Blog

Home Weekly Newsletter Japan Clinical Trials Unlocked: PMDA Pre-Consultation to First Patient In

Pharma Focus

Japan Clinical Trials Unlocked: PMDA Pre-Consultation to First Patient In

December 18, 2025

Flowchart showing the PMDA pre-consultation and Clinical Trial Notification (CTN) process for initiating clinical trials in Japan, including timelines, consultation steps, and regulatory requirements.
Tags:

Editor’s Note

Japan represents one of the world’s largest pharmaceutical markets. Its regulator Pharmaceuticals and Medical Devices Agency (PMDA), now targets ~12-month review timelines, with median NDA approval taking roughly 333 days (~11 months). Entering the Japanese market requires understanding the Clinical Trial Notification (CTN) system—distinct from the U.S. IND pathway—and engaging early with the PMDA to accelerate trial approval and market access.

This executive summary distills key regulatory strategies, timelines, and real-world precedents for sponsors planning Japan market entry during clinical development.

CTN vs. IND: Critical Regulatory Distinctions

Japan does not operate an IND system like the U.S. Instead, sponsors must submit a Clinical Trial Notification (CTN) to the Ministry of Health, Labour and Welfare (MHLW) before initiating trials.

Key Differences

Aspect U.S. IND Japan CTN
Regulatory Authority FDA (CDER/CBER) MHLW
(with PMDA scientific oversight)
Pre-Submission Consultation IND Meetings
(2–3 months total)		 Pre-Consultation Meetings
(5–6 months total)
Review Timeline 30 days 30-day MHLW review post-CTN submission
Language Requirement English accepted Japanese is required for major documents
Approval Pathway “Study May Proceed” letter or objections are issued CTN is “acknowledged”; no formal approval letter

 

Key Insight: PMDA consultation is more intensive and prolonged than U.S. IND meetings, reflecting Japan’s emphasis on pre-trial alignment. However, early engagement clarifies expectations and prevents costly protocol revisions.

Strategic PMDA Consultation: Timeline and Approach

PMDA consultation is the critical first milestone for Japan market entry. The process requires 5–6 months total:

Consultation Timeline:

  • T–5 to 6 weeks: Submit briefing package (max 20 pages; preferably on Monday)
  • T–2 to 4 weeks: PMDA pre-consultation meeting (~30 minutes; free, no official minutes)
  • T–1 month: Negotiation phase; PMDA issues preliminary inquiries (2–3 rounds)
  • T–0: Formal consultation meeting (~2 hours; applicant presents outline, then detailed discussion)
  • T+1 month: PMDA issues draft meeting minutes and final opinion

Consultation Package Must Address:

  1. Development strategy and unmet medical need
  2. Nonclinical pharmacology and toxicology
  3. Clinical pharmacology data (PK/PD properties)
  4. Manufacturing and quality (CMC) summary
  5. Proposed protocol outline with endpoints and investigator qualifications
  6. Ethnic bridging strategy – Why the Japanese Phase 1 study is or is not needed
  7. Timeline and commercial context

 

Action Item: Initiate consultation planning 2–3 months in advance, with formal requests submitted on the first business day of each month.

Real-World Case Study: Lecanemab (Leqembi®) – Eisai & Biogen

Strategic Approach: Rather than requiring standalone Japanese efficacy/safety trials, Eisai and Biogen submitted pooled CLARITY AD data (global Phase III MRCT with Japanese/Asian cohorts) to PMDA, supported by pre-submission consultations on ethnic factors and applicability of foreign data to Japanese patients.

PMDA Confirmation:
• Sufficient Japanese patients in CLARITY AD satisfied local data expectations
• Ethnic factors (genetics, concomitant medications, disease progression) did not materially differ between Japanese and non-Japanese cohorts
• Foreign efficacy data directly applicable under ICH E5 bridging principles

Timeline & Outcome:
• January 2023: Priority Review designation (Japan)
• July 2023: FDA full approval
• September 2023: MHLW approval (~2.5 months after FDA)

Lesson: Early PMDA engagement plus robust ethnic bridging justification enabled accelerated market access and simultaneous global development, avoiding sequential, Japan-specific trials.

Ethnic Bridging & December 2023 PMDA Guidance

Game-Changing Update: In December 2023, PMDA fundamentally revised its stance on Japanese Phase 1 studies. The new guideline states that an additional Japanese Phase 1 study is NOT needed in principle, provided sponsors:

  1. Conduct rigorous ethnic sensitivity assessment (ICH E5 principles)
  2. Evaluate whether safety/tolerability can be predicted from available data (nonclinical, foreign PK/PD, exposure-response analyses)
  3. Demonstrate scientifically that ethnic-specific risks are clinically acceptable

 

Key Assessment Factors: Pharmacokinetic variability (e.g., CYP-mediated metabolism differences), pharmacodynamic sensitivity (e.g., biomarker/genetic prevalence differences), safety concerns (ethnic-specific adverse event patterns), and disease characteristics (onset, severity, progression).

