Law and Admin

Question 1

What are some changes the QP needs to be aware of?

Answer 1

Windsor Framework
Supply chain for Northern Ireland
Medicinal products intended for the UK market (including NI) must: (i) be authorized by the MHRA; and (ii) bear a clear “UK only” label, which may be placed anywhere on the pack.
Effective from 1 January 2025

Question 2

What are the legal duties of a QP

Answer 2

Defined in HMR (SI2012:19196) schedule 7 part 3
- each batch of medicinal products manufactured checked in accordance with national regulations
- Each batch has undergone a full qualitative analysis and quantitative analysis of all the active substances, all other tests or checks necessary to ensure the quality of medicinal products in accordance with the requirements of the MA
- Certification is recorded in a register or equivalent document.

Question 3

Difference between legal duties for UK and EU QP

Answer 3

EU QP complies with 2001/83
Also includes safety features

Question 4

What countries does the UK have an MRA with?

Answer 4

UK MRA’s are:
EEA
Australia
Canada
Israel
Japan
New Zealand
Switzerland
United States of America

Question 5

Which products does the MRA not apply to?

Answer 5

Australia
Advanced Therapy Medicinal Products

Canada
Medicinal products derived from human blood or blood plasma
Advanced Therapy Medicinal Products

Israel
Medicinal gases
Homeopathic products
Medicinal products derived from human blood or blood plasma
Advanced Therapy Medicinal Products

Japan
Medicinal gases
Medicinal products derived from human blood or blood plasma
Advanced Therapy Medicinal Products

New Zealand
Advanced Therapy Medicinal Products

United States of America
Vaccines
Advanced Therapy Medicinal Products
Medicinal products derived from human blood or blood plasma

Question 6

What do you know about the International Recognition Procedure?

Answer 6

It is effective from 01 Jan 2024,

New licensing route for medicines (pre and post authorisation procedures) allows the MHRA to conduct targeted assessments by recognising approvals from trusted partner agencies.

Approved Reference Regulators are Australia, Canada, European Commission, Japan, Switzerland, Singapore and the USA

Recognition A and B (different timelines). B is for: ATMP, First-in-class new active substance, Incorporates novel or cutting-edge technologies, Fractionated plasma product

Question 7

Where can the Routine duties be found. Can you state them?

Answer 7

Annex 16

1. All activities associated with manufacture and testing of the medicinal product have been conducted in accordance with the principles and
   guidelines of GMP.
2. The entire supply chain of the active substance and medicinal product up to the stage of certification is documented and available for the QP. This should include the manufacturing sites of the starting materials and packaging materials for the medicinal product and any other materials
   deemed critical through a risk assessment of the manufacturing process.
3. All audits of sites involved in the manufacture and the testing of the been carried out and that the audit reports are available.
4. All sites of manufacture, analysis and certification are compliant with the terms of the MA for the intended territory.
5. All manufacturing activities and testing activities are consistent with those described in the MA.
6. The source and specifications of starting materials and packaging materials used in the batch are compliant with the MA.
7. Active substances manufactured in accordance with GMP and distributed in accordance with GDP
8. Importation of AS comply with the requirements of Article 46(b) of Directive 2001/83/EC.
9. Excipients have been manufactured in accordance with GMP.
10. TSE status known and compliant with MA
11. All records are complete and endorsed by appropriate personnel. All
    required in-process controls and checks have been made.
12. All manufacturing and testing processes remain in the validated state.
    Personnel are trained and qualified as appropriate.
13. Finished product quality control (QC) test data complies with the Finished
    Product Specification described in the MA, or where authorised, the Real
    Time Release Testing programme.
14. Post-marketing commitments relating to on-going stability data continues to support certification.
15. Change impact evaluated and additional checks and tests are complete.
16. Investigations to batch certification including OOS and OOT.
17. Complaints, investigations or recalls do not negate conditions for certification.
18. Required TA’s in place.
19. SI programme is active and current.
20. Distribution and shipment arrangements are in place.
21. Safety features have been affixed to the packaging.

Question 8

What are the legal duties of an IMP QP?

