Semaglutide is a 31-amino-acid synthetic peptide developed by Novo Nordisk that selectively activates the GLP-1 (glucagon-like peptide-1) receptor. The molecule is built on the native human GLP-1(7-37) backbone with three engineered changes: an alpha-aminoisobutyric-acid (Aib) substitution at position 8 to block DPP-4 cleavage, an arginine substitution at position 34 to remove a competing acylation site, and a C18 fatty diacid attached to lysine 26 via a gamma-glutamic-acid plus 2 x AEEA spacer to drive albumin binding and a multi-day half-life. Average molecular weight is 4113.58 g/mol. It is supplied as a lyophilised powder for in-vitro and laboratory research only.

What did the STEP and SELECT trials show?

The STEP series was the Phase 3 obesity programme. The pivotal STEP-1 paper (Wilding et al., NEJM 2021) ran 1961 adults with obesity but without type-2 diabetes for 68 weeks and reported a mean body-weight reduction of 14.9 percent at the 2.4 mg weekly dose, against 2.4 percent on placebo. STEP-2 in adults with type-2 diabetes plus obesity reported approximately 9.6 percent reduction. STEP-5 ran for 104 weeks and confirmed the loss was sustained over a longer treatment window. The SELECT cardiovascular outcomes trial (Lincoff et al., NEJM 2023) ran 17604 adults with overweight or obesity plus established cardiovascular disease but without type-2 diabetes, and reported a 20 percent reduction in major adverse cardiovascular events at the 2.4 mg weekly dose over a mean follow-up of 39.8 months. The SELECT data was the first demonstration that a GLP-1 receptor agonist reduces cardiovascular events in a population without diabetes.

Why does Semaglutide have a once-weekly half-life?

Native GLP-1 has a half-life of around 90 seconds because it is rapidly cleaved by the dipeptidyl peptidase-4 (DPP-4) enzyme and cleared by the kidneys. Semaglutide extends this to approximately 165 hours (about 7 days) through three combined modifications. First, the Aib residue at position 8 prevents DPP-4 from cleaving the molecule. Second, the C18 fatty diacid attached at lysine 26 binds reversibly to serum albumin, the most abundant plasma protein, which dramatically slows kidney filtration. Third, the arginine substitution at position 34 stops the C18 fatty acid from being mis-attached to a different lysine during synthesis. Together these three changes produce an 11000-fold increase in effective half-life over native GLP-1 and enable once-weekly subcutaneous dosing in published research.

What are Ozempic, Wegovy, and Rybelsus?

All three are Novo Nordisk's branded prescription products containing the same semaglutide active molecule. Ozempic is the once-weekly subcutaneous injection licensed for type-2 diabetes (FDA December 2017, MHRA 2018). Wegovy is the higher-dose once-weekly subcutaneous injection licensed for chronic weight management in adults (FDA June 2021, MHRA 2021) and for adolescents 12 years and older (FDA December 2022). Rybelsus is the oral once-daily tablet formulation licensed for type-2 diabetes (FDA September 2019), notable as the first oral GLP-1 receptor agonist to reach market. Black & White Peptides Ltd does not supply any of these branded prescription products. Our research-grade semaglutide is a separate product category for laboratory and in-vitro research only.

How do I verify a Semaglutide batch is real?

Three checks. (1) HPLC report: a single tall peak on a reversed-phase chromatogram, purity reported above 99 percent in the analytical summary, no significant secondary peaks. The semaglutide market has been awash with counterfeit and underdosed material since the global Ozempic and Wegovy supply shortages of 2022 and 2023, so the chromatogram trace itself matters more than the headline percentage. (2) Mass spectrometry: where included, the molecular ion in positive ion mode confirms the 4113.58 g/mol average mass; multiply-charged species at characteristic m/z values around 1372, 1029, 824 and 687 (the [M+3H]3+, [M+4H]4+, [M+5H]5+ and [M+6H]6+ states) are typical and useful as cross-checks. (3) The lyophilised cake should be a uniform porous white puck filling the bottom of the vial, with no yellowing, no caramelisation, and no loose granular powder. The Janoshik certificate verification key on the issuing lab's public portal is the standard reference.

