Structure Therapeutics Reports Positive Topline Data from Phase 2 ACCESS II Trial with Once-Daily Oral Small Molecule GLP-1 Receptor Agonist, Aleniglipron

Rhea-AI Summary

Structure Therapeutics (NASDAQ: GPCR) reported positive Phase 2 ACCESS program topline data for oral GLP-1 receptor agonist aleniglipron. Placebo-adjusted mean weight loss at 44 weeks was -16.3% (180 mg) and -16.0% (240 mg); OLE 56-week loss reached -16.2% (120 mg).

Tolerability improved using a 2.5 mg starting dose (AE-related discontinuations 2.0–3.4%). No drug-induced liver injury or QTc prolongation observed across >625 participants. End-of-Phase 2 FDA meeting set for Q2 2026; Phase 3 initiation on track for 2H 2026.

Positive

• Placebo-adjusted weight loss of 16.3% at 180 mg
• Placebo-adjusted weight loss of 16.0% at 240 mg
• 16.2% weight loss at 56 weeks (120 mg) in OLE
• Low AE-related discontinuations of 2.0–3.4% with 2.5 mg start
• No liver injury or QTc signal across >625 participants
• Type B FDA meeting scheduled Q2 2026; Phase 3 on track 2H 2026

Negative

• Common GI adverse events (nausea, vomiting) during titration
• ACCESS II enrolled only 85 participants, limiting broader generalizability

Key Figures

Weight loss 180 mg: 16.3% (39 lbs) Weight loss 240 mg: 16.0% (37 lbs) Weight loss 120 mg OLE: 16.2% (40.5 lbs) +5 more

8 metrics

Weight loss 180 mg 16.3% (39 lbs) Placebo-adjusted mean loss at 44 weeks in ACCESS II

Weight loss 240 mg 16.0% (37 lbs) Placebo-adjusted mean loss at 44 weeks in ACCESS II

Weight loss 120 mg OLE 16.2% (40.5 lbs) Mean loss at 56 weeks in ACCESS OLE

AE discontinuation ≥120 mg 3.7% AE-related discontinuation in ACCESS II from 28–44 weeks

AE discontinuation OLE 2% Overall AE-related discontinuation rate in ACCESS OLE (median 20 weeks)

AE discontinuation body comp 3.4% Overall AE-related discontinuation rate in body composition study

Weight loss at 20 weeks 6.8% Weight loss with 2.5 mg start in body composition study

Participants exposed More than 625 Total participants across all aleniglipron studies

Market Reality Check

Price: $56.65 Vol: Volume 587,053 is below t...

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$56.65 Last Close

Volume Volume 587,053 is below the 20-day average of 809,016 (relative volume 0.73x) ahead of this news. normal

Technical Price $53.75 is trading above the 200-day MA of $39.84, following a prior move from the $13.22 52-week low.

Peers on Argus

Sector peers showed mixed moves pre-news: ELVN (-4.86%), AMLX (-3.52%), PGEN (+5...

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Sector peers showed mixed moves pre-news: ELVN (-4.86%), AMLX (-3.52%), PGEN (+5.72%), NUVB (+0.68%), TRML (flat). Momentum scanner only flagged TRVI at -0.91%, suggesting stock-specific rather than coordinated sector action around GPCR.

Previous Clinical trial Reports

5 past events · Latest: Dec 17 (Positive)

Same Type Pattern 5 events

Date	Event	Sentiment	Move	Catalyst
Dec 17	Phase 1 initiation	Positive	-2.8%	Started first-in-human Phase 1 trial of oral amylin agonist ACCG-2671.
Dec 08	Topline Phase 2 data	Positive	+102.5%	Reported strong 36-week ACCESS topline aleniglipron weight-loss results.
Jun 20	Preclinical obesity data	Positive	+1.7%	Presented preclinical obesity data for amylin agonist and GLP-1 program posters.
Nov 13	Phase 2b dosing start	Positive	+3.6%	Dosed first patients in Phase 2b ACCESS and announced ACCESS II higher-dose study.
Jun 03	Phase 2a topline	Positive	+54.2%	Reported positive Phase 2a obesity and PK data for oral GLP-1 GSBR-1290.

Pattern Detected

Clinical updates have often triggered strong upside moves, with one major obesity readout producing a triple-digit gain, though not all clinical milestones have been rewarded (one notable negative reaction).