Answer 8

SI 2004:1031 Part 6 Section 43
EU regulation 536/2014 and Regulation 2017/1569
- Manufactured and assembled to GMP, PSF and appropriate authorisations,
- import from outside the EU/EEA then it is made to GMP equivalent to UK GMP
- testing carried out to comply with PSF
- Certify and document in a register or equivalent

Question 9

What are the legal duties of a QP for Veterinary Products?

Answer 9

SI 2013:2033 Schedule 2 Part 1 Section 11
EU regulation 2019/6
- Manufactured and assembled to GMP, and marketing authorisation
- import from the EU/EEA to carry out full qualitative analysis, quantitive of actives, other tests show compliance to MA
- Where MRA applies, accept on CofA.
- Certification on a control report

Question 10

What are the different types of variations?

Answer 10

Type 1 - prior approval not required
- 1A - submit within 12 month of change
- 1AIN - notify immediately after implementation

Type 2 - prior approval required

Type 1B - neither type 1A or 2

Question 11

Updates to legislation a QP needs to be aware of

Answer 11

Brexit
FMD
EU - CT Regs

Question 12

Name the countries approved for import by the MHRA

Answer 12

Regulation 18A of the Human Medicines Regulations 2012 will allow importation of human medicines into Great Britain under a UK wholesale dealer’s licence from the following countries, provided that the UK wholesale dealer confirms that each batch has been certified by a Qualified Person (QP) in a listed country

EU countries, plus Iceland, Liechtenstein and Norway.

Question 13

What are the safety features?….Are they required for all products?…What about IMPs

Answer 13

Directive 2011/62/EU (FMD) introduced requirement for all prescription medicinal to have safety features. - to enable verification of individual packs - tamper evidence seals of outer packaging.

Delegated regulation 2016/161 (to apply from Feb 2019).
Safety features required for the sale, distribution and supply of products:
- 2D barcode, and human readable format containing the following:
1. Product Code – Name, common name, pharmaceutical form, strength, pack size and type
2. Serial Number – numeric or alphabetic – must be randomised and comprise a max of 20 characters
3. National Reimbursement Number (if present)
4. Batch Number and Expiry Date
- Tamper-evident device

European Medicines Verification System <EMVS> to allow verification of authenticity by Wholesalers & distributers. verified and decommissioned before being dispensed. High risk also verified at the wholesaler.</EMVS>

Required for prescription but some exceptions e.g. Homeopathic, ATMPs, Radiopharmaceuticals, Medicinal gases, Electrolyts
Not required for non prescription, unless in the annex (omeprazole, also national CAs can add)
Not required for IMP but tamper evidence is required anyway and the IRT (interactive Response Tech) tracks.

Question 14

You have an API manufactured and tested in India, Drug Product Manufactured and Tested in the US, Imported into Germany, QP in the UK

Answer 14

• Licences for all Sites (MIA in EU and MA), Check GMP certificates of API+DP manufacturer, API QP dec, Excipient risk assessment
• Import: DP import testing (if it’s not on the MRA), API cert of conformity (not required as not being imported to EU)
• Supply chain: mapped and risk assessed
• Audits: manu & test of DP and manu of API (conf distribution and storage arrangements)
• Reference: (at manu site or import testing site) and retention (at QP release site) samples
• Stability: does not NEED to be in the EU
• Batch release: per annex 16
• QTA: Details above , including QP shared responsibilities.

Question 15

What is the regulatory basis for the QP?

Answer 15

Directive 2001/83/EC: (41 and 48) : MAH must have at least one QP, (49) qualifications/practical experience, (50) ‘transitional’ QPs who acted as a QP pre 20 May 1975, (51) legal responsibilities, (52) MS ensures duties of the QP are fulfilled. Directive 2001/83/EC needs to be transposed into National Law of each MS.

SI: 2012-No.1916 (17 parts and 35 schedules). Most relevant parts for the QP are Schedule 7: QP: educational requirements, experience and responsibilities

Question 16

What is a directive?

Answer 16

Unlike regulations, Directives are interpreted into national laws (S.I. in the UK)

Question 17

How are the regulations transposed into UK law?

Answer 17

Regulations have binding legal force throughout every Member State and enter into force on a set date.

Question 18

What information is contained in a PSF?

Answer 18

EU GMP Volume 4 Annex 13:
A Product Specification File is a file containing or referring to all info needed to draft the instructions on: processing, packaging, QC, batch release and shipping of an IMP.

