Semaglutide: Difference between revisions

Semaglutide is a long-acting GLP-1 receptor agonist developed by Novo Nordisk, marketed as Ozempic (weekly subcutaneous, for type 2 diabetes mellitus),^[1] Wegovy (weekly subcutaneous, for obesity, cardiovascular risk reduction in obesity without diabetes, and MASH with fibrosis),^[2][6][7] and Rybelsus (daily oral tablet, for T2DM).^[3] It is, by revenue, among the highest-grossing medicines on the planet as of 2024.^{[citation needed]} Semaglutide is the second weekly GLP-1 RA from Novo Nordisk's incretin program (after liraglutide)^[5] and the molecule that, more than any other, made obesity treatment a mainstream rather than a specialty intervention.^{[citation needed]} + Add a problem

+ Add a titration strategy

Subjective effects vary considerably with dose and titration speed but reliably include:

• Early satiety — meals feel "complete" at a fraction of prior intake^[4]
• Food noise quieting — the most commonly volunteered subjective change. Patients report that intrusive food-related thoughts simply stop.^{[citation needed]}
• Reduced alcohol craving — corroborated by observational and small RCT data; mechanism likely shared with food reward circuitry^[8]
• Nausea — dose-dependent, worst in first 1–2 weeks of any new dose level^[1]
• Constipation or diarrhea (variable, can alternate)^[1]
• Sulfurous eructation (a small but very real subgroup)^{[citation needed]}
• Reduced taste preference for fatty / sweet foods in many users^{[citation needed]}

+ Add an effect

Chemistry. 31-amino-acid acylated peptide analog of human GLP-1 (7–37), with Aib substitution at position 8 (blocks DPP-4 cleavage) and a C18 fatty diacid linked via γGlu-2×OEG spacer at Lys26 (drives albumin binding → ~165 h half-life)^[5]

Acylation with a C18 fatty diacid drives non-covalent binding to serum albumin, slowing renal clearance and DPP-4 access. The Aib8 substitution renders the peptide DPP-4-resistant. Resulting terminal half-life ~165 h means once-weekly subcutaneous dosing produces near-steady-state plasma levels.^[5]

Oral semaglutide (Rybelsus) is co-formulated with SNAC (sodium N-[8-(2-hydroxybenzoyl)amino]caprylate), a permeation enhancer that transiently raises gastric pH and protects the peptide locally — yielding ~0.4–1% bioavailability, which is sufficient at 14 mg daily to match Ozempic 0.5 mg weekly for glycemic effect (but not for weight loss).^[3][9] Strict fasting administration is mandatory; any concurrent food or beverage destroys absorption.^[3]

Predominantly catabolic clearance via proteolysis; renal and hepatic impairment do not require dose adjustment.^[1] No CYP-mediated metabolism, so the interaction profile is dominated by gastric emptying effects on other oral medicines, not pharmacokinetic competition.^[1]

Receptor pharmacology. Selective long-acting agonist of the GLP-1 receptor (class B GPCR). Produces glucose-dependent insulin secretion, glucagon suppression, delayed gastric emptying, hypothalamic appetite suppression, and direct cardiovascular and renal protective effects.^[10]

At maintenance doses semaglutide produces:

• HbA1c reduction of ~1.5–2.0 percentage points (Ozempic 1 mg)^[11]
• Weight loss of ~6 kg (Ozempic 1 mg, T2DM)^[11] to ~14.9% body weight (Wegovy 2.4 mg, obesity without T2DM, STEP-1)^[4]
• Systolic BP reduction of ~5 mmHg^[6]
• Modest LDL-C reduction, larger triglyceride reduction^{[citation needed]}
• 20% relative risk reduction in MACE in obesity without T2DM (SELECT)^[6]
• 24% relative risk reduction in kidney + CV composite in T2DM + CKD (FLOW)^[12]

  Interactions

Category formerly X-equivalent; current FDA labeling: avoid in pregnancy.^[1] Animal embryofetal toxicity is well-documented.^[1] Because the half-life is ~1 week, current guidance is to discontinue at least 2 months before any planned conception.^[1]

Postpartum: not recommended during breastfeeding pending more data; small molecule transfer to milk is unlikely given peptide structure but not formally characterized.^{[citation needed]}

Importantly: semaglutide is not a contraceptive, and the medicine may restore ovulation in patients with PCOS or obesity-associated anovulation.^{[citation needed]} Patients of childbearing potential should be counseled about contraception before starting.

• Baseline: HbA1c, weight, BP, renal function, lipid panel, ALT/AST (especially for MASH problem)
• Personal or family history of MTC or MEN2 — contraindicated, do not start^[1]
• Every 3 months for first year: HbA1c, weight, GI tolerability, signs of pancreatitis or gallbladder disease
• Annual: renal function, lipids
• Pre-procedure: hold weekly dose ≥7 days before any planned anesthesia (per ASA 2024 guidance) due to delayed gastric emptying / aspiration risk^[13]

  Patient counseling

• Slow titration is non-negotiable for tolerability. Patients who insist on faster ramps usually quit from GI side effects.
• Inject SC in abdomen, thigh, or upper arm; rotate sites. Pen is single-patient, multi-dose.^[1]
• GI side effects almost always peak in first 2–4 weeks of any new dose level, then attenuate.^[1]
• Eat smaller portions earlier in the day. Plate sizes will feel comically large after a few weeks — that is the medicine working, not a problem to fix.
• Hydrate aggressively (volume depletion → AKI is a real risk).^[1]
• Resistance training during weight loss protects lean mass and is strongly encouraged.^{[citation needed]}
• If a weekly dose is missed: take within 5 days; if >5 days, skip and resume on the next regular day.^[1]
• Avoid alcohol during titration weeks (compounds nausea).
• Pregnancy planning: stop ≥2 months before trying to conceive.^[1]
• Surgery: tell every anesthesiologist and surgeon you are on a weekly GLP-1 RA. Hold dose 7 days pre-op.^[13]

  Relevant anecdote

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GLP-1 receptor agonist · Tirzepatide · Liraglutide · Dulaglutide · Exenatide · Type 2 diabetes mellitus · Obesity · MASH