Recent Company History

Over the past two years, Structure Therapeutics has steadily advanced its obesity pipeline. Early Phase 2a data in June 2024 and initiation of the Phase 2b ACCESS program in November 2024 were followed by multiple positive GLP‑1 obesity readouts, including a major ACCESS update in December 2025 that drove a 102.49% move. Additional obesity work includes preclinical and Phase 1 development for amylin agonist ACCG‑2671. Today’s ACCESS II and OLE results build directly on this sequence of escalating clinical evidence in obesity.

Historical Comparison

+31.8% avg move · Clinical-trial headlines for GPCR have averaged a 31.84% move, with one ACCESS obesity readout excee...

clinical trial

+31.8%

Average Historical Move clinical trial

Clinical-trial headlines for GPCR have averaged a 31.84% move, with one ACCESS obesity readout exceeding 100%. Today’s Phase 2 ACCESS II and OLE data extend that same obesity story, fitting into a pattern where robust efficacy updates have often been major catalysts.

Across prior clinical-trial releases, GPCR moved from early Phase 2a obesity data to Phase 2b ACCESS initiation, then to robust 36-week ACCESS topline and higher-dose ACCESS II results. The new 44- and 56-week ACCESS II/OLE data continue this progression toward Phase 3 obesity development for aleniglipron, while amylin agonist ACCG‑2671 advances in parallel.

Regulatory & Risk Context

Active S-3 Shelf

Shelf Active

Active S-3 Shelf Registration 2025-08-06

The company has an active automatic shelf registration on Form S-3ASR filed on 2025-08-06, effective through 2028-08-06, with 0 recorded usages in the provided data. Specific capacity amounts are not available here, but the shelf structure allows the company flexibility to issue securities if it chooses.

Market Pulse Summary

This announcement adds mature 44- and 56-week data to Structure Therapeutics’ obesity program, with ...

Analysis

This announcement adds mature 44- and 56-week data to Structure Therapeutics’ obesity program, with placebo-adjusted weight loss up to 16.3% and AE-related discontinuation rates as low as 2–3.7%. These findings extend a history of positive GLP‑1 obesity readouts and support plans for Phase 3 initiation in 2H 2026. An existing S-3ASR shelf and prior equity raises highlight financing flexibility as the program scales, while safety, durability of effect, and regulatory feedback remain key metrics to monitor.

Key Terms

glp-1 receptor agonist, open label extension (ole), adverse events, body mass index (bmi), +3 more

7 terms

glp-1 receptor agonist medical

"oral small molecule glp-1 receptor agonist, aleniglipron, for the treatment of obesity"

A GLP-1 receptor agonist is a medicine that mimics a natural gut hormone to trigger insulin release, slow stomach emptying, and curb appetite — like using a key to turn on a lock that controls blood sugar and hunger signals. For investors, these drugs matter because they treat common conditions such as diabetes and obesity, can drive large prescription and sales growth, reshape healthcare costs, and heavily affect drug pipelines, competition and company valuations.

open label extension (ole) medical

"continued weight loss up to 16.2% ... in the access open label extension (ole) study"

An open label extension (OLE) is a follow-up phase of a clinical trial where participants continue receiving a study treatment and both researchers and patients know what drug is being given. It matters to investors because OLEs produce longer-term safety and effectiveness information, help retain trial participants, and can strengthen regulatory filings or commercial plans—like a long-term test drive that shows whether a product performs safely and reliably over time.

adverse events medical

"low (2.0 – 3.4%) study drug discontinuations due to adverse events with the lower 2.5 mg"

Adverse events are any harmful or unwanted medical occurrences experienced by people using a drug, device, or undergoing a treatment, whether or not the problem is caused by the product. Think of them as complaints or breakdowns noticed during a trial or after a product is on the market; regulators record and investigate them. Investors care because clusters or serious adverse events can delay approvals, trigger costly studies or recalls, change labeling, and quickly alter a company’s revenue and risk profile.

body mass index (bmi) medical

"enrolled 85 adult participants living with obesity or overweight (defined as a bmi of greater than 25 kg/m2)"

Body mass index (BMI) is a simple number calculated from a person’s weight and height that gives a rough indication of whether their body size falls into categories such as underweight, normal, overweight, or obese. For investors, BMI matters because it’s a common screening measure used in public health, insurance underwriting, clinical trials and market research; shifts in population BMI can affect demand for medical services, drugs, insurance costs and related business risks, like a quick fuel-gauge that signals broader health trends.

placebo-adjusted technical

"placebo-adjusted mean weight loss of 16.3% (39 lbs) at the 180 mg dose"

