Domain 03 · foundation · clinical trials

Clinical trials: the full study lifecycle.

Clinical trials are where the molecule meets the patient under the regulator's watch. The discipline of designing, executing, monitoring, and submitting studies that produce evidence both scientifically and ethically defensible. Phase I–IV, ICH-GCP, the rising structured-protocol era of ICH M11, the operational shift toward decentralised and adaptive designs.

Open the chapters → See the methodology
Anchor: ICH-GCP E6(R3) Structure: ICH M11 Quality system: ICH E8(R1) / E9
Library/Clinical Trials
Clinical trials Overview Pillars Substrate History · Evolution Current 2026 Future 2026-2035 AI lens Flow of trials Players & stakeholders Notes
/ 00

What a clinical trial looks like, end-to-end.

Phase I–IV · adaptive · decentralised

A clinical trial is the regulator-witnessed sequence by which a molecule earns the right to reach patients. Phase I establishes safety. Phase II finds efficacy signal. Phase III is pivotal — the regulator-facing evidence. Phase IV is post-market reality. The operational shift ICH E6(R3) calls for is here: adaptive designs branch off the traditional sequence, and decentralised elements move trial activity off-site to where the patient actually lives.

/ 1 · Decentralised / 2 · Phase I → IV (sample size = width) / 3 · Adaptive site patient home remote e-consent wearable tele-visit DCT · investigator site + remote patient touchpoints Phase I n ≈ 20–80 · safety Phase II n ≈ 100–300 · efficacy signal Phase III n ≈ 1000–3000 · pivotal · regulator-facing Phase IV n ≈ 10000s · post-market · real-world evidence gate phase progression — molecule → patient Adaptive MAMS multi-arm multi-stage Seamless II/III combined Bayesian dose-finding adaptive elements · branch off Phase II / regulatory framework ICH-GCP E6(R3) Step 4 · 6 Jan 2025 ICH M11 structured protocol RBQM risk-based monitoring CONSORT 2025 reporting standard EU CTR · FDA · MHRA multi-jurisdictional
/ At a glance

The iFeed.clinical-trials reference, in headlines.

2026-05-02 · live
Phase architecture

I → IV.

First-in-human · proof of concept · pivotal confirmation · post-marketing. The phase logic has held since the 1960s. What changes per decade is the operational layer underneath.

Anchor regulation

ICH E6(R3).

Step 4 endorsement on 6 January 2025. Twelve overarching principles. Annex 1 (Interventional) Step 4. Annex 2 (Non-traditional designs) in development. Structural rewrite, not an addendum.

Regulators

7 anchored.

ICH E6(R3) · FDA 21 CFR 312/50/56 · EMA Reg (EU) 536/2014 + CTIS · PMDA J-GCP · CDSCO NDCT 2019 · MHRA UK CTR · Health Canada Division 5.

GCP pillars

9 dimensions.

Informed consent · IRB/IEC · investigator qualification · monitoring (RBM) · data integrity (ALCOA+) · safety reporting (E2A/E2B) · TMF · source documentation · computerised systems.

/ Connection

This domain connects to three.

Clinical trials don't sit alone

Clinical trials run on the bioanalytical spine for PK and biomarker measurement and share ICH-GCP discipline with bioequivalence. Governance gates everything. Click a node to open that space.

Bio analytical Bio equivalence Clinical trials Governance
/ Chapters

Nine chapters · open any.

Each chapter is its own page · secondary nav above
Chapter 01 · flagship

Pillars: cross-regulator GCP comparison.

ICH E6(R3) Step 4 (Jan 2025) · 12 overarching principles · Annex 1 interventional · Annex 2 non-traditional. FDA 21 CFR 312/50/56 · EMA CTR 536/2014 + CTIS · PMDA J-GCP · CDSCO NDCT 2019 · MHRA UK CTR · Health Canada Division 5.

Open chapter →
Chapter 02 · operational layer

Trial substrate.

Trial sites (academic + private + DCT). EDC ecosystems (Veeva Vault CDB, Medidata Rave, OpenClinica, Castor). CTMS · eTMF (TMF Reference Model 3.3) · eConsent · ePRO/eCOA · IxRS/RTSM. CRO landscape large vs niche.

Open chapter →
Chapter 03 · the multi-decade arc

History & evolution.

Nuremberg Code 1947 · Helsinki 1964 · Belmont 1979 · ICH-GCP E6(R1) 1996 · Reed Decision · ICH E6(R2) 2016 risk-based monitoring · ICH E6(R3) Step 4 January 2025 the structural reframe.

Open chapter →
Chapter 04 · live now

Current state: 2026.

ICH E6(R3) operative since January 2025. EU Clinical Trials Regulation (EU) 536/2014 fully applicable since 31 Jan 2022; CTIS mandatory 31 Jan 2023; legacy Directive 2001/20/EC trials transition completed 31 Jan 2025. FDA DCT final guidance (17 Sep 2024). India ICH Observer (CDSCO). ICH M11 (Step 4 19 Nov 2025).

Open chapter →
Chapter 05 · projection

Future scope: 2026-2035.

Decentralised-default trial design. Synthetic control arms accepted as supportive evidence. In-silico evidence packages. N-of-1 protocol patterns. ICH E6(R4) on the horizon. Continuous-submission paradigm. Climate · sustainability metrics on the regulator agenda.

Open chapter →
Chapter 06 · validation surface

AI in clinical trials.

Patient recruitment models. Site-selection ML. ICH M11 structured-protocol authoring assist. Risk-based monitoring optimisation. Adverse-event signal detection. PCCP framework relevance. EU AI Act Annex III high-risk classification of trial-conduct AI.

Open chapter →
Chapter 07 · operational pipeline

Flow of a clinical trial.

Protocol design → regulatory submission → IRB/IEC review → site selection → SIV → first-patient-in → enrolment → conduct · monitoring · SAE reporting → LPLV → database lock → analysis → CSR → submission. Sequential and gated.

Open chapter →
Chapter 08 · who runs the field

People: use cases, players, stakeholders.

Eight regulatory triggers (Phase I FIH, pivotal Phase III, post-marketing, biosimilar, paediatric, RWE, gene-therapy LTFU, decentralised pilots). Five player categories: sponsors, CROs, sites/PIs, regulators, IRBs. Stakeholder map.

Open chapter →
Chapter 09 · the living feed

Notes: clinical-trials writing.

The feed of writing relevant to clinical-trials practice. ICH E6(R3) principles-based GCP, ICH M11 structured protocols, AI in trial design and conduct. Filtered from the global notes archive.

Open chapter →
/ 01

The four phases.

Drug development arc

The phase architecture has held since the 1960s. What changes in the AI-native era is not the phases — it's the operational layer underneath them. Recruitment, monitoring, data capture, signal detection: each of these is being reshaped while the phase logic remains.

/ Phase I

First-in-human.

Healthy volunteers (mostly). Safety, tolerability, PK, dose-escalation. The first time the molecule meets the population.

Subjects 20–100Duration months
/ Phase II

Proof of concept.

Patients with the target indication. Efficacy signal, dose selection, expanded safety. Pivotal go/no-go decision point.

Subjects 100–500Duration 1–2 yrs
/ Phase III

Pivotal confirmation.

Large, randomised, controlled. Confirmation of efficacy, comprehensive safety database, label-ready evidence package.

Subjects 1k–5k+Duration 2–5 yrs
/ Phase IV

Post-marketing.

Real-world evidence, long-term safety, expanded indications, comparative effectiveness. The lifecycle continues after approval.

Subjects variableDuration ongoing
/ 02

Operations lifecycle.