How is Semaglutide stored?

The lyophilised cake is shipped sealed in amber glass and is stable for 24 months or more at 2 to 8 degrees Celsius, kept dry, sealed, and protected from light. Once reconstituted with bacteriostatic water, the published preclinical analytical literature commonly references stability over a window of four to six weeks under refrigeration; readers should refer to the specific assay or research method they are running for the exact figure for their context. Standard practice is to avoid freeze-thaw cycles on the reconstituted solution, which is the most common cause of measurable activity loss in any reconstituted research peptide.

How does Semaglutide compare to Tirzepatide and Retatrutide?

Semaglutide is a single-target GLP-1 receptor agonist; tirzepatide adds a second receptor (the dual GIP and GLP-1 twincretin); retatrutide adds a third (the trinity GIP plus GLP-1 plus glucagon agonist). The published trial endpoints scale roughly with this receptor coverage. STEP-1 (semaglutide 2.4 mg, 68 weeks) reported 14.9 percent body-weight reduction. SURMOUNT-1 (tirzepatide 15 mg, 72 weeks) reported 20.9 percent. The Phase 2 retatrutide obesity trial (Jastreboff 2023, 12 mg, 48 weeks) reported 24.2 percent. Each successive generation widens the receptor footprint and produces a measurably larger effect on the published endpoints. The trade-off is that semaglutide has the longest licensure history, the most cardiovascular outcome data, and the only oral formulation; tirzepatide is the newest licensed in-class agent; retatrutide is still in Phase 3.

Is Semaglutide legal in the UK?

Semaglutide as the licensed prescription products Ozempic, Wegovy, and Rybelsus is authorised by the MHRA. Those licensed products are prescription-only medicines administered or self-administered under prescriber supervision and dispensed by a registered pharmacy. Research-grade semaglutide as supplied by Black & White Peptides Ltd is a separate product category: an unscheduled research-grade reference reagent for laboratory and in-vitro research use only, with no human or veterinary use intended or implied, and is NOT a substitute for, equivalent to, or marketed as a generic of the licensed Ozempic, Wegovy or Rybelsus products. Patients holding a prescription for any of those branded products should obtain them through their pharmacist and not through the research-peptide supply chain.

Semaglutide Explained: The GLP-1 Receptor Agonist (UK 2026)

TL;DR. Semaglutide is a 31-amino-acid synthetic peptide that activates the GLP-1 receptor. Built on the native human GLP-1(7-37) backbone with three engineered changes (Aib at position 8 for DPP-4 resistance, Arg substitution at position 34 to remove a competing acylation site, and a C18 fatty diacid attached to Lys26 via gamma-Glu plus 2 x AEEA spacer for albumin binding). Average molecular weight is 4113.58 g/mol; effective half-life around 165 hours, supporting once-weekly subcutaneous dosing. Pivotal data: STEP-1 (Wilding et al., NEJM 2021) reported 14.9 percent body-weight reduction at 2.4 mg weekly over 68 weeks, and SELECT (Lincoff et al., NEJM 2023) was the first demonstration that a GLP-1 agonist reduces cardiovascular events in a population without diabetes (20 percent MACE reduction). Verify a real research-grade batch the same way as any other peptide: a clean single-peak HPLC chromatogram at 99%+ purity, mass-spec confirmation of the 4113.58 g/mol mass, and a uniform porous white lyophilised cake. Research use only. Not a substitute for prescription Ozempic, Wegovy or Rybelsus.

What Semaglutide actually is

Semaglutide is a long-acting analogue of human glucagon-like peptide-1, the gut hormone released after a meal that drives a glucose-dependent insulin response in the pancreatic beta cells along with a wider set of effects on satiety, gastric emptying, and adipose-tissue function. The native human GLP-1 peptide is biologically powerful but pharmacologically useless on its own: it has a circulating half-life of around 90 seconds, because the dipeptidyl peptidase-4 (DPP-4) enzyme cleaves it almost as fast as it is released and the kidneys clear what remains.