The placebo-adjusted effect is the measured benefit of a treatment after subtracting any improvement seen in people who received a dummy or inactive treatment (placebo). Think of it like checking how much louder a new speaker is by comparing it to a broken speaker playing the same track; it isolates the true contribution of the product itself. Investors watch this because it shows the real clinical benefit that regulators, doctors, and payers will use to judge a therapy’s approval, demand, and pricing potential.

randomized, double-blind, placebo-controlled technical

"access ii is a randomized, double-blind, placebo-controlled, clinical study of aleniglipron"

A "randomized, double-blind, placebo-controlled" process is a method used to test the effectiveness of a new treatment or intervention. Participants are randomly assigned to different groups, with one receiving the real treatment and the other a fake version, called a placebo. Neither the participants nor the researchers know who is receiving which, which helps ensure unbiased results. For investors, this rigorous approach increases confidence that the findings are accurate and not influenced by guesswork or bias.

qtc prolongation medical

"and no qtc prolongation across all aleniglipron studies"

QTc prolongation is a lengthening of the heart’s electrical “reset” time between beats, measured on an electrocardiogram and adjusted for heart rate. It matters to investors because prolonged QTc can signal a drug or device safety risk that may lead to regulatory warnings, clinical trial delays, label restrictions, market withdrawals, or higher liability costs—similar to a car whose brakes take longer to reset, increasing the chance of a dangerous failure.

AI-generated analysis. Not financial advice.

Placebo-adjusted mean weight loss of 16.3% (39 lbs) at 180 mg and 16.0% (37 lbs) at 240 mg at 44 weeks with no evidence of weight loss plateau in ACCESS II, demonstrating highest efficacy among oral GLP-1RAs and comparable efficacy to injectable GLP1-RAs

Continued weight loss up to 16.2% (40.5 lbs) observed with 120 mg dose in the ACCESS Open Label Extension (OLE) study at 56 weeks, with no evidence of weight loss plateau

Updated interim data from ACCESS OLE and Body Composition studies continue to support improved tolerability and low (2.0 – 3.4%) study drug discontinuations due to adverse events with the lower 2.5 mg starting dose

End-of-Phase 2 meeting with FDA scheduled in the second quarter of 2026;
Phase 3 initiation remains on track for 2H 2026

Company to host conference call today at 8:30 a.m. Eastern Time

SAN FRANCISCO, March 16, 2026 (GLOBE NEWSWIRE) -- Structure Therapeutics Inc. (NASDAQ: GPCR), a clinical-stage global biopharmaceutical company developing novel oral small molecule therapeutics for metabolic diseases, with a focus on obesity, today announced positive topline data from the ACCESS clinical program of aleniglipron for the treatment of people living with obesity and/or overweight with at least one weight related co-morbidity. This includes 44-week data from the Phase 2 ACCESS II study and interim data from the ongoing body composition study and the ACCESS open label extension (OLE) study. Aleniglipron is an investigational orally-available, once-daily, nonpeptide small molecule agonist of the glucagon-like-peptide-1 (GLP-1) receptor designed to address patient needs and accessibility.

In the Phase 2 ACCESS II study, aleniglipron achieved clinically meaningful and statistically significant placebo-adjusted mean weight loss of 16.3% (39 lbs; p<0.0001) at the 180 mg dose and 16.0% (37 lbs; p<0.0001) at the 240 mg dose at 44 weeks. In the ACCESS OLE study, aleniglipron achieved continued weight loss from 36 weeks, up to 16.2% (40.5 lbs) with 120 mg at 56 weeks. Both studies continue to demonstrate no evidence of weight loss plateau.

Aleniglipron continues to demonstrate a tolerability profile that is consistent with the GLP-1 receptor agonist class and a compelling safety profile with no off-target events. In ACCESS II, across all active arms in participants who reached doses 120 mg or higher from 28 to 44 weeks, there was only one (3.7%) adverse event (AE)-related treatment discontinuation.

With a median follow-up of 20 weeks, the tolerability data as of the February 20, 2026 cutoff date from the interim analyses of the OLE and the body composition studies provide further support that the use of 2.5 mg as a lower starting dose very meaningfully reduces the rate of AE-related discontinuations during the titration phase. In the OLE, with a median follow-up of 20 weeks, there was an overall AE-related discontinuation rate of 2%. In the body composition study, with a median follow-up of 20 weeks, there was an overall AE-related discontinuation rate of 3.4% in the aleniglipron arm.