Start-up → closure

The operational arc of any clinical study is six stages. Each produces specific deliverables. Each has named regulator-facing artefacts. Each is where AI is reshaping the work most visibly.

/ 01
Start-up.

Site selection, ethics approval, regulatory submission, contracting.

/ 02
Recruitment.

Patient identification, screening, randomisation, enrolment.

/ 03
Conduct.

Visit execution, data capture, sample collection, IMP management.

/ 04
Monitoring.

Source data verification, risk-based monitoring, safety surveillance.

/ 05
Analysis.

Database lock, statistical analysis, CSR drafting, regulatory submission.

/ 06
Closure.

TMF closure, audit/inspection-readiness, archive, retrospective.

/ 03

ICH framework.

The substrate the operations sit on
ICH-GCP E6(R3)
Good Clinical Practice. The foundational guideline. R3 modernises for risk-based, decentralised, AI-augmented trials. Step 4 reached 2025.
2025
ICH E8(R1)
General Considerations for Clinical Trials. Quality-by-design framework. The "fit-for-purpose" architecture for trial design.
2021
ICH E9 / E9(R1)
Statistical Principles + estimands framework. The statistical substrate for trial design and analysis. Estimands re-orient the analysis around the question being asked.
live
ICH M11
Clinical Study Protocol Template (structured). Machine-readable protocol structure. AI-readable substrate for trial design.
2025+
ICH E2A–F
Pharmacovigilance + safety reporting suite. Adverse event handling, periodic reporting, signal detection. Critical for AI-augmented PV.
live
ICH E17
Multi-regional clinical trials. Framework for studies that submit across regions simultaneously. Increasingly common in modern programmes.
2017+
/ 04

Modern shifts.

What the operations are becoming

Three shifts are reshaping clinical operations through 2026 and into 2030. Each is regulator-acknowledged. Each requires the immunity layer iFeed builds.

/ Shift 01

Decentralised trials (DCT).

Visits move from sites to homes. Wearables, ePRO, telehealth. ~30% of new starts in 2026 use DCT components. The data-integrity question shifts shape.

/ Shift 02

Adaptive · seamless designs.

Phase II/III seamless designs, basket and umbrella studies, response-adaptive randomisation. Statistical sophistication now table-stakes for oncology and rare disease.

/ Shift 03

AI-assisted operations.

Patient identification, protocol drafting, eTMF organisation, signal detection, regulatory dossier preparation. The validation layer is the bottleneck, not the capability.

/ 05

The GCP pillars · cross-regulator comparison.

5 regulators · 9 GCP pillars

Nine pillars define the operational shape of a defensible GCP programme — from sponsor oversight through trial master file. Below: a quick-reference grid · then a colour-coded drilldown comparing ICH E6(R3) · FDA · EMA · MHRA · PMDA on each. Sponsor oversight (★), decentralised trial elements (★), and electronic systems (★) are where divergence runs deepest in 2026.

Quick reference · the nine GCP parameters.

/ 5.1
Principles of GCP.

ICH E6(R3) Step 4 (Jan 2025) · principle-based framework · 12 overarching principles · structural rewrite (not addendum) · quality-by-design from protocol inception · participant-centric language explicit.

/ 5.2
Sponsor oversight.

Risk-based quality management · sponsor responsibility for trial integrity · vendor oversight expansion · proportionate (not universal) monitoring. R3 raises the bar; FDA/EMA implementation guidance still maturing 2025–2026.

/ 5.3
Investigator responsibilities.

Qualifications · IB receipt · protocol adherence · delegation log · safety reporting timelines. 21 CFR 312.60-69 (FDA) operationalises; ICH E6(R3) principle-based; PMDA per-site GCP Ordinance.

/ 5.4
Informed consent.

Process, documentation, vulnerable populations · 21 CFR 50 Subparts B/D (FDA) · CTR Annex I (EMA) · Helsinki/Belmont substrate · remote consent now permitted across most regulators post-COVID.

/ 5.5
Protocol & amendments.

IRB/IEC submission, protocol deviations, substantial amendment classification. CTR substantial-modification regime via CTIS; FDA IND amendments via 21 CFR 312.30; PMDA pre-consultation heavy.

/ 5.6
Risk-based monitoring.

RBM, central monitoring, on-site, source data verification (SDV). E6(R2) introduced; E6(R3) makes proportionate monitoring default. Pre-R3 universal-SDV practice now reads as out-of-compliance.

/ 5.7
Electronic systems & data integrity.

ICH E6(R3) Annex on computerised systems · EU Annex 11 (computerised systems) · 21 CFR Part 11 (e-records / e-sigs) · PMDA ER/ES guidance. Validation expectations diverge between FDA Part 11 and EU Annex 11 detail level.

/ 5.8
Decentralised trial elements.

DCT/hybrid · FDA DCT final guidance · 'Conducting Clinical Trials with Decentralized Elements' (17 September 2024) · EMA 2022 recommendation paper updated 2024 · MHRA combined-review DCT-friendly · PMDA cautious (remote consent under conditions). The deepest 2026 divergence on operational substance.

/ 5.9
Trial Master File (TMF).

eTMF structure · DIA TMF Reference Model v3.x · archiving timelines (typically 25 years EU CTR, 2 years post-marketing FDA) · inspection-readiness as continuous state, not endpoint.

Cross-regulator comparison · ICH E6(R3) · FDA · EMA · MHRA · PMDA.

