark M, et al. Oral semaglutide and cardiovascular outcomes in patients with type 2 diabetes. N Engl J Med. 2019;381(9):841–851. doi:10.1056/NEJMoa1901118PIONEER 6 CV safety trial (N=3,183): demonstrated non-inferiority for MACE (HR 0.79; 95% CI 0.57–1.11); the earlier, smaller CV trial that preceded SOUL.
  4. Marso SP, Bain SC, Consoli A, et al. Semaglutide and cardiovascular outcomes in patients with type 2 diabetes. N Engl J Med. 2016;375(19):1834–1844. doi:10.1056/NEJMoa1607141SUSTAIN-6 trial of subcutaneous semaglutide showing 26% MACE reduction; provided foundational CV evidence for the semaglutide molecule.
Guidelines
  1. American Diabetes Association Professional Practice Committee. Standards of Care in Diabetes — 2025. Diabetes Care. 2025;48(Suppl 1). doi:10.2337/dc25-SINTRecommends GLP-1 RA with proven CV benefit as preferred agent in T2DM patients with established ASCVD, HF, or CKD; oral semaglutide now qualifies for this recommendation following SOUL.
  2. Marx N, Federici M, Schutt K, et al. 2023 ESC Guidelines for the management of cardiovascular disease in patients with diabetes. Eur Heart J. 2023;44(39):4043–4140. doi:10.1093/eurheartj/ehad192European guideline positioning GLP-1 RAs and SGLT2 inhibitors as first-line cardiometabolic therapies alongside metformin for patients with T2DM and CVD.
Mechanistic / Basic Science
  1. Bucheit JD, Pamulapati LG, Carter N, et al. Oral semaglutide: a review of the first oral GLP-1 receptor agonist. Diabetes Technol Ther. 2020;22(1):10–18. doi:10.1089/dia.2019.0185Comprehensive review of oral semaglutide pharmacology, SNAC absorption enhancer mechanism, and PIONEER clinical program overview.
  2. Granhall C, Sondergaard FL, Thomsen M, Anderson TW. Pharmacokinetics, safety and tolerability of oral semaglutide in subjects with renal impairment. Clin Pharmacokinet. 2018;57(12):1571–1580. doi:10.1007/s40262-018-0649-2Demonstrates no clinically meaningful change in semaglutide PK across varying degrees of renal impairment; supports no dose adjustment recommendation.
Pharmacokinetics / Special Populations
  1. Baekdal TA, Thomsen M, Kupcinskate A, et al. Pharmacokinetics, safety, and tolerability of oral semaglutide in subjects with hepatic impairment. J Clin Pharmacol. 2018;58(10):1314–1323. doi:10.1002/jcph.1131No clinically relevant PK changes with hepatic impairment; supports no dose adjustment in mild, moderate, or severe hepatic disease.
  2. Jordy AB, Breitschaft A, Christiansen E, et al. Current understanding of SNAC as an absorption enhancer: the oral semaglutide experience. Clin Diabetes. 2024;42(1):74–82. doi:10.2337/cd23-0055Detailed review of SNAC technology, absorption mechanism, bioavailability (~0.8%), and evidence that once absorbed, oral and subcutaneous semaglutide behave identically.
  3. Aroda VR, Erber J, Engell RT, et al. Efficacy and safety of oral semaglutide across the PIONEER clinical trial program. Curr Med Res Opin. 2020;36(9):1489–1500. doi:10.1080/03007995.2020.1792350Pooled analysis of PIONEER trials 1–8; source for adverse reaction rates, discontinuation data, and efficacy benchmarks across clinical scenarios.
  4. Lewis AL, McEntee N, Holland J, Sheridan J. Development and approval of rybelsus (oral semaglutide): ushering in a new era in peptide delivery. Drug Deliv Transl Res. 2022;12(1):1–6. doi:10.1007/s13346-021-01000-wRegulatory development perspective on the SNAC co-formulation technology and its role in enabling oral peptide delivery.