PSF is continually updated through development (with version control). Includes the following, at a minimum:
- Protocol
- Randomisation codes
- Approved label copy
- Manufacturing methods
- Specs and test methods for starting materials, packaging materials, Intermediate, bulk and finished product
- Stability data
- Storage and shipping conditions
- QTA

Question 19

What changes to EU GMP guidance does the QP need to be aware of?

Answer 19

Annex 1: (PC Dani 5)
- PUPSIT will stay
- CCI expectation is 6 monthly to annual CCI checks (some MS require all batches)
- Distilation is no longer the only process for WFI production
- Align with PIC/S - i.e. there was US involvement
- New technology (isolators/RABS must be used)
- ICHQ9 and Q10 principles incorporated
- 5um particle monitoring in qualification of cleanroom not required

Annex 15: refers to the EMA guidance regarding a full toxicological assessment to derive a safe HBEL. A subsequent Q+A (2016) introduces the concept of “non highly hazardous” products which considers the 1/1000th minimum therapeutic dose approach as sufficiently conservative.
Annex 17: to become real time release
This will no longer only relate to Sterility testing - based on risk
Annex 21- Importers of Medicinal Products
To clarify requirements re: sampling and testing of imported products. (Physical and FISCAL importation)
ATMP GMP
Published as Vol 4 Part 4.
EP for Water for Injection (WFI)
EP for WFI revised, allowing Osmosis

Question 20

What are the legal duties of the PVQP?

Answer 20

This was changed by amending Dir 2010/84/EU, The only QP PV info included in 2001/83/EC is:
- needs to be permanently available 24/7 and contact should be available to the CAs
- shall reside and operate in the EU
- shall be responsible for the establishment and maintenance of the pharmacovigilance system.

Further duties detailed in the Guidelines on Good PV Practices (GVP) and Eudralex volume 9, such as:
- Pharmacovigilance System master file (PSMF)
- Back up
- Safety profiles, Concerns and commitments relating to safe use
- Submit Data for PV correctly , and prompt response to requests

Question 21

What is the difference between PIC and PIC/S?

Answer 21

PIC (founded 1970): The Pharmaceutical Inspection Convention - a legal agreement between reg authorities of countries with treaty status (for human or veterinary use).

PIC/S: The Pharmaceutical Inspection Co-operation Scheme (founded 1995) - An informal extension of PIC (49 authorities world wide - EU countries, north american countries, Australasian and some asian, some south america and south africa - detailed on PIC/S website……), as EU law did not allow individual EU countries to sign agreements with other non EU PIC countries. only the commission could sign agreements and they arn’t a member of PIC.

Question 22

What are the responsibilities of an RP

Answer 22

2013/C 343/01 requires wholesale dealers to appoint a Responsible Person (RP) for GDP and details the requirements.
Responsibilities are detailed, such as
- ensuring a quality management system is implemented and maintained;
- training programmes are implemented and maintained;
- coordinating and promptly performing any recall operations and customer complaints are dealt with effectively;

Question 23

describe the FMD and discuss the relevant sections?

Answer 23

The Falsified Medicines Directive is to protect the public from falsified medicines.

• Safety features
• GMP for Actives
• Risk assessments for Excipients
• GDP for Actives and DP
• Sales at a distance

Question 24

Do the MHRA publish guidelines – are you aware of any?

Answer 24

The orange guide - GMP
The green guide - GDP
The grey guide - GCP
The purple guide - Pharmacovigelence
Based on the Eudralex.

Also publish their own guidance, for example:
- MHRA GMP Data Integrity Guidance for Industry Draft version for consultation July 2016
- Out of Specification Guidance 2017
- Borderline products

Question 25

How are the MHRA and ICH related?

Answer 25

The International Council for Harmonisation of Technical Requirements for Pharmaceuticals for Human Use (ICH) brings together:
- regulatory authorities
- pharmaceutical industry
to discuss scientific and technical aspects of drug registration.

Question 26

Describe the key aspects of pharmacovigilance system

Answer 26

The summary of the pharmacovigilance system should be provided in Module 1.8.1
- proof of QPPV (Contact details of QPPV)
- MS where QPPV resides and operates
- Responsibilities listed in 2001/83/EC, Title IX (Parmacovigelence) eg trending / safety updates
- Reference to location of pharmacovigilance system master file (PSMF)

Question 27

How could QP monitor that delegated duties were operating correctly?