ICH E6(R3) FDA EMA / CTR MHRA PMDA
/ 5.1 Principles of GCP.ICH E6(R3) Step 4 (Jan 2025) · principle-based framework · 12 overarching principles. +
At a glance · convergence vs divergence
CONVERGE
All five regulators recognise ICH E6 lineage. R3 (Jan 2025) is a structural rewrite (not an R2 addendum) carrying 12 overarching principles, Annex 1 (interventional) Step 4, and Annex 2 (non-traditional designs) in development.
DIVERGE
Implementation pace differs: EMA adopted 2025 · MHRA aligned · FDA draft 2025, final late 2026 · PMDA GCP Ordinance amendment 2026–2027. ANVISA RDC 945/2024 high-alignment with R3 spirit; CDSCO India still primarily E6(R2) but R3 alignment in progress.
ICH E6(R3)Jan 2025
Step 4 · structural rewrite
12 overarching principles · Annex 1 interventional · Annex 2 non-traditional in development · participant-centricity explicit.
Acceptance criteria12 principles · Annex 1 + Annex 2
FDA2025–2026
Draft 2025 · final late 2026
FDA draft implementation guidance 2025 · final expected late 2026 · 21 CFR 50/56/312/812 baseline persists.
Acceptance criteria21 CFR 50/56/312/812 + R3
EMA / CTRAdopted 2025
CTR 536/2014 + R3 adopted
EMA adopted R3 in 2025 · CTR 536/2014 + CTIS submission framework + R3 GCP framework integrated.
Acceptance criteriaCTR + R3 adopted
MHRA2025
UK CTR · R3 aligned
MHRA aligned with R3 in 2025 · UK Clinical Trials Regulation post-Brexit framework + combined review.
Acceptance criteriaUK CTR + R3 aligned
PMDA2026–2027
GCP Ordinance amendment
PMDA GCP Ordinance amendment 2026–2027 · pre-consultation-heavy pathway persists · per-site IRB with central pilots.
Acceptance criteriaGCP Ordinance + R3 in progress
/ 5.2 Sponsor oversight & quality management.Risk-based · vendor oversight · proportionate monitoring · the R3 reset. +
At a glance · convergence vs divergence · the R3 reset pillar
CONVERGE
All accept sponsor as ultimately accountable for trial integrity · vendor oversight expanded vs E6(R2) · quality-by-design from protocol inception · proportionate (not universal) monitoring as the R3 default.
DIVERGE
FDA Bioresearch Monitoring (BIMO) retains sponsor-investigator inspection paradigm · EMA via Reporting Member State with parallel Concerned Member State view · MHRA combined-review single-process. PMDA pre-consultation expectations heaviest. ANVISA RDC 945 streamlines parallel CONEP/CEP.
ICH E6(R3)Jan 2025
Annex 1 · quality by design
Annex 1 §3 sponsor oversight · vendor oversight explicit · quality-by-design from protocol · proportionate monitoring default.
Acceptance criteriaQbD · vendor oversight · proportionate monitoring
FDA21 CFR 312
BIMO inspection paradigm
21 CFR 312.50-58 sponsor responsibilities · BIMO inspection of sponsor + investigator + IRB · vendor oversight via 21 CFR 312.52.
Acceptance criteria21 CFR 312.50-58 · BIMO inspectable
EMA / CTR2022 live
RMS / CMS · Part I/II
Reporting Member State Part I assessment · Concerned Member State parallel view · CTIS public disclosure default · sponsor accountable across MS.
Acceptance criteriaRMS-led · CTIS public disclosure
MHRAUK CTR
Combined review · single process
UK Combined Review (regulatory + ethics in one process) · sponsor oversight per UK CTR · risk-adapted monitoring favoured.
Acceptance criteriaCombined review · risk-adapted
PMDAGCP Ord.
Pre-consultation heavy
Pre-CTN consultation is the real driver · sponsor expected to engage PMDA scientifically before formal submission · per-site IRB.
Acceptance criteriaPre-CTN consultation · per-site IRB
Inspector's eye
Pre-2024 universal-SDV monitoring plans now read as out-of-compliance with R3's proportionate-monitoring default. Document the risk assessment that justifies the monitoring intensity per CRF section · auditors trace a missing risk assessment as the audit-trigger keyword. For PMDA-bound programmes, the pre-CTN consultation record is itself a sponsor-oversight artefact.
/ 5.3 Investigator responsibilities.Qualifications · IB receipt · protocol adherence · delegation log. +
At a glance · convergence vs divergence
CONVERGE
All require qualified investigator, current IB receipt, protocol adherence with documented deviations, delegation log, and timely safety reporting. ICH E6(R3) Annex 1 §4 codifies the principle set.
DIVERGE
FDA 21 CFR 312.60–.69 operationalises with specific Form FDA 1572 commitments. PMDA per-site IRB persists; central IRB pilots only. CTR Part II runs at national level; one vs many ECs per Member State varies. MHRA combined review embeds investigator commitments inside one process.
ICH E6(R3)Jan 2025
Annex 1 §4 · principle-based
Annex 1 §4 investigator responsibilities · participant-centric framing · qualifications, IB receipt, protocol fidelity, deviation handling.
Acceptance criteriaAnnex 1 §4 · delegation log · deviations
FDA21 CFR 312
312.60-69 · Form 1572
21 CFR 312.60–.69 operational specifics · Form FDA 1572 commitment · financial disclosure 312.64.
Acceptance criteriaForm 1572 · financial disclosure
EMA / CTR2022 live
CTR Part II national
Part II national assessment · investigator commitments via national EC processes · one vs many ECs per MS varies.
Acceptance criteriaPart II national · EC commitments
MHRAUK CTR
Combined review · single record
Investigator commitments embedded in combined-review submission · HRA + REC + MHRA single-process record.
Acceptance criteriaCombined review · HRA/REC
PMDAGCP Ord.
Per-site IRB persists
Per-site IRB GCP Ordinance baseline · central IRB pilots only · investigator qualifications closely site-bound.
Acceptance criteriaPer-site IRB · central pilots
/ 5.4 Informed consent.Process · documentation · vulnerable populations · remote consent. +
At a glance · convergence vs divergence
CONVERGE
All trace to Nuremberg (1947) + Helsinki (1964) + Belmont (1979) substrate. All require process-not-form, documentation, vulnerable-population safeguards. Remote consent now permitted across most regulators post-COVID 2020.
DIVERGE
FDA: 21 CFR 50 Subpart B (emergency exception) and Subpart D (children) operationalise specifics. EMA: CTR Annex I + national-level vulnerable-population rules. MHRA: HRA national framework. PMDA: written-consent strict, remote conditional. ANVISA: CONEP/CEP integration via RDC 945.
ICH E6(R3)Jan 2025
Annex 1 §3 + §4 · participant-centric
Annex 1 codifies process-not-form · participant-centric language explicit · remote consent acknowledged.
Acceptance criteriaProcess · documented · remote permitted
FDA21 CFR 50
Subpart B + D operational
21 CFR 50 informed consent · Subpart B emergency exception (1996) · Subpart D children (2001).
Acceptance criteria21 CFR 50 + Subpart B/D
EMA / CTR2022 live
CTR Annex I + national
CTR Annex I consent requirements · vulnerable-population rules national · mandatory lay summary post-trial.
Acceptance criteriaAnnex I · lay summary
MHRAHRA
HRA national framework
HRA national framework · combined-review consent submission · remote consent under specific conditions.
Acceptance criteriaHRA framework · remote conditional
PMDAGCP Ord.
Written-consent strict
Written-consent strict baseline · remote consent permitted under specific conditions · vulnerable-population safeguards via per-site IRB.
Acceptance criteriaWritten-consent · remote conditional
/ 5.5 Protocol & amendments.IRB/IEC submission · substantial amendments · deviations. +
At a glance · convergence vs divergence
CONVERGE
All require IRB/IEC review · substantial-amendment classification · documented deviations · CAPA for systemic deviations.
DIVERGE
FDA IND amendment via 21 CFR 312.30 (3 categories: protocol, IB, new investigator); CTR substantial-modification regime in CTIS, RMS-led with CMS comments; MHRA combined-review handles non-substantial via streamlined process; PMDA pre-consultation strongly preferred for design changes.
ICH E6(R3)Jan 2025
Annex 1 §6 · deviations
Annex 1 §6 protocol · deviations classified by impact · CAPA for systemic deviations.
Acceptance criteriaSubstantial classification · CAPA
FDA21 CFR 312.30
IND amendment · 3 categories
21 CFR 312.30 IND amendment · protocol amendment, IB amendment, new investigator · safety reports separate.
Acceptance criteria3 categories · safety separate