Together, these positive efficacy, tolerability and safety findings continue to support the advancement of aleniglipron into Phase 3 clinical development, with initiation anticipated in the second half of 2026.

“The totality of efficacy and tolerability data across the Phase 2 program continue to demonstrate clear differentiation of aleniglipron, with the highest weight loss observed for an oral GLP-1RA to date and a safety profile appropriate for chronic use in a disease that impacts millions of people,” said Raymond Stevens, Ph.D., CEO of Structure Therapeutics. “The consistent weight loss observed across multiple studies to date reaffirms aleniglipron’s potential to be a best-in-class oral GLP-1, with injectable-like efficacy that could become a backbone oral small molecule therapy for obesity.”

“The weight-lowering data from these ACCESS studies, without apparent plateau by Week 56, are encouraging—particularly the weight loss from baseline of up to -15.3% vs +1.1% at 180mg in ACCESS II that hopefully will be confirmed in larger, longer-term studies,” said Julio Rosenstock, MD, Chair of the ACCESS program Steering Committee and Clinical Professor of Medicine, Univ. of Texas, Southwestern Medical Center. “In addition, the tolerability profile of starting at a low dose of 2.5 mg and the slow titration, positions the program ready for Phase 3 studies.”

ACCESS II Study - Evaluating higher doses up to 240 mg
ACCESS II is a randomized, double-blind, placebo-controlled, clinical study of aleniglipron that enrolled 85 adult participants living with obesity or overweight (defined as a BMI of greater than 25 kg/m2) with at least one weight-related comorbidity. The 44-week study was designed to evaluate two higher doses of aleniglipron. Participants started at 5 mg of aleniglipron (or placebo) and followed a 4-week titration schedule up to target doses of 120 mg, 180 mg and 240 mg.

As reported in December 2025, at 36 weeks, each of the three dose cohorts in the ACCESS II study met statistical significance compared to placebo. Results from the primary efficacy estimandⁱ at 44 weeks are as follows:

	Aleniglipron 120 mg	Aleniglipron 180 mg	Aleniglipron 240 mg	Placebo
Mean percent change in body weight at 44 weeks compared to baseline	-13.6	-15.3	-15.0	+1.1
Placebo-adjusted mean percent change in body weight at 44 weeks compared to baseline	-14.7	-16.3	-16.0	-
P-value	p<0.0001	p<0.0001	p<0.0001	-

Aleniglipron demonstrated a tolerability profile consistent with the GLP-1 receptor agonist class following repeated, once-daily dosing of up to 240 mg. As expected for the GLP-1 receptor agonist drug class, the most common AEs were gastrointestinal (GI)-related, and the two most common AEs in the titration phase were nausea and vomiting.

Body Composition Study - Evaluating lower 2.5 mg starting dose
Structure Therapeutics is conducting a randomized, placebo-controlled body composition study that enrolled 71 adult participants to assess the effect of aleniglipron (up to 120 mg) on body fat loss over a 40-week evaluation period. Participants in the aleniglipron treatment arm start at a 2.5 mg dose, and titrate up monthly to a target dose of 120 mg.

Data from a pre-specified interim analysis after a median follow-up of 20 weeks demonstrated that starting at a lower dose of 2.5 mg for the first four weeks supported a manageable tolerability profile with meaningful improvements in AE-related discontinuations compared to what was observed at a starting titration dose of 5 mg in the ACCESS and ACCESS II studies. Additionally, at a 2.5 mg start and after a median follow up of 20 weeks (~ 30 mg titration step) aleniglipron showed a 6.8% weight loss.

ACCESS Open-Label Extension Study - Following randomized 36-week period, evaluating lower 2.5mg starting dose in the placebo crossover arm and efficacy beyond 36 weeks in previously treated participants
Following the 36-week randomized controlled portion of the Phase 2b ACCESS study, participants were provided an option to roll over into the OLE and receive aleniglipron for an additional 36 weeks. A pre-specified interim analysis after a median follow-up of 20 weeks (a total of 56 weeks) demonstrated continuing weight loss in all dose cohorts, with no evidence of weight loss plateau. Patients who received aleniglipron in the three active dose arms during the initial double-blind portion were titrated to a maximum dose of 120mg during the OLE. These patients achieved continued weight loss of up to 16.2% from baseline out to 56 weeks.