Answer 27

Quality councils, Reach out sessions, Quality Management Review Meetings, QA department review meetings, Self inspections, Deviation & Root cause monitoring, Corporate Quality KPI/metrics, PQRs

Question 28

How would you launch a new product and submit an MAA?

Answer 28

Follow all the relevant ICH guidelines and Eudralex volume 4 guidelines during development and in setting up for commercial manufacture/ testing. Also follow EMA preauthorisation guidance Q&A
* decentralised procedure (DCP) : > 1 MS - Reference and conscerned MS review
* mutual recognition procedure if already authorised in a MS - (National is reference MS and need a conscerned)
* national procedure if you want to market a medicine only one MS
* centralised procedure to EU - submit to EMA - Reference and conscerned MS review

To do evaluations, The EMA have access to committees eg - Committee for Medicinal Products for Human Use (CHMP), the Pharmacovigilance Risk Assessment Committee (PRAC) and the Committee for Advanced Therapies (CAT). Timing applications appropriately enables the working plan to be as efficient as possible.

Question 29

What is the role of the RPi?

Question 30

What is the role of the DMRC?

Answer 30

Defective Medicines Report Centre

minimise the hazard to patients arising from the distribution of defective medicines by providing an emergency assessment and communication system between manufacturers, distributors, wholesalers, pharmacies, regulatory authorities and users.

Question 31

You have 4 QPs on site and they cannot agree to the batch disposition on one batch which has an issue, what do you do?

Question 32

What are recent regulatory updates for UK and EU? What is NIMAR and Northern Ireland protocol?

Question 33

What are the two laws governing UK medicines?

Answer 33

HMR SI 2012:1916
SI2004:1031

Question 34

What is 536/2014? From the new detailed commission guideline (new Annex 13) what are the principles UK decided to adopt?

Question 35

What is the content of PSF and IMPD?

Question 36

How are vaccines released in UK ? What is role of NIBSC ?

Question 37

Who is RPI? How is he/she different to RP role?

Question 38

What are the changes to Annex 1? What is Contamination control strategy?

Question 39

API site is moving from UK to India. Finished product site is moving from UK to South Africa. What documents would you require and how would you manage this change?

Question 40

You mentioned ‘Approved Country’s’ what are these?

Answer 40

White List for the UK

• Brazil
• Israel
• Switzerland
• Korea
• Austraulia
• Japan
• USA

Question 41

Commercial EU & UK product moving their manufacturing & testing plant from Romina to Egypt.
- Where would the testing facility need to be located for EU and UK QP certification (I think they wanted me to demonstrate that importation testing performed in the EU doesn’t need to be repeated in the UK)

Question 42

What can you tell me about Brexit from a QP perspective?

Question 43

What can you tell me about COVID from a QP perspective? Have you heard of regulation 174?

Question 44

What are the differences to certification process for blood derived products or vaccines?

Answer 44

Batches of biological medicines require national certification before they can be placed onto the Great Britain market.

NIBSC
Great Britain will carry out its own independent certification of batches of biological medicines at the NIBSC.
The expectation is that the NIBSC will independently test and certify batches that are to be used exclusively in the UK.

Exception: batches that were manufactured and certified by a country with whom the UK has a relevant Mutual Recognition Agreement (MRA). UK will have an MRA in place to cover batches manufactured and released in Switzerland or Israel.

Question 45

Vaccine made and packed in USA, certified in GB. Concerns? What needs to be in place for QP. What if they want to speed things up and send samples separate to batch?

Question 46

Tell me about recent legislative changes impacting the UK

Answer 46

IRP - International Recognition Procedure
Effective as of 01 Jan 2024
Licensing route using reference regulators (EU, Australia, Canada, Japan, Switzerland,, Singapore, USA)

Windsor Framework
Approval of medicines for the whole UK market, including NI
Pack must include ‘UK only’
implementation 01 Jan 2025

Question 47

Changes in guidance?

Answer 47

ICH Q2 - Validation of Methods
ICH Q14 - Analytical Method development
changes around stability indicating properties, using performance charateristics for different techniques, covering QbD