Back to List
TMF0 Views

Safety Management Plan (SMP) — GLPI103-301

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.

🧪
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.

📄
About this document — a plain-language guide

What it is. The Safety Management Plan — how adverse events are collected, assessed, and reported during the trial.

Why it exists. Serious adverse events must be captured and expedited to regulators within strict timelines (ICH E2A). This plan defines definitions, causality assessment, and the reporting workflow that keeps subjects and regulators informed.

How it is produced here. It is an operational trial document — a plan, charter, or template of the kind kept in the Trial Master File. It describes how the trial is run, rather than reporting the trial's results.

Format & governing standard. ICH E2A; E6(R3); E2D; CIOMS; 21 CFR 312.32; EU CTR 536/2014


Safety Management Plan (SMP) — GLPI103-301

FieldValue
Document IDTMF-SMP
Version2.0
StatusFinal
Study No.GLPI103-301
SponsorVirtual Biopharma Inc.
StandardICH E2A; E6(R3); E2D; CIOMS; 21 CFR 312.32; EU CTR 536/2014
ConfidentialityConfidential — TMF

Change History

VersionDateAuthorSummary of Change
1.02026-06-29PharmacovigilanceInitial SMP
2.02026-07-05PharmacovigilanceFull — severity/causality definitions, special situations, unblinding, and expedited-reporting matrix

1. Definitions and Collection

Adverse events (AE) and serious adverse events (SAE) are defined per ICH E2A. Treatment-emergent AEs (TEAE) are those with onset on or after the first dose. For each event the site records severity (mild/moderate/severe), causality (related/not related to investigational product), seriousness, action taken, and outcome, on the CRF (CRF-301), standardized to the SDTM AE domain and MedDRA-coded.

AttributeCategoriesNotes
SeverityMild / Moderate / Severeintensity, not seriousness
SeriousnessDeath · life-threatening · hospitalization/prolongation · disability · congenital anomaly · other medically importantany one criterion = SAE
CausalityRelated / Not relatedinvestigator's clinical judgement; sponsor may upgrade
ExpectednessExpected / Unexpectedvs Reference Safety Information (IB-001 §7)

2. Adverse Events of Special Interest (AESI)

Gastrointestinal events; acute pancreatitis; thyroid C-cell neoplasia (MTC/MEN2); hypoglycaemia; and cardiovascular/heart-rate effects (APJ mechanism) — each with a targeted follow-up questionnaire and, where relevant, adjudication (PROT-301 §10; RMP suite).

3. SAE and Expedited Reporting

Sites report SAEs to the sponsor within 24 hours of awareness. The sponsor assesses seriousness, causality, and expectedness and performs expedited regulatory/ethics reporting to the timelines below.

EventAssessmentRegulatory timeline
Fatal/life-threatening SUSARserious + related + unexpected7 calendar days (initial), 8 days follow-up
Other SUSARserious + related + unexpected15 calendar days
Other SAEsseriousper protocol/aggregate (DSUR)
Safety issues affecting benefit–riskurgentwithout delay to authorities/IECs

Expedited reports follow CIOMS/E2B(R3); expectedness is judged against the IB Reference Safety Information (IB-001 §7).

4. Special Situations

Pregnancy and lactation (report and follow to outcome; treatment stopped), overdose, medication error, lack of efficacy with clinical consequence, occupational exposure, and suspected transmission of an infectious agent are collected and reported per E2D even when not otherwise meeting SAE criteria.

5. Unblinding for Safety

Emergency unblinding is available via the IWRS (TMF-RAND) when knowledge of treatment is essential for participant management. Unblinding events are documented; for SUSAR reporting the sponsor unblinds only the affected case as required, preserving the study blind otherwise.

6. Reconciliation and Oversight

SAE reconciliation between the clinical and safety databases is completed before database lock. An independent DSMB provides periodic unblinded safety oversight per its charter (TMF-DSMB), and can recommend modification or stopping.

7. Signal Detection and Periodic Reporting

Ongoing signal detection (Signal Management Plan, SIGNAL-001) and periodic aggregate reporting — DSUR during development (DSUR-001) and PSUR/PBRER post-authorization (PSUR-001) — are performed consistent with the RMP suite (RMP-EU/US/KR).

Comments (0)

No comments yet. Be the first to say something!