Participants who received placebo in the initial double-blind portion transitioned to aleniglipron at a starting dose of 2.5 mg and titrated monthly to a target dose of 120 mg. Initial data from this group of participants after a median follow-up of 20 weeks are consistent with the findings from the body composition study, showing that starting at a 2.5 mg and titrating slowly was associated with a meaningful improvement in key tolerability markers compared to what was observed in the starting 5 mg titration dose in ACCESS and ACCESS II studies.

Aleniglipron Safety
Aleniglipron demonstrated a compelling safety profile in more than 625 participants across all studies. Importantly, to date, there have been no cases of drug-induced liver injury, no persistent liver enzyme elevations, and no QTc prolongation across all aleniglipron studies.

Phase 3 Preparation
Data from ACCESS, ACCESS II, body composition, and the ACCESS OLE studies continue to provide a strong foundation to advance aleniglipron into Phase 3 clinical development. The Company has a Type B End-of-Phase 2 meeting with the United States Food and Drug Administration (FDA) scheduled in the second quarter of 2026 to finalize the Phase 3 design, which is currently designed with a starting titration dose of 2.5 mg with the intent to evaluate multiple doses up to 240 mg. Structure Therapeutics anticipates initiating the Phase 3 program in the second half of 2026.

Conference Call and Webcast Information
Structure Therapeutics will host a conference call and webcast today, March 16, 2026 at 8:30 a.m. Eastern Time. A live webcast of the call will be available on the Investor Relations page of Structure Therapeutics’ website at https://ir.structuretx.com/events-presentations/events. To access the call by phone, participants should visit this link to receive dial-in details. The webcast will be made available for replay on Structure Therapeutics’ website beginning approximately two hours after the live event. The replay of the webcast will be available for 90 days.

About Aleniglipron and Structure Therapeutics’ Oral Metabolic Franchise
Aleniglipron (GSBR-1290) is an investigational orally-available, small molecule agonist of the glucagon-like-peptide-1 (GLP-1) receptor, a validated drug target for the treatment of obesity and type 2 diabetes mellitus (T2DM). Through Structure Therapeutics’ structure-based drug discovery platform, aleniglipron was designed to be a biased G Protein-Coupled Receptor (GPCR) agonist, which selectively activates the G-protein signaling pathway. Beyond aleniglipron, Structure Therapeutics is developing next generation oral small molecules including amylin receptor agonists, and other combination GLP-1 receptor agonists candidates such as glucose-dependent insulinotropic polypeptide (GIP), glucagon and apelin oral small molecules.

About Structure Therapeutics
Structure Therapeutics is a science-driven clinical-stage biopharmaceutical company focused on discovering and developing innovative oral small molecule treatments for chronic metabolic conditions with significant unmet medical needs. Utilizing its next generation structure-based drug discovery platform, the Company has established a robust GPCR-targeted pipeline, featuring multiple wholly-owned proprietary clinical-stage oral small molecule compounds designed to surpass the scalability limitations of traditional biologic and peptide therapies and be accessible to more people living with obesity around the world. For additional information, please visit www.structuretx.com.