EMA / CTR2022 live
Substantial modification regime
CTR substantial-modification via CTIS · RMS-led assessment with CMS comments · non-substantial notification streamlined.
Acceptance criteriaCTIS substantial mod · RMS-led
MHRAUK CTR
Combined review · streamlined
Combined-review handles substantial and non-substantial via single process · HRA + REC + MHRA aligned timelines.
Acceptance criteriaCombined review · aligned
PMDAGCP Ord.
Pre-consultation preferred
Pre-consultation strongly preferred for design changes · CTN amendment process formal but PMDA expects scientific dialogue first.
Acceptance criteriaPre-consultation · CTN amend
/ 5.6 Risk-based monitoring.RBM · central monitoring · on-site · SDV proportionate. +
At a glance · convergence vs divergence
CONVERGE
E6(R2) introduced risk-based monitoring; E6(R3) makes proportionate monitoring the default. Central monitoring + targeted on-site + risk-targeted SDV converged across all five regulators.
DIVERGE
Pre-R3 universal-SDV (100% SDV) practice persisted longest in PMDA inspection expectations and certain CDSCO submissions. FDA 2013 RBM guidance + EMA 2013 reflection paper aligned earliest. AI-assisted SDV piloting 2024+ but no formal framework yet.
ICH E6(R3)Jan 2025
Proportionate monitoring default
Annex 1 §3 quality management · proportionate monitoring as default · risk assessment documented.
Acceptance criteriaProportionate · risk assessed
FDA2013
RBM guidance · aligned
FDA 2013 risk-based monitoring guidance + 2019 update · central monitoring + targeted on-site combination.
Acceptance criteriaRBM 2013/2019 + R3
EMA / CTR2013
RBM reflection paper · aligned
EMA 2013 risk-based quality management reflection paper · CTR monitoring expectations + R3 alignment.
Acceptance criteriaRBM reflection + R3
MHRAUK CTR
Risk-adapted favoured
Risk-adapted approach historically favoured · MHRA inspection expectations align with R3 default.
Acceptance criteriaRisk-adapted · R3 aligned
PMDAGCP Ord.
SDV practice traditionally heavy
PMDA inspection expectations historically tilt toward heavier SDV · R3 alignment in progress 2026–2027.
Acceptance criteriaHeavy-SDV legacy · R3 in progress
/ 5.7 Electronic systems & data integrity.E6(R3) Annex · EU Annex 11 · 21 CFR Part 11 · PMDA ER/ES. +
At a glance · convergence vs divergence · the e-systems pillar
CONVERGE
All require validated computerised systems for trial data · ALCOA+ data-integrity principles · audit trails · access controls · e-signature integrity.
DIVERGE
21 CFR Part 11 (FDA) is e-records / e-signatures specific with detailed technical controls. EU Annex 11 is computerised-systems-validation specific in pharmaceutical context. PMDA ER/ES guidance closest to Part 11 but Japan-specific. ICH E6(R3) Annex on computerised systems harmonises principles but technical specifics regional.
ICH E6(R3)Jan 2025
Annex on computerised systems
R3 Annex carries computerised-systems-validation principles · ALCOA+ embedded · audit trail expectations.
Acceptance criteriaCSV principles · ALCOA+
FDA21 CFR 11
Part 11 · e-records / e-sigs
21 CFR Part 11 codifies technical controls for e-records and e-signatures · closed/open systems distinction · FDA inspection trace.
Acceptance criteria21 CFR Part 11 technical controls
EMA / EudraLexEudraLex V4
Annex 11 · CSV pharma
EU Annex 11 (EudraLex Volume 4) computerised-systems-validation in pharmaceutical context · supplier audits · periodic review.
Acceptance criteriaEU Annex 11 CSV
MHRA2018 GxP
MHRA GxP Data Integrity
MHRA GxP Data Integrity Guidance (2018) · ALCOA+ explicit · one of the most-cited inspection references globally.
Acceptance criteriaMHRA GxP DI · ALCOA+
PMDAER/ES
ER/ES Japan-specific
PMDA ER/ES guidance closest to Part 11 · Japan-specific implementation · pre-consultation common for new e-systems.
Acceptance criteriaER/ES · pre-consultation
Inspector's eye
Cross-region trials hit two distinct technical bars: 21 CFR Part 11 controls (closed-system audit trail, e-sig binding, system-level access) AND EU Annex 11 controls (validation lifecycle documentation, supplier audit, periodic review). MHRA GxP DI 2018 phrasing is the most-quoted inspection language globally · treat ALCOA+ traceability as the audit-trigger keyword. PMDA pre-consultation on a new EDC or eTMF saves a Japan-specific inspection finding later.
/ 5.8 Decentralised trial elements.DCT/hybrid · FDA 2024 final · EMA 2024 update · the deepest 2026 divergence. +
At a glance · convergence vs divergence · the deepest operational pillar
CONVERGE
All five accept hybrid trials with telemedicine visits, home nursing, ePRO, direct-to-participant IMP. COVID 2020 accelerated; by 2024 all major regulators have written DCT positions.
DIVERGE
FDA DCT final guidance · 'Conducting Clinical Trials with Decentralized Elements' (17 September 2024) · EMA 2022 recommendation paper updated 2024 · MHRA combined-review DCT-friendly · PMDA cautious (remote consent under specific conditions). Cross-border data flow (GDPR, DPDP, LGPD) is the unresolved friction point. Inspector readiness uneven: source-data verification at home, IP accountability direct-to-participant.
ICH E6(R3)Jan 2025
Annex 2 in development
Annex 2 (non-traditional designs) Step 4 still in development · will codify DCT principles at ICH level.
Acceptance criteriaAnnex 2 · principles emerging
FDA2024 final
DCT guidance final
FDA DCT guidance final (2024) · remote consent + telemedicine + direct-to-participant IMP + home nursing operational.
Acceptance criteriaDCT 2024 final
EMA / CTR2024 update
2022 paper · 2024 update
EMA 2022 recommendation paper updated 2024 · cross-border data-flow under GDPR remains friction point.
Acceptance criteria2024 recommendation · GDPR friction
MHRAUK CTR
Combined-review DCT-friendly
UK Combined Review explicitly DCT-friendly · HRA + REC + MHRA single-process for hybrid designs.
Acceptance criteriaCombined review · DCT-friendly
PMDAGCP Ord.
Cautious · remote conditional
PMDA cautious · remote consent permitted under specific conditions · DCT-specific guidance still evolving.
Acceptance criteriaRemote conditional · DCT evolving
Inspector's eye
For multi-region DCT/hybrid programmes, the binding constraint is rarely the regulator's DCT position itself — it is cross-border data-flow under GDPR, India DPDP, Brazil LGPD. Map data-flow before site selection. Inspector readiness is uneven: source-data verification at the participant's home and IP accountability when shipping direct-to-participant are the audit-trigger keywords. PMDA-bound programmes assume remote-consent justification will be scrutinised in pre-CTN consultation.
/ 5.9 Trial Master File (TMF).eTMF · DIA TMF Reference Model · archiving timelines. +
At a glance · convergence vs divergence
CONVERGE
All require sponsor TMF + investigator site file (ISF) · eTMF acceptable across all five regulators · DIA TMF Reference Model is the de-facto operational standard · inspection-readiness as continuous state, not endpoint.
DIVERGE
Archiving timelines diverge: EU CTR typically 25 years after end of trial; FDA 21 CFR 312.62 typically 2 years post-marketing approval (or trial discontinuation); MHRA UK CTR aligned to EU historically; PMDA typically 5 years post-approval. Cross-region programmes default to longest applicable retention.
ICH E6(R3)Jan 2025
Annex 1 · essential records
Annex 1 essential records · eTMF principles · sponsor + investigator records distinguished.
Acceptance criteriaEssential records · sponsor + ISF
FDA21 CFR 312.62
2 years post-marketing
21 CFR 312.62 retention · typically 2 years after marketing approval or trial discontinuation · eTMF acceptable.
Acceptance criteria312.62 · 2y post-marketing
EMA / CTR2022 live
CTR · ~25 years
CTR Article 58 retention · typically 25 years after end of trial · eTMF acceptable.
Acceptance criteriaCTR Art 58 · 25y
MHRAUK CTR
Aligned to EU historically
UK CTR retention historically aligned to EU CTR baseline · eTMF acceptable · HRA national rules apply.
Acceptance criteriaUK CTR · EU-aligned
PMDAGCP Ord.
~5y post-approval
PMDA GCP Ordinance retention · typically 5 years post-approval · eTMF acceptable subject to ER/ES.
Acceptance criteria~5y · ER/ES applies
/ 06