Semaglutide solves both problems with three small changes to the native GLP-1(7-37) sequence. The molecule was discovered and characterised at Novo Nordisk by Lotte Bjerre Knudsen and her team across the early 2010s, and the foundational publication is Lau et al., "Discovery of the Once-Weekly Glucagon-Like Peptide-1 (GLP-1) Analogue Semaglutide" (J. Med. Chem. 2015). Three modifications, one engineering goal: stop the molecule being cleaved, slow the molecule being cleared.

Length	31 amino acids (with C-terminal glycine)
Average MW	4113.58 g/mol
Modification 1	Aib at position 8 (alpha-aminoisobutyric acid replaces native Ala) - blocks DPP-4 cleavage
Modification 2	Arg at position 34 (replaces native Lys) - removes competing acylation site
Modification 3	C18 fatty diacid attached at Lys26 via gamma-Glu plus 2 x AEEA spacer - drives albumin binding
Receptor profile	Single-target GLP-1 receptor agonist (no GIP, no glucagon)
Half-life	~165 hours (~7 days), supports once-weekly subcutaneous administration
Lyophilised stability	24+ months at 2–8 °C, sealed and protected from light
Branded prescription products	Ozempic (subcut, T2D), Wegovy (subcut, obesity), Rybelsus (oral, T2D)

The three engineering changes that built the molecule

How three small substitutions produced an 11000-fold half-life jump.

Native GLP-1: cleaved by DPP-4 at the Ala8 - Glu9 bond within seconds of release, half-life around 90 seconds. Change 1, position 8 Ala becomes Aib. Aib (alpha-aminoisobutyric acid) is a non-natural amino acid with a sterically hindered alpha carbon that DPP-4 simply does not recognise. The cleavage step is gone.

That alone takes you from seconds to minutes, but the kidneys still filter the molecule out within hours. Change 2, attach a long fatty diacid to Lys26 via a small linker (gamma-Glu plus 2 x AEEA) so the molecule binds reversibly to serum albumin. Albumin is the most abundant protein in plasma. A peptide that sticks to albumin clears at roughly the rate albumin clears, which is days, not hours.

The fatty acid wants to attach to any free lysine side chain during synthesis, so without a third change you would get a mixture of Lys26-acylated and Lys34-acylated product. Change 3, swap Lys34 for Arg. Same backbone shape, but the side chain is no longer a target for the acylation chemistry. The synthesis is now clean and the final molecule is a defined, single-modification compound.

End result: native GLP-1 half-life ~90 seconds, semaglutide half-life ~165 hours. About 6600-fold longer in the bloodstream from three deliberate residue choices. Modern long-acting peptide design in one molecule.

The STEP and SELECT trial data

The Phase 3 programme has been one of the most consequential metabolic-research trial sets of the last decade. Two parallel arcs.

SUSTAIN (type 2 diabetes)

Seven trials (SUSTAIN-1 through 7+) in adults with type-2 diabetes. Across the series, semaglutide produced larger reductions in HbA1c and body weight than placebo, dulaglutide, exenatide ER and insulin glargine at matched dose comparisons. SUSTAIN-6 (Marso et al., NEJM 2016) was the first cardiovascular outcomes trial in the programme and showed non-inferiority on major adverse cardiovascular events.

STEP (obesity, no diabetes required)

The pivotal obesity trial, STEP-1, was published as Wilding et al., NEJM 2021, PMID 33567185. 1961 adults with obesity (mean BMI 37.9) but without type-2 diabetes were randomised to placebo or semaglutide 2.4 mg weekly for 68 weeks.

