prequalification programme quality control laboratories testing projects jitka sabartova...
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Prequalification ProgrammePrequalification ProgrammeQualityQuality Control LaboratoriesControl Laboratories
Testing ProjectsTesting Projects
Jitka Sabartova
Prequalification Programme: Priority Essential Medicines
HSS/PSM/QSM
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 2 |
Prequalification Programme for Priority Essential Medicines
Prequalification Programme for Priority Essential Medicines
A United Nations Programme managed by WHO
Action plan of UN from 2001 for expanding access of patients to priority medicines for treatment of
– HIV/AIDS– Malaria– Tuberculosis– Reproductive health– Potentially other categories of products
• Antiviral medicines efficacious for avian flu• Paediatric formulations
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 3 |
Prequalification Programme for Priority Essential Medicines
Prequalification Programme for Priority Essential Medicines
WHO PQ Team working in co-operation with partners
– UNICEF
– UN Population Fund (UNFPA)
– UNAIDS
– UNITAID
– The Global Fund
– World Bank
– Anti-malarial and anti-TB products: Roll Back Malaria and Stop TB (Global Drug Facility); HIV/AIDS Department
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Prequalification Programmefor Priority Essential Medicines
Prequalification Programmefor Priority Essential Medicines
Objective
To ensure quality, efficacy and safety of medicines procured using international funds (e.g. GFTAM, UNITAID)
Components Evaluation of Quality, Safety and Efficacy of prioritised Essential
medicines, inspections of manufacturers and monitoring of the products after their prequalification
Prequalification of quality control laboratories Building capacity of regulators, manufacturers and quality control
laboratories
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Prequalification of QC laboratoriesPrequalification of QC laboratories
Need to increase the access to QC laboratories that
– meet recommended standards for testing of medicines
– are committed to provide a service of testing of medicines, including but not limited to HIV/AIDS, Tuberculosis and Malaria products to UN agencies
Procedure established in 2004
Participation of a QC laboratory is voluntary
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Procedure for assessing the acceptability, in principle, of quality control laboratories for use by UN agencies
Procedure for assessing the acceptability, in principle, of quality control laboratories for use by UN agencies
Published in 2004 (WHO TRS, No. 917, Annex 4)
Revision published in 2007 (WHO TRS, No. 943, Annex 5)
Related documents– Good practices for national pharmaceutical control laboratories (WHO
TRS, No. 902 Annex 3)
– WHO GMP: main principles for pharmaceutical products. In: Quality assurance of pharmaceuticals. A compendium of guidelines and related materials. Vol. 2, 2nd updated edition. Good manufacturing practices and inspection (Geneva, World Health Organization, 2007)
– Guidelines for preparing a laboratory information file (WHO TRS, No. 917, Annex 5)
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Based on the following principlesBased on the following principles
Reliance on the information supplied by the national drug regulatory authority
General understanding of the quality control activities of the laboratory
Evaluation of information submitted by the laboratory
Assessment of consistency in quality control through compliance with GMP(s) and WHO guidelines
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Invitation for Expression of InterestInvitation for Expression of Interest
3rd EOI published in September 2007– http://www.who.int/prequal/info_applicants/eoi/EOI-QCLabsV3.pdf
Previous invitations limited to QC laboratories in Africa, currently no regional limitation
Priority in the assessment will be given to– National QC laboratories and laboratories providing testing
services to the government– QC laboratories in areas where UN agencies identify the need for
quality testing
Any laboratory (private or governmental) can participate
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Steps of the procedureSteps of the procedure
1. Expression of interest
2. Submission of laboratory information− Laboratory Information File - LIF needed to get basic information on
laboratory's activities and suggested scope of prequalification
− A good LIF makes the procedure faster
− Guidelines for preparing LIF available• Documentation and QA system, Personnel, Handling of samples, Materials,
Premises, Equipment, Contract operations and activities, Out-of-specification investigation, Self-inspection
• Stability Testing, Microbiological testing, Water system, where applicable − Quality Manual can be submitted (amended as necessary)− Evidence of participation in proficiency testing schemes
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Steps of the procedureSteps of the procedure
3. Screening of submitted laboratory information− Formal completeness
− Amendment requested, if necessary
4. Evaluation of the laboratory information− To assess the laboratory's potential to pass successfully the
inspection
− If the LIF indicates that the laboratory would comply - WHO starts arranging an inspection
– If the LIF is not adequate – WHO• Starts arranging an inventory audit or• Asks for more information or• Returns the LIF
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Steps of the procedureSteps of the procedure
5. Site inspection / inventory audit
− Planned and coordinated by WHO (normally for 2-3 days)
− Experts appointed by WHO preferably from regulatory authority inspectorates, experienced in quality control
• Required to sign declaration of interest and confidentiality declaration
− Compliance with WHO recommended standards• Good Practices for National Pharmaceutical Control Laboratories• Good Manufacturing Practices as recommended by WHO for such
laboratories– ISO certification encouraged and considered– However, GMP aspects to be taken into account during inspection
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Steps of the procedureSteps of the procedure
5. Site inspection / inventory audit (cont.)
− For the inspection representative(s) of the DRA of the country where the laboratory is located invited
− Inventory audit less formal, combined with discussions of problems and assessment of need of technical assistance
– Possibility to recognize the outcome of an inspection done by another authority/organization?
• Detailed comparison of standards• Availability of the audit report• Case by case consideration
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Steps of the procedureSteps of the procedure
6. Report and outcome of evaluation− Final Report in the established WHO format communicated to the
laboratory and a copy sent to the national DRA– If corrective actions to be taken by the laboratory, WHO
postpones its final conclusion until evaluation of corrective actions− In case of disagreement, possibility of an appeal− Ownership of the report lies with WHO
7. Results of assessment– Information is sent to the laboratory and national DRA– If compliant, laboratory is included in the published list and
WHOPIR is published– The list will be subjected to review at least once a year
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Steps of the procedureSteps of the procedure
8. Re-evaluation after prequalification - on-going monitoring− Re-inspections at regular intervals (normally 3 years)
− Evaluation of results from participation in proficiency testing• WHO External Quality Assurance Scheme, AFSSAPS network of Francophone
African countries
− Brief report to be submitted annually• Overview on number of analysed samples, methods used, services provided to
UN agencies• Outcomes from proficiency testing• Changes to key personnel, facility or other significant impact to the laboratory• Update of LIF, in case of changes with significant impact on LIF content
− WHO may suspend or withdraw a laboratory from the list when there is evidence of noncompliance
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Steps of the procedureSteps of the procedure
9. Monitoring of complaints− WHO will investigate complaints concerning the results of
analysis or service provided by the laboratory• Written report and where appropriate recommendations for action • Copy of the report to the laboratory, manufacturer of the product and
DRA of the country where the manufacturing site is located• DRA could also be invited to participate in the investigation of the
complaint
10.Cost recovery– WHO reserves the right to charge for the quality assessment
procedure on a cost-recovery basis
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 16 |
Status of prequalification of QC LabsNovember 2007
Status of prequalification of QC LabsNovember 2007
4 QC laboratories prequalified– South Africa, CENQAM - 6/2005– South Africa, RIIP - 7/2005– Algeria, LNCPP - 10/2005– South Africa, Adcock Ingram – 8/2007