History: from Reed to E6(R3).

Origin events · 1900–2024

Modern clinical trial regulation is the residue of scandal answered by ethics answered by codification. Each line in the timeline below is a moment where the conduct of research on human beings shifted from investigator conscience to written, enforceable rule.

1900 · Dec
Walter Reed yellow fever protocol (Cuba, Quemados) — first documented written, bilingual, witnessed informed consent. Volunteers signed contracts acknowledging risk of death; Spanish Consul-General countersigned. Pre-dates Nuremberg by 47 years; isolated investigator conscience, not regulatory norm.
1932–1972
Tuskegee Syphilis Study — USPHS observed 399 untreated Black sharecroppers for 40 years; investigators actively prevented penicillin access from 1947. Peter Buxtun → Jean Heller AP wire leak terminated the study in July 1972. The scandal that produced the National Research Act.
1947 · Aug
Nuremberg Code (U.S. v. Karl Brandt et al., Military Tribunal I) — ten-point verdict rationale. Foundational sentence: "voluntary consent of human subject absolutely essential". 23 Nazi physicians tried, 7 hanged. No operational specificity; pure ethical scaffold.
1962 · Oct
Kefauver-Harris Drug Amendments — response to thalidomide (10,000 phocomelia cases 1957–1961). First statute requiring substantial evidence of effectiveness. Birth of the modern clinical trial as registration requirement; parent of 21 CFR 312.
1964 · June
Declaration of Helsinki (WMA 18th General Assembly) — therapeutic vs. non-therapeutic distinction; ethics committee protocol review; physician duty to put participant welfare above science. Revised 9 times; 2024 revision addresses data integrity and vulnerable populations.
1974
National Research Act (PL 93-348) — mandated IRBs for federally-funded research; established the National Commission that would publish Belmont.
1979 · Apr
Belmont Report — three principles: respect for persons, beneficence, justice. Philosophical scaffold for 45 CFR 46 and 21 CFR 50/56.
1981 · Jan
21 CFR 50 (informed consent) + 21 CFR 56 (IRBs) — codified Belmont into binding US regulation. Subpart D (children) added 2001.
1987
21 CFR 312 IND Rewrite — modern investigational drug application framework. Interlocks with 21 CFR 4 (combination-product cGMP, 2013) and 21 CFR 812 (IDE).
1996 · May
ICH E6(R1) Step 4 — first global GCP harmonisation. Eight principles, 13 IRB requirements, 22 investigator responsibilities, 25 sponsor responsibilities. The Protocol/IB/CRF triad and TMF structure every CRO SOP descends from.
2001 · Apr
EU Clinical Trials Directive 2001/20/EC — attempted EU harmonisation; produced 27 Member States → 27 implementations. Between 2007–2011, EU CT applications fell 25%.
2016 · Nov
ICH E6(R2) — addendum, not rewrite. Risk-based quality management, sponsor vendor oversight, electronic records, CAPA for deviations. Acknowledged EDC-era reality.
2019 · Mar
India NDCT Rules 2019 — replaced Schedule Y. Compulsory compensation for CT-related injury, orphan-drug recognition, academic-trial framework, 30/90-day CDSCO timelines.
2020 · Mar
FDA Conduct of Clinical Trials Guidance (COVID-19 response) — remote consent, direct-to-participant IMP, telemedicine visits, decentralised source data became operational within months. A decade of debate compressed.
2022 · Jan 31
EU CTR 536/2014 goes live (CTIS portal) — single submission, single Reporting Member State assessment (Part I), parallel national (Part II); mandatory protocol/lay summary/results disclosure. Transition window closed 31 Jan 2025.
2022 · Dec
FDORA Section 3602 — Diversity Action Plan statutory mandate for Phase 3/pivotal trials. FDA Modernization Act 2.0 (same month) removed explicit animal-testing requirement from FFDCA §505.
2024 · May 28
Brazil Law 14.874/2024 (Marco Legal das Pesquisas Clínicas) — statutory 90-day clock for synthetic drugs, 180 for biologics. RDC 945/2024 operationalised it; single-window VICTOR portal.
2024 · Jan
ICH E6(R3) Step 4 — structural rewrite, not addendum. 12 overarching principles, Annex 1 (interventional), Annex 2 (non-traditional designs, in development). Quality-by-design from protocol inception; participant-centric language. FDA/EMA implementation guidance through 2025–2026.
/ 07

Evolution: seven eras.

Decade arcs · 1900–2035

The history is not a smooth curve. It is a sequence of eras, each defined by the question the field was answering. The current era is decentralisation overlaid with AI augmentation; the next is what comes after that.

/ Era 01 · 1900–1947

Pre-regulatory.

Reed's yellow-fever consent (1900) is isolated investigator conscience. Tuskegee begins (1932) without regulatory friction. The era ends not because the field reformed itself but because Nuremberg forced reform from outside.

/ Era 02 · 1947–1979

Ethical foundation.

Nuremberg (1947), Helsinki (1964), Belmont (1979) articulated principles. Regulatory codification lagged 15 years behind ethical articulation. Principles without operational specifics.

/ Era 03 · 1962–1987

Regulatory codification.

Kefauver-Harris (1962), 21 CFR 50/56/312 (1981–1987). US operational framework established. No international harmony — sponsors duplicated dossiers across regions.

/ Era 04 · 1972–1992

Scandal-reactive.

Tuskegee revelation (1972) forced National Research Act (1974). EU 2001/20/EC (2001) attempted harmonisation and failed. Fragmentation persisted; sponsors moved trials to North America and Asia.

/ Era 05 · 1996–2016

ICH-GCP industrialisation.

E6(R1) 1996 set the mutual-acceptance standard. R2 2016 added risk-based thinking. CRO operational playbooks standardised globally. Trial Master File became the universal artefact.

/ Era 06 · 2020–2026

Decentralised · digital.

COVID accelerated remote consent, telemedicine, direct-to-participant IMP. FDA, EMA, MHRA, Health Canada, PMDA, ANVISA all have DCT frameworks by 2024. WHO GCTP 2024 is design-agnostic. CTIS goes live (2022); transition window closes (2025).

/ Era 07 · 2024–2035

AI/ML-augmented · adaptive.

AI cohort enrichment, site selection, eligibility screening, signal detection moving from novel to baseline. ICH E20, FDA PCCP, EU AI Act parallel obligation framework. ICH E6(R4) horizon ~2032–2035 will absorb non-traditional designs and AI-in-conduct.

/ 08

Current state, 2026.

What is live now

The 2026 picture is a five-regulator divergence matrix overlaid with a partially harmonised E6(R3) substrate. The shifts below are operational, not theoretical — they affect dossier preparation today.

/ ICH E6(R3) status

Step 4 reached, implementation rolling.

FDA draft guidance 2025, final late 2026. EMA adopted 2025. MHRA aligned. PMDA GCP Ordinance amendment 2026–2027. CDSCO still primarily R2. ANVISA RDC 945 high-alignment with R3 spirit.

/ EU CTR · CTIS

Transition window closed.

All ongoing EU trials under CTR 536/2014 from 31 Jan 2025. Single submission, Reporting MS / Concerned MS dynamics stabilising. Public disclosure (protocols, lay summaries, results) default with limited deferral. Midcap and academic sponsors under-resourced.

/ Five-regulator matrix

Divergence persists.

FDA (21 CFR 50/56/312) · EMA (CTR 536/2014, CTIS) · CDSCO (NDCT 2019, 30/90-day) · PMDA (GCP Ordinance, pre-consultation heavy) · ANVISA (RDC 945/2024, 90/180-day, VICTOR).

/ Submission timelines

FDA most predictable.