Forward Looking Statements
This press release contains “forward-looking statements” within the meaning of the “safe harbor” provisions of the Private Securities Litigation Reform Act of 1995. All statements other than statements of historical fact are statements that could be deemed forward-looking statements, including, without limitation, statements concerning: the Company’s future plans and prospects; any expectations regarding the potential benefits, tolerability and safety profile, accessibility, scalability, combinability, capability, efficacy, convenience, expected effects and future application of aleniglipron; the belief that data to date from the ACCESS, ACCESS II, body composition, and the ACCESS OLE studies support and inform advancement of the Phase 3 clinical development of aleniglipron; the belief that aleniglipron represents a potentially best-in-class oral small molecule GLP1 and may be a backbone therapy for obesity; the expected timing for the meeting with the FDA to finalize the Phase 3 trial design and the Phase 3 program initiation of aleniglipron; any presumption that topline, interim or preliminary data will be representative of final data or data in later clinical trials; and the belief that the results from ACCESS program represent a promising advance in the therapeutic landscape and brings the Company closer to a future where people living with obesity have multiple, accessible options to address their needs. In addition, when or if used in this press release, the words and phrases “anticipated,” “believe,” “expect,” “may,” “on track,” “plan,” “potential,” “suggests,” “to be,” “to begin,” “will,” and similar expressions and their variants, as they relate to the Company may identify forward-looking statements. Forward-looking statements are neither historical facts nor assurances of future performance. Although the Company believes the expectations reflected in such forward-looking statements are reasonable, the Company can give no assurance that such expectations will prove to be correct. Readers are cautioned that actual results, levels of activity, safety, performance or events and circumstances could differ materially from those expressed or implied in the Company’s forward-looking statements due to a variety of risks and uncertainties, which include, without limitation: risks and uncertainties related to topline results that the Company reports are based on preliminary analysis of key efficacy and safety data, and such data may change following a more comprehensive review of the data related to the clinical trial and such topline data may not accurately reflect the complete results of a clinical trial, the preliminary nature of the results due to the length of the study and sample size and the results from earlier clinical studies not necessarily being predictive of future results; the reported efficacy and safety data is not based on head-to-head studies and therefore may not be comparable to other oral or injectable GLP-1’s due to differences in study design, participant characteristics and how companies quantify or qualify eligibility criteria, and how results are recorded; aleniglipron is in clinical development and even if the Company is successful in obtaining regulatory approval, there can be no guarantees that aleniglipron will outperform other therapies in terms of efficacy or tolerability; potential delays in the commencement, enrollment and completion of the Company’s planned Phase 3 clinical program and other clinical studies, whether as a result of feedback from the End-of-Phase 2 meeting with FDA or otherwise; the Company’s ability to advance aleniglipron, ACCG-2671, ACCG-3535, ANPA-0073, LTSE-2578, and its other therapeutic candidates, obtain regulatory approval of, and ultimately commercialize the Company’s therapeutic candidates; competitive products or approaches limiting the commercial value of the Company’s product candidates; the timing and results of preclinical and clinical studies; the Company’s ability to fund development activities and achieve development goals; the Company's reliance on third parties, including clinical research organizations, manufacturers, suppliers and collaborators, over which it may not always have full control; general geopolitical and macroeconomic conditions, including as a result of tariffs and various global conflicts; the Company’s ability to protect its intellectual property; and other risks and uncertainties described in the Company’s filings with the Securities and Exchange Commission (SEC), including the Company’s latest Annual Report on Form 10-K and future reports the Company may file with the SEC from time to time. All forward-looking statements contained in this press release speak only as of the date on which they were made and are based on management’s assumptions and estimates as of such date. The Company undertakes no obligation to update such statements to reflect events that occur or circumstances that exist after the date on which they were made, except as required by law.

Investors:
Corey Davis, Ph.D.
LifeSci Advisors, LLC
212-915-2577
cdavis@lifesciadvisors.com

Jun Yoon
Structure Therapeutics Inc.
ir@structuretx.com

Media:
Dan Budwick
1AB
Dan@1abmedia.com

_________________________

ⁱ The primary efficacy estimand represents efficacy had all randomized participants remained on study treatment (with possible dose interruptions and/or dose modifications) for 44 weeks without initiating rescue weight management treatments or surgeries.

FAQ

What topline weight-loss results did Structure Therapeutics (GPCR) report for aleniglipron in ACCESS II on March 16, 2026?

Aleniglipron produced placebo-adjusted mean weight loss of 16.3% (180 mg) and 16.0% (240 mg) at 44 weeks. According to Structure Therapeutics, these results were statistically significant (p<0.0001) and represent the highest efficacy reported for an oral GLP-1RA to date.

How did the ACCESS OLE and body composition studies affect tolerability and discontinuation rates for GPCR's aleniglipron?

Starting at a 2.5 mg dose reduced AE-related discontinuations to 2.0–3.4% in interim analyses. According to Structure Therapeutics, median follow-up was 20 weeks and lower starting dose materially improved tolerability during titration versus a 5 mg start.

What safety signals did Structure Therapeutics (GPCR) report across all aleniglipron studies as of March 16, 2026?

No drug-induced liver injury, no persistent liver enzyme elevations, and no QTc prolongation were reported across >625 participants. According to Structure Therapeutics, the overall safety profile was consistent with the GLP-1RA class and appropriate for chronic use.

When is Structure Therapeutics (GPCR) meeting the FDA and when will Phase 3 for aleniglipron begin?

A Type B End-of-Phase 2 meeting with the FDA is scheduled in Q2 2026, and Phase 3 initiation remains planned for 2H 2026. According to Structure Therapeutics, Phase 3 design contemplates a 2.5 mg start and evaluation of doses up to 240 mg.

What efficacy trend did ACCESS II and OLE show for aleniglipron through 56 weeks for GPCR investors?

Data showed continued weight loss with no apparent plateau through 56 weeks, including up to 16.2% loss (120 mg) in OLE. According to Structure Therapeutics, both ACCESS II and OLE demonstrated ongoing weight reduction beyond 36 weeks.