Trial	Population	Duration	Body-weight change at endpoint
STEP-1	Adults with obesity, no T2D	68 weeks	−14.9 % (vs −2.4 % placebo)
STEP-2	Adults with T2D + obesity	68 weeks	−9.6 % (vs −3.4 % placebo)
STEP-3	Adults with obesity + intensive behavioural therapy	68 weeks	−16.0 % (vs −5.7 % placebo)
STEP-5	Adults with obesity, no T2D	104 weeks	−15.2 % sustained
STEP-8	Head-to-head vs liraglutide	68 weeks	Beat liraglutide on every primary endpoint

SELECT (cardiovascular outcomes in obesity, no diabetes)

The single most important data point published on semaglutide outside diabetes was the SELECT trial, Lincoff et al., NEJM 2023, PMID 37962078. 17604 adults with overweight or obesity plus established cardiovascular disease but without type-2 diabetes were randomised to placebo or semaglutide 2.4 mg weekly. After a mean follow-up of 39.8 months, the primary composite endpoint (cardiovascular death, non-fatal myocardial infarction, or non-fatal stroke) was reduced by 20 percent in the semaglutide arm.

SELECT was the first demonstration in the published trial literature that a GLP-1 receptor agonist reduces cardiovascular events in a non-diabetic population. The 2024 expansion of the FDA Wegovy label to include cardiovascular risk reduction in adults with established CVD plus overweight or obesity rests on this data.

The branded products

Ozempic (subcutaneous injection, type-2 diabetes). FDA approved December 2017, MHRA 2018.
Rybelsus (oral once-daily tablet, type-2 diabetes). FDA approved September 2019. The first oral GLP-1 receptor agonist to reach market.
Wegovy (subcutaneous injection, chronic weight management). FDA approved June 2021 for adults, December 2022 for adolescents 12+. MHRA 2021.

What to look for on the Certificate of Analysis

If you've read our walk-through of a Janoshik HPLC report, the standard structure applies. For semaglutide specifically:

1. A single tall peak on the reversed-phase HPLC chromatogram

One dominant peak at the semaglutide retention time, a flat baseline elsewhere, 99%+ purity in the analytical summary. The semaglutide market has been awash with counterfeit and underdosed material since the global Ozempic and Wegovy supply shortages of 2022 and 2023. The trace itself matters more than the quoted percentage.

2. Mass spectrometry confirmation of the 4113.58 g/mol mass

Semaglutide is large enough that electrospray mass spectra show multiply-charged species rather than a single intact molecular ion. The typical positive-ion charge states are [M+3H]3+ at m/z 1372.2, [M+4H]4+ at m/z 1029.4, [M+5H]5+ at m/z 823.7, and [M+6H]6+ at m/z 686.6. A real spectrum from Janoshik or any competent peptide-analysis lab will show a characteristic ladder of these charge states with the masses cross-summable back to 4113.58 g/mol average.

3. The Janoshik verification key resolves on their portal

Every Janoshik certificate carries a short alphanumeric verification key. That key plus the task ID printed on the certificate can be cross-referenced on the issuing lab's public records. A real semaglutide batch resolves; a fabricated COA does not. Cross-check it yourself.

Storage and handling at your bench

Refrigerate at 2–8 °C in the original sealed amber-glass vial. Semaglutide is stable for 24 months or more in the lyophilised state when kept dry, sealed, and protected from light.
Reconstitute with bacteriostatic water by adding the water slowly down the inside wall of the vial and gently swirling (not shaking, never vortexing) until the cake fully dissolves. The resulting solution should be clear and colourless.
Reconstituted shelf life is shorter than the lyophilised form. The published preclinical analytical literature commonly references stability over a window of four to six weeks under refrigeration.
Avoid freeze-thaw cycles on the reconstituted solution. The lipid modification makes semaglutide micelle-prone in solution and repeated freeze-thaw is the most common cause of measurable activity loss.
Ship and store in amber glass. Less photolabile than copper-coordinated peptides like GHK-Cu, but cold-chain amber-glass is the right default for any modern long-acting lipopeptide.