FDA IND 30-day safe-to-proceed (reliable). EMA CTR Part I 45 days + 31+31 (CTIS validation adds 10–25 days). CDSCO 30 working days (SEC bottleneck). PMDA 30 days post-CTN. ANVISA 90/180 working days (variance high).

/ Decentralised trials

Regulatory option, not experimental.

FDA final DCT guidance 2024. EMA 2022 recommendation paper updated 2024. MHRA combined-review DCT-friendly. Health Canada explicit 2024. PMDA cautious. CDSCO less codified. ANVISA RDC 945 recognises DCT elements.

/ Diversity Action Plans

Operational standard.

FDA FDORA Section 3602 draft guidance June 2024 now operational for Phase 3/pivotal drug-device trials. Enrolment goals (race, ethnicity, sex, age) plus rationale and operational measures. Q1 2026 first full-cycle data. Rare-disease sponsors flag feasibility.

/ Combination products

MDR Article 117 in force.

FDA 21 CFR 4 + PMOA-led IND or IND+IDE. EU: CTR medicinal portion + MDR Article 117 notified-body opinion for device-integral DDCs. CDSCO recognised but determination less codified. PMDA Combination Office. ANVISA RDC 751 + RDC 945 case-by-case.

/ ANVISA RDC 945

Brazil most attractive LATAM CT jurisdiction.

Statutory 90/180 working-day timelines holding. VICTOR single-window operational. CONEP/CEP integration improved. DCT recognition welcomed. Combination-product RDC 945 + RDC 751 requires sponsor coordination.

/ India ICH trajectory

CDSCO Observer → Member.

NDCT 2019 codifies modern framework. E6(R2) substantially implemented. E6(R3) alignment in progress. Q-series mature. PvPI expanding. Industry expectation: 2027–2029 full ICH Regulatory Member status conditional on inspection capacity.

/ Ethics review divergence

Single-IRB now common in US.

FDA local + central IRB permitted. EMA Part II national (1 vs. multiple EC per MS varies). CDSCO central + IEC registered, mandatory re-registration. PMDA per-site IRB with central pilots. ANVISA CONEP federal + CEP local.

/ Not yet regulated

Frontier remains open.

Synthetic control arms in pivotals (case-by-case). AI/ML adaptive designs (ICH E20 traditional framework, AI-specific limited). In-silico trial evidence (mechanistic/device niche). Continuous submission models (pilot). Genomic-stratified ultra-rare (immature).

/ Cross-border data flow

Friction, not convergence.

GDPR (EU), DPDP (India), LGPD (Brazil), HIPAA (US). DCT direct-to-participant IMP and telemedicine intersect three or four regimes per trial. Source-data verification across jurisdictions remains an inspection question.

/ WHO GCTP 2024

Design-agnostic baseline.

WHO Good Clinical Trials Practice 2024 frames quality without prescribing design. Useful for LMIC regulators bootstrapping frameworks. Listed Authority pathway parallel-tracks regulator maturity.

/ 09

Future scope, 2026–2035.

Projections · with confidence

Forward views below are calibrated by confidence: high means trend is operational and trajectory clear; medium means direction is plausible but politically or technically uncertain; low means the substrate exists but the regulatory and reimbursement infrastructure does not.

/ 2029 horizon High

AI/ML-enabled trial designs become regulatory baseline.

Cohort enrichment / site selection standard from 2024+. Extending to adaptive design optimisation, real-time eligibility screening, AI-assisted SDV, safety-signal detection. FDA PCCP framework extends to trial AI ~2027. ICH E20 incorporates AI-adaptive. EU AI Act parallel obligation framework.

/ 2030 horizon Med

Synthetic control arms in pivotal trials accepted.

FDA rare-disease/oncology acceptance through 2025. EMA via Scientific Advice. Moving to broader ethical/feasibility-constrained use. FDA RWE Framework + ICH E11A + HMA-EMA Big Data Steering Group outputs shape trajectory. Single SCA failure-to-replicate would re-tighten.

/ 2030–2033 Low–Med

In-silico evidence supplementing registration.

FDA Modernization Act 2.0 removed animal-testing mandate (headroom for alternatives including in-silico). CDRH accepted computational device modelling since 2016. Realistic: in-silico supplementing (not substituting) pivotal drug claims 2028–2033; full substitution device-side only.

/ 2030 horizon High

Genomic-stratified · N-of-1 mainstream for ultra-rare.

Tumour-agnostic precedent (pembrolizumab MSI-H 2017) extends to biomarker-defined approvals. Bespoke Gene Therapy Consortium, FDA N-of-1 ASO draft 2021, EMA PRIME designation. Reimbursement barriers exceed regulatory ones.

/ 2030 horizon High

Decentralised becomes default.

Hybrid trials (home nursing, telemedicine, direct-to-participant IMP) standard, not special. Phase-3-with-50-sites persists for complex imaging/surgical. Site-density question replaces yes/no. Cross-border data-transfer (GDPR, DPDP, LGPD) may divergence rather than converge.

/ 2028–2034 Med

Global CTR-equivalent harmonisation spreads.

EU CTR/CTIS template → ASEAN Joint Assessment, AVAREF extension, possible ACCESS Consortium expansion (FDA-MHRA-Health Canada-TGA-Singapore-Swissmedic). Project Orbis extends into CT-stage. Geopolitical decoupling could fracture consortium.

/ 2032–2035 Med

ICH E6(R4) horizon.

R1 1996 → R2 2016 → R3 2025 suggests R4 ~2032–2035. Will absorb Annex 2 (non-traditional designs), embed AI/ML in trial conduct, strengthen participant-as-stakeholder, integrate continuous submission, absorb SCA/RWE into main framework. R3 implementation gaps could defer R4 by 2–3 years.

/ 2027–2030 High

India full ICH Regulatory Member.

NDCT 2019 track record, E6(R3) alignment via CDSCO inspection guidance 2026–2027, Q-series mature, PvPI expanding. WHO Listed Authority framework parallel-tracks maturity. Formal membership formalises bidirectional acceptance; India becomes regulatory-attractive, not just cost-attractive.

/ 2030–2035 Low–Med

Continuous submission · living dossier.

Real-time data flow sponsor → regulator. AI-assisted review. Automated safety reporting. FDA PDUFA VII pilots. EMA DARWIN EU. Binding constraint: regulator IT infrastructure (historically optimistic by 2–3x).

/ 2028–2032 Med

Climate · sustainability metrics on the regulator agenda.

EMA 2023 reflection paper. MHRA signalled interest. Carbon footprint monitoring travel, disposable waste, IT infrastructure. Soft-regulation trajectory (expectation not statute). More visible EU than US politically.

/ 10

AI in clinical trials.

Use cases · what each replaces or augments · maturity

The honest map of AI in trial conduct sorts use cases by what they actually replace and how mature the regulator's posture is. Some are production (deployed at sponsors and inspection-acceptable), some inspection-acceptable with caveats, some still piloting. One is regulator-flagged as a high-risk finding.

/ AI 01 · Production

Cohort enrichment · site selection.

Patient matching to inclusion criteria; demographic targeting; geographic optimisation. Replaces manual eligibility screening; augments site selection. Standard 2024+ at Medidata, IQVIA, Syneos. Inspection risk low — site selection aid, not protocol violation.

/ AI 02 · Insp-OK

Real-time eligibility screening at site.

Augments inclusion/exclusion documentation accuracy. Emerging 2024–2026, not yet standard. Regulator gates on protocol fidelity, not AI mechanism. Risk: if AI screen misses an exclusion, FDA cites protocol deviation — not the model.