 

PMDA Accepts: Population PK modeling, PBPK simulation, covariate analysis, and sensitivity analyses to justify a Phase 1 waiver if justified by existing data.

CTN Submission: Essential Documents & Timeline

Mandated by MHLW, first CTNs must be submitted ≥31 days before first patient (30-day review period), and follow-on amendments have a 14-day review period. From April 1, 2026, PMDA will only accept regulatory submissions in eCTD version 4.0 format for new applications. Submissions in older formats such as eCTD v3.2.2 will no longer be accepted after that date.

Mandatory CTN Documents (Older formats-March 2026):

  1. Scientific rationale statement
  2. Clinical trial protocol (with predefined estimands, inclusion/exclusion, endpoints)
  3. Informed consent form (ICF) – must be in plain Japanese
  4. Investigator’s Brochure (IB) – in Japanese, including ethnic factor analysis
  5. Nonclinical study reports (toxicology, pharmacology)
  6. Manufacturing and quality (CMC) summary
  7. Investigator curriculum vitae and trial experience
  8. Case Report Form (CRF) samples
  9. Data management and safety monitoring plan
  10. Japanese trial site certifications and patient demographics

 

Submission Timeline:

  • T–31 days: Submit CTN for new active ingredients, new routes, or novel combinations
  • T–14 days: Submit CTN for other drug categories
  • T+30 days: If no MHLW objection, CTN acknowledged and trial may commence

 

Preparation Time: 6–12 weeks from PMDA consultation completion to CTN submission (includes 4–8 weeks for document translation into Japanese + 2–3 weeks for internal QA).

Real-World Case: Baloxavir Marboxil (Xofluza®) – Shionogi

Strategic Approach: Conduct Phase II/III trials in Japan ahead of global submissions to generate local efficacy/safety data satisfying both Japanese and international regulatory expectations.

Development Timeline:
• February 2018: Japan approval (following CTN review and Phase III success)
• October 2018: FDA Priority Review (U.S.)
• December 24, 2018: FDA approval

Key Success Factor: Early PMDA consultations confirmed Phase III design, bridging strategies, and global development alignment. Local Japanese data accelerated U.S. and global approvals, establishing Japan as a lead market for innovation.

Implementation Timeline: 20-Month Roadmap

Phase

Timeline

Key Actions

Market Entry Planning

Month 1–2

Engage Japan-based consultant; assess MRCT eligibility

Consultation Prep

Month 3–4

Develop a briefing package; draft ethnic bridging strategy

PMDA Pre-Consultation

Month 5–6

Submit request; obtain preliminary feedback

Formal Consultation

Month 7–10

Conduct 2-hour meeting; address PMDA inquiries

Protocol & Translation

Month 11–15

Revise per PMDA guidance; translate to Japanese; QA

Internal Review

Month 16–18

Medical/legal/compliance sign-off

CTN Submission

Month 19

Submit to MHLW; manage 30-day review

Trial Initiation

Month 20

Site initiation; commence enrollment

Key Takeaways & Action Items

  1. Initiate PMDA Consultation Early: Begin planning 5–6 months before target CTN submission; early engagement prevents costly protocol revisions.
  2. Leverage December 2023 PMDA Guidance: Use robust ethnic sensitivity assessment + PopPK modeling to justify MRCT participation without mandatory Japanese Phase 1 studies.
  3. Integrate Japan into MRCT Design: Incorporate Japanese requirements into global trial protocols from inception; select endpoints and populations applicable to Japanese clinical practice.
  4. Allocate Time for Localization: Budget 4–8 weeks for comprehensive document translation and QA into Japanese.
  5. Build a Dedicated Japan Team: Engage Japan-focused CRO, local regulatory consultant, and in-house Japan manager for PMDA interactions and site management.
  6. Document All PMDA Guidance: Maintain detailed records of consultation meeting minutes and responses to ensure consistency and build regulatory precedent.
  7. Plan for ~20 Months: From market entry planning to trial initiation in Japan requires coordinated execution; early planning prevents delays.

How BLA Regulatory can help?

BLA Regulatory Japan supports clients through the full Japan trial lifecycle — from PMDA consultation strategy and briefing package development to CTN submission, document localization, and regulatory translation QA.
With an established presence in Japan and bilingual experts on the ground, we bridge global and local requirements, manage CRO coordination, and deliver data-driven ethnic sensitivity justifications (popPK/PBPK, ICH E5-compliant) to streamline your MRCT or Japan-only trial execution.

References

Contact Us