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Module 2.7.6 — Synopses of Individual Studies

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. Structured synopses of each individual clinical study in the program.

Why it exists. Before a reviewer opens a full study report in Module 5, Module 2.7.6 offers a standardized one-to-few-page synopsis of each study — design, population, and key results — as a quick reference and index.

How it is produced here. It contains no new data. It is a distillation — it gathers, summarizes, and cross-references the underlying study reports and datasets into the shorter form a regulator reads first.

Format & governing standard. ICH M4E(R2) §2.7.6


Module 2.7.6 — Synopses of Individual Studies

FieldValue
Document IDM276
Version1.0
CompoundGLPI-103 (GLP-1/APJ dual agonist)
StandardICH M4E(R2) §2.7.6
ConfidentialityConfidential

One-page synopsis per clinical study. Pivotal figures trace to outputs/ (reconciled); early-phase [MOCK].

Change History

VersionDateAuthorSummary
1.02026-06-29ClinicalInitial synopses

GLPI103-101 (Phase 1, SAD) — CSR-101

Randomized, DB, placebo-controlled single ascending dose in 40 healthy volunteers (5 cohorts × 8; 6:2). Objectives: safety, tolerability, PK; PD (plasma apelin). Result [MOCK]: no dose-limiting toxicity; ~dose-proportional PK; long half-life supporting QW dosing.

GLPI103-102 (Phase 1b, MAD) — CSR-102

Randomized, DB, placebo-controlled multiple ascending dose, ≤12 weeks, in 40 overweight/obese adults with T2DM/prediabetes (4 cohorts × 10; 8:2). Result [MOCK]: titration-manageable GI AEs; dose-dependent HbA1c (−0.8%) and weight (−3 kg); favourable NT-proBNP/hsCRP.

GLPI103-201 (Phase 2, dose-finding) — CSR-201

Randomized, DB, placebo-controlled, 4 arms (PBO + low/med/high), 24 weeks, 240 T2DM on metformin. Primary: HbA1c CFB. Result [MOCK]: monotonic dose–response; dose-dependent weight loss; GI AEs dose-related. Supported Phase 3 doses (Gate-3 decision; PM-002).

GLPI103-301 (Phase 3, pivotal) — CSR-301

Randomized, DB, double-dummy, active-controlled (vs oral semaglutide), 1:1:1, 52 weeks, 900 randomized to target (IV 300 / Oral 301 / Sema 299; 1,700 screened) T2DM inadequately controlled on metformin. Primary: HbA1c CFB at Week 52.

  • Result: superiority — IV −0.68% (95% CI −0.81, −0.55; p<0.001), Oral −0.34% (−0.47, −0.21; p<0.001); LS means −2.57 / −2.23 / −1.89.
  • Secondary: weight −14.5 / −10.3 / −7.6 kg; ≥10% weight loss 100.0 / 83.0 / 44.2%; HbA1c <7.0% 94.1 / 94.6 / 86.2%.
  • Safety: any TEAE 75.7 / 67.8 / 72.2%; nausea higher with IV (32.3% vs 21.4%, p=0.003); 10 SAEs, 2 deaths; discontinuation 9.3%.
  • Conclusion: superior efficacy with a class-consistent, manageable safety profile.

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