/ AI 03 · Pilot

Adaptive design optimisation.

AI-assisted sample-size recalculation; dose-escalation sequencing; interim-analysis decisions. ICH E20 traditional framework mature; AI-extensions under discussion. PCCP framework (device-side) may extend conceptually. Adaptive design already complex; AI adds a layer.

/ AI 04 · Insp-OK

AI-assisted SDV.

Augments manual record review. Vendors piloting 2024+. No specific framework yet. Risk medium — overreliance on algorithm vs. auditor judgment. Inspectable when paired with risk-based monitoring SOP.

/ AI 05 · Production

Safety signal detection.

AE signal identification across pharmacovigilance datasets. Deployed in some CROs and sponsors. Sits in PV regulation (E2A) rather than CT regulation. Risk low — supplementary to human review.

/ AI 06 · Pilot

Synthetic control arm curation.

AI + real-world data for external control cohort selection. FDA-led rare-disease and oncology pilots. SCA frameworks developing; AI-specific mechanism underspecified. Risk medium — representativeness contested, data quality.

/ AI 07 · Pilot

Informed consent simplification (NLP).

ICF readability assessment. Research-stage. No specific framework. Risk low if used for readability check only, not authorship.

/ AI 08 · Pilot

DCT logistics optimisation.

Telemedicine visit scheduling; direct-to-participant IMP shipment routing. Operational tool, not protocol-affecting. Emerging 2024–2026. Risk low.

/ AI 09 · High risk

Generative AI authoring · protocols, ICF, CSR.

Replaces human writing — if allowed. Proposed by some vendors. FDA, EMA, PMDA have signalled unacceptable without human-in-the-loop. High-risk inspection finding if detected. Authorship integrity question is not solved.

/ 11

Flow of a trial.

Concept → submission · 12 steps

The lifecycle below is the operational pipeline that sits beneath the four-phase architecture. Each step has a regulator-facing artefact; each is a place where studies most often slip schedule or trigger inspection findings.

01

Concept · target product profile.

Sponsor defines indication, mechanism, comparator landscape, target label. Strategy precedes protocol. Decision: pursue or not.

02

IND-enabling · preclinical package.

21 CFR 312 mandatory toxicology, PK, mechanism data before human exposure. Typically 2–5 years pre-clinical → clinical transition. CMC ready in parallel.

03

IND / CTA submission.

FDA IND (30-day safe-to-proceed). EMA CTR Part I + II via CTIS. CDSCO NDCT. PMDA CTN. ANVISA via VICTOR. Ethics committee submission parallel or sequenced.

04

Protocol · ICH M11 structured.

Quality-by-design from inception (E6(R3) requirement). Estimands per E9(R1). Statistical analysis plan locked. Investigator brochure, ICF, CRF triad finalised.

05

Site selection · feasibility.

Therapeutic-area fit, PI track record, recruitment realism, system readiness (EDC, eTMF, IRT). DCT components feasibility assessed at site level.

06

Site initiation · SIV.

Contracts and budgets executed. Site-level EC/IRB approvals confirmed. Investigator and staff trained on protocol, ICF, e-systems. Drug supply at site. Green-to-enrol.

07

Recruitment · screening · randomisation.

Patient identification, informed consent, screening assessments, inclusion/exclusion check, IRT randomisation. Diversity Action Plan operational measures live (FDA Phase 3 pivotal).

08

Dosing · visit conduct.

IMP administration, scheduled visits, sample collection, PRO and ePRO capture. Telemedicine and home-nursing for hybrid DCT. Source data captured at site / direct-to-participant.

09

Monitoring · SDV · safety surveillance.

Risk-based monitoring per E6(R3). Source data verification (proportionate, not universal). AE reporting. Independent DSMB review for blinded interim analyses. CAPA for deviations.

10

Database lock · DBL.

All data queries resolved. CRF finalised. Coding (MedDRA, WHODrug) reconciled. Statistician and DM sign-off. Database frozen.

11

Statistical analysis · CSR.

Pre-specified analysis per SAP. Estimand-aligned outputs. Clinical Study Report (ICH E3) drafted. TMF closure parallel.

12

Submission · NDA / MAA / NDS.

FDA NDA / EMA MAA / CDSCO NDA / PMDA J-NDA / ANVISA Registro. Module 5 CSRs anchor; ISS/ISE integrate across studies. Inspection-readiness file maintained.

/ 12

Use cases: what trials are run for.

Why the domain exists

Trials are not run for their own sake. Each design exists to answer a specific regulatory or commercial question. The use cases below cover the modern field; sponsors typically run several in parallel across a single asset's lifecycle.

/ Use 01

Phase 1 · first-in-human.

Safety, tolerability, PK, dose-escalation. Healthy volunteers (mostly). Site-based Phase I units. Open-label. Triggers: post-IND approval, first clinical assessment.

/ Use 02

Phase 2a · proof-of-concept.

Preliminary efficacy signal in target patient population. Dose-range finding. ICH E8 early clinical development. Triggers: Phase 1 data acceptable, mechanism rationale.

/ Use 03

Phase 2b · dose-ranging.

Optimal-dose selection for pivotal. Confirm mechanism in target population. Typically 100–500 patients. Triggers: Phase 2a signals POC.

/ Use 04

Phase 3 · pivotal registration.

21 CFR 314 NDA / EMA CTR / CDSCO NDCT requirement: substantial evidence of effectiveness. Double-blind RCT vs. control. 1,000–10,000 patients. Now must incorporate Diversity Action Plan (FDORA §3602).

/ Use 05

Combination product trial.

Drug-device dual constituent. 21 CFR 312 + 812 (US); CTR + MDR Article 117 (EU, notified-body opinion). PK/PD for drug, performance/safety for device. Sponsors: Boston Scientific, Medtronic, Abbott.

/ Use 06

Decentralised · hybrid trial.

FDA DCT final guidance · 'Conducting Clinical Trials with Decentralized Elements' (17 September 2024), EMA recommendation paper, ANVISA RDC 945 recognition. Remote consent, telemedicine visits, home nursing, direct-to-participant IMP. Reduces site burden, broadens access.

/ Use 07

Real-world evidence · pragmatic.

FDA PDUFA VI commitment, EMA HMA-EMA joint guidance 2024, WHO GCTP 2024. Observational, registry-based. Fewer exclusions than Phase 3. Supplements or replaces traditional evidence under specified conditions.

/ Use 08

Paediatric · PIP.

EU Paediatric Regulation EC 1901/2006. FDA PREA / BPCA. Mandatory for most new actives. Formulation development, PK/PD in children. Triggers: paediatric population clinically relevant.

/ Use 09

Rare disease · N-of-1.

FDA Bespoke Gene Therapy Consortium. FDA N-of-1 ASO guidance draft 2021. Single-patient or ultra-small cohorts with variant-specific intervention. Tumour-agnostic precedent (pembrolizumab MSI-H 2017).

/ Use 10

Biosimilar · comparative PK/PD.

FDA 351(k) pathway, EMA biosimilar guideline, ANVISA RDC 55/2010. Comparative PK almost always required. Immunogenicity parallel. Totality-of-evidence framework.

/ Use 11

Phase 4 · post-marketing.

21 CFR 312 Subpart I (expanded access). Post-marketing commitments and requirements. Real-world safety. Long-term effectiveness. Label-expansion data.

/ Use 12

Vaccine · biologic trials.

COVID, mpox, RSV, influenza, malaria. Sponsors: Moderna, BioNTech, Pfizer, GSK. Large Phase 3 efficacy populations. Cold-chain, immunogenicity assays, long-term safety follow-up. WHO PQ for LMIC roll-out.