Common red flags when sourcing semaglutide

Walk-away signals when buying semaglutide

The lyophilised cake in the supplier's product photos is yellowed, cream-coloured, or shown as a heap of loose granular powder rather than a uniform porous white cake. Semaglutide done correctly produces a clean white puck.
No batch-specific Certificate of Analysis included with the order. The semaglutide market is the second-most-counterfeited peptide segment globally (after tirzepatide); a generic "we test our products" line on the website is not the same as a per-batch COA tied to the vial in your hand.
The COA carries no verification key, or the key does not resolve on the issuing lab's public portal.
The chromatogram (if shown) has multiple peaks of comparable height. Semaglutide synthesis at 99%+ produces a single dominant peak with minor impurities, not a cluster of near-equal peaks.
Mass-spectrometry data is absent or shows only one of the multiply-charged species in isolation. A real semaglutide spectrum has the multi-charge-state ladder.
The supplier markets "semaglutide" oral capsules that claim to match Rybelsus pharmacokinetics. Rybelsus is a complex formulation built around a permeation enhancer (SNAC) and is not reproducible by simply encapsulating research-grade powder.
Pricing far below the broader market rate. Semaglutide is not a cheap molecule to synthesise correctly to 99%+ purity. A vial at a fraction of the going rate is, more often than not, a vial of an older, cheaper GLP-1 analogue with a semaglutide label on it, or an underdosed product.
Vial label has no batch number, no fill weight, or no manufacturer identifier.

Where this fits in the metabolic-research family

Semaglutide is the first generation of the long-acting GLP-1 architecture; tirzepatide is the second generation (dual GIP plus GLP-1); retatrutide is the third (trinity GIP plus GLP-1 plus glucagon). The receptor footprint widens with each generation and the published trial endpoints scale roughly with that footprint. Our side-by-side write-ups cover the trade-offs:

Semaglutide vs Retatrutide - single-target vs trinity agonist
Tirzepatide vs Semaglutide - dual vs single agonist
Semaglutide vs Liraglutide - once-weekly vs once-daily, two generations of the same architecture

What we supply

We stock semaglutide as a lyophilised cake in 5mg, 10mg and 20mg amber-glass vials, plus a pre-filled pen format in matching dose strengths, independently HPLC-verified by Janoshik Analytical to 99%+ purity. The Janoshik Certificate of Analysis ships in the box with every order where one is available for the current batch, and the report is also published on our Purity page for independent reference. The product page with current pricing, the integrated dose calculator (built around the STEP-1 0.25 / 0.5 / 1 / 1.7 / 2.4 mg weekly titration ladder), the research-protocol tabs, and the BAC-water option is at /peptides/semaglutide.html.

Important regulatory note. Novo Nordisk's branded semaglutide products are licensed in the UK as Ozempic (type-2 diabetes), Wegovy (chronic weight management), and Rybelsus (oral type-2 diabetes). Those licensed products are prescription-only medicines administered or self-administered under prescriber supervision and dispensed by a registered pharmacy under the regulatory framework that applies to MHRA-authorised medicines. Black & White Peptides Ltd supplies semaglutide as a research-grade reference reagent for laboratory and in-vitro research only. Our product is NOT a substitute for, equivalent to, or marketed as a generic of Ozempic, Wegovy or Rybelsus. We do not provide therapeutic claims, dosing guidance, administration protocols, or any content relating to human or veterinary use. If a clinician has prescribed any of those branded products for you, the licensed pharmacy product is the correct route.

Research use only. The compound information described above is drawn from peer-reviewed analytical and clinical literature and is provided for laboratory and in-vitro research context.

Joe, founder of Black & White Peptides Ltd. UK-registered research-peptide supplier, Companies House number 16876162. Writing on the technical side of the market that most suppliers prefer to leave fuzzy. Questions? WhatsApp or email - real human reply.

Semaglutide explained: the GLP-1 receptor agonist that defined the modern era.