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Development Safety Update Report (DSUR) — GLPI-103

July 12, 2026

📚 Part of the GLPI-103 Regulatory Dossier — Reader's Guide. This article shows the live document; edits to the source appear here automatically.

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Mock / simulation document

This is a mock / simulation document, made for a portfolio and for learning. The drug (GLPI-103), the sponsor, the people, and the data are all fictional. It is not a real regulatory submission and has no clinical, legal, or regulatory standing. What is real is the shape of the thing — the document structure, the standards it follows, and the analysis methods; the content inside is illustrative.

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About this document — a plain-language guide

What it is. The Development Safety Update Report — the annual safety report while a drug is still in clinical development.

Why it exists. ICH E2F requires sponsors to review and report the evolving safety profile of an investigational drug once a year to all regulators. The DSUR summarizes exposures, serious events, and any changes to the risk understanding across all ongoing trials.

How it is produced here. It is a pharmacovigilance ('drug safety watch') document: it gathers and interprets the simulated safety data on the fixed schedule regulators expect once a drug enters development or the market.

Format & governing standard.


Development Safety Update Report (DSUR) — GLPI-103

FieldValue
Document IDDSUR-001
Version1.0
StatusFinal (portfolio)
DSUR reporting intervalDevelopment International Birth Date (DIBD) + 12 months [MOCK]
CompoundGLPI-103 (GLP-1 / Apelin [APJ] receptor dual agonist)
SponsorVirtual Biopharma Inc.
Standard(s)ICH E2F · E2A · E6(R3) · CIOMS
ConfidentialityConfidential

[MOCK — deep-knowledge assumption] Annual Development Safety Update Report covering the GLPI-103 clinical development program. Pivotal Phase 3 figures trace to CSR-301 (outputs/); early-phase content is illustrative.

Change History

VersionDateAuthorSummary
1.02026-06-30PharmacovigilanceInitial DSUR (annual)

1. Introduction

This DSUR presents a comprehensive, thoughtful annual review and evaluation of safety information for GLPI-103 collected during the reporting period across the development program, prepared per ICH E2F. GLPI-103 is an investigational dual GLP-1/APJ receptor agonist in development for type 2 diabetes mellitus (T2DM).

2. Worldwide Marketing Approval Status

GLPI-103 is investigational and not approved in any country; it is under clinical development under IND (US), CTA/IMPD (EU), and IND (KR) [MOCK].

3. Actions Taken for Safety Reasons

No clinical-trial suspensions, terminations, protocol modifications for safety, dosing changes, or restrictions were taken during the reporting period. Routine titration/dose-modification provisions for gastrointestinal tolerability operated as designed (PROT-301 §6).

4. Changes to Reference Safety Information (RSI)

The Investigator's Brochure RSI (IB-001 §7) was reviewed; the listed expected events (gastrointestinal events, injection-site reactions, hypoglycaemia with secretagogues) remain current. The class boxed-warning risks (thyroid C-cell/MTC, pancreatitis) continue to be managed by labeling and the RMP.

5. Inventory of Clinical Trials Ongoing/Completed in the Period

StudyPhaseStatusNNotes
GLPI103-101 (SAD)1Completed40Healthy volunteers
GLPI103-102 (MAD)1bCompleted40T2DM/prediabetes
GLPI103-201 (PoC)2Completed240Dose-finding
GLPI103-301 (pivotal)3Completed900Active-controlled

6. Estimated Cumulative Exposure

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Why exposure is tallied every year

The DSUR is the annual safety check-up while the drug is still investigational. Cumulative exposure — how many subjects, for how long, across all trials — is the denominator that gives the year's safety findings meaning.

Cumulative investigational exposure across the program is approximately 1,220 subjects (40+40+240+900), with up to 52 weeks of exposure in the pivotal study; healthy-volunteer and patient exposure are summarised separately [MOCK].

7. Data in Line Listings and Summary Tabulations

Serious adverse events and adverse events of special interest are presented as cumulative interval line listings and summary tabulations (appendices [MOCK]). In the pivotal study, 10 serious adverse events and 2 deaths were reported, none assessed as treatment-related (CSR-301 §12.5).

8. Significant Findings in the Period

  • Efficacy-tolerability: dose-related gastrointestinal events (notably nausea, higher in the higher-exposure intravenous arm: 32.3% vs 21.4% comparator) — consistent with the GLP-1 class and managed by titration.
  • Nonclinical: the 2-year rat carcinogenicity thyroid C-cell finding was investigated and characterised as rodent-specific/low human relevance (M4-2.3; QA-003 ISS-012); carried as a labeled class risk.
  • No new or unexpected serious safety signal was identified during the period.

9. Late-Breaking Information

None.

10. Overall Safety Assessment and Conclusion

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The yearly verdict

The report ends with a plain judgement: does anything learned this year change the understanding of the drug's safety, and does the benefit-risk balance still support continuing? That conclusion is the point of the whole exercise.

The cumulative safety profile of GLPI-103 remains consistent with the GLP-1 receptor agonist class and clinically manageable, with a gastrointestinal tolerability trade-off in the higher-exposure formulation addressed by titration, infrequent hypoglycaemia, no hepatotoxicity signal (eDISH; no Hy's-law cases), and class risks (MTC, pancreatitis) managed by labeling and the RMP. The benefit-risk for continued development and the marketing application remains favourable (M2.5.6). No changes to the RSI or risk-minimization measures are warranted at this time.

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