/ 13

Big players.

Sponsors · CROs · regulators · networks

The clinical trial economy is dense. The map below groups the named institutions sponsors and regulators interact with most often. None of these are endorsements; the list is the operational reality.

/ Pharma sponsors · major

Pfizer, Merck, Moderna, Roche, AbbVie, Johnson & Johnson, Amgen, Bristol Myers Squibb, Novartis, Eli Lilly. IND/CTA sponsors. Phase 1–4 design authority. Define indication, comparator, label strategy.

/ Pharma sponsors · mid-cap · specialty

Agios, Vertex, Sangamo, Uniqure, Editas. Rare disease, gene therapy, cell therapy clinical programmes. Disproportionate share of N-of-1 and ultra-rare designs.

/ Biologics · vaccines

Moderna, BioNTech, Pfizer (vaccines), GSK. COVID, mpox, RSV, influenza, malaria. Large Phase 3 efficacy populations and post-approval safety follow-up.

/ Device-pharma · combination products

Boston Scientific, Medtronic, Abbott, Stryker, J&J (DePuy), Zimmer Biomet. Drug-coated implants, drug-eluting stents, autoinjectors. Run combination-product trials under 21 CFR 4 / MDR Article 117.

/ CROs · full-service

PAREXEL (Fortrea), Syneos Health, IQVIA, PPD, Charles River. Phase 1–4 trial management, bioanalytical, pharmacovigilance, regulatory affairs.

/ CROs · specialty · site networks

Covance (Phase I), WuXi AppTec (early development), Richmond Pharmacology (Phase I), Parexel MPI (device), Medpace, Accelovance, Chiltern, PharmaLogic Research. Phase I units, niche expertise, site recruitment, PI relationships.

/ Regulators

FDA (CDER, CBER, CDRH; expedited programs; pre-submission meetings) · EMA (CHMP, PRAC; CTR assessment via Reporting Member State) · CDSCO (India; Subject Expert Committee; ICH Observer) · PMDA (Japan; Combination Product Office; pre-consultation pathway) · ANVISA (Brazil; RDC 945/2024 VICTOR; CONEP) · MHRA (UK; combined-review DCT-friendly) · Health Canada · TGA (Australia) · WHO Prequalification (LMIC vaccine and biologic assessment).

/ Ethics review bodies

IRBs (US, including single-IRB models) · RECs (UK) · ECs (EU Member States; per-Member-State approval under CTR Part II) · IECs (India CDSCO-registered, mandatory re-registration) · CEPs + CONEP (Brazil, local + federal).

/ Tech · eClinical vendors

EDC: Medidata Rave, Veeva CDMS, Oracle Clinical One, Castor · eTMF: Veeva Vault eTMF, Wingspan, Phlexglobal · CTMS: Veeva CTMS, Medidata, Bioclinica · IRT/RTSM: Endpoint Clinical, Suvoda, Almac · ePRO · eCOA: Clario, Signant Health, Medable · Safety / PV: Oracle Argus, ArisGlobal LifeSphere · AI patient-matching: Medidata Acorn AI, IQVIA, Deep 6 AI.

/ Professional bodies · standards

ICH (E-series guidelines) · WHO (GCTP 2024, prequalification) · CDISC (CDASH, SDTM, ADaM data standards) · DIA (Drug Information Association) · SCDM (Society for Clinical Data Management) · ACRP, RAPS, TransCelerate BioPharma.

/ Patient advocacy · recruitment

Patient-centred outcomes research networks; disease-specific advocacy (American Heart Association, Cancer Network, NORD); Bespoke Gene Therapy Consortium; site-based recruitment staff. Role: informed consent, retention, post-trial access advocacy.

/ 14

Stakeholders.

Interest · leverage

Every clinical trial is a negotiation between unequal parties with overlapping interests. The stake-table below names each party and the lever it actually pulls. The map matters because most operational disputes (timeline, scope, deviation handling) trace back to a misread leverage relationship.

Sponsor
InterestApproval timeline, recruitment timeline, data quality, inspectable dossier.
LeverageDevelopment budget, market entry timing, choice of CRO and sites.
CRO trial mgr
InterestProtocol efficiency, site compliance, bioanalytical reliability, deliverable margin.
LeverageSite capacity, investigator relationships, system readiness, escalation discretion.
Investigator / PI
InterestInformed consent quality, protocol feasibility, site burden (visits, assessments).
LeverageRecruitment capacity, data accuracy, willingness to enrol or decline study.
Healthy volunteer
InterestSafety, fair compensation, transparent withdrawal mechanism, valid consent.
LeverageRecruitment willingness, dropout risk, post-trial reputation in volunteer panels.
Patient subject
InterestTherapeutic benefit (or trial benefit), safety, post-trial access, data privacy.
LeverageRecruitment, protocol compliance, dropout risk, post-approval real-world feedback.
Regulator
InterestGCP compliance, data integrity, valid consent, ethics-committee diligence, safety reporting.
LeverageClinical hold, deficiency letters, inspection authority, approvability decisions.
Ethics · IRB / EC
InterestParticipant protection, consent adequacy, risk/benefit favourable, vulnerable populations.
LeverageTrial approval or rejection, amendment requirements, suspension authority.
Sponsor QA / RA
InterestE6(R3) compliance, TMF readiness, deviation and CAPA management.
LeverageInspection readiness, regulatory decision timing, internal escalation.
Bioanalytical team
InterestMethod validation, ISR, chain-of-custody documentation.
LeverageMethod lifecycle management, inspection defensibility of PK data.
Pharmacovigilance
InterestSignal detection, AE reporting timeliness, periodic safety updates.
LeverageRegulatory communication authority, dose-adjustment / stopping decisions, DSUR.
Statistician
InterestEstimand integrity (E9(R1)), SAP fidelity, blinded interim analysis discipline.
LeverageDatabase lock sign-off, primary-analysis defensibility, regulatory statistical defence.
Monitor / CRA
InterestRisk-based monitoring fidelity, SDV proportionality, deviation capture.
LeverageSite escalation, sponsor visibility, source-data integrity findings.
Payer / health system
InterestCost-effectiveness evidence, real-world outcomes, post-approval access.
LeverageReimbursement decisions, formulary placement, HTA negotiation.
Combo device mfr
InterestDual-pathway clarity (21 CFR 312 + 812; CTR + MDR Art. 117).
LeveragePMOA jurisdiction, notified-body opinion timing, combined-review efficiency.
/ 15

Selected writing on clinical trials.

From the archive
2021-02-25

ICH-GCP · quiz and reflection.

Reading ICH-GCP E6 carefully. The grey zones inspectors look at first. What practitioners get wrong on the first read.

GCP comparison →
2022-08-23

Software-enabled clinical trials.

The architectural shift: eCRF, CTMS, eTMF, eDMS, eQMS, LMS as a connected suite. What changes when the suite actually integrates.

AI lens →
2025-04

Latest trends in clinical trials: what you need to know.

Decentralised, adaptive, AI-assisted. What the field looks like through 2026 and into 2030.

Future 2026-2035 →
2025-04

Overcoming challenges in clinical trials: a pathway to success.

Site selection, recruitment, sample handling, bioanalytical readiness. Where studies most often break down operationally.

Current 2026 →
2025-03

Quality management systems in clinical research.

The QMS substrate underneath GCP. ICH E8(R1) as quality-by-design. What modern QMS looks like operationally.

~6 min
2025-05

QMS · ensuring excellence in clinical operations.

How QMS earns its keep at the operational level. Why most QMS implementations fail to produce inspection-readiness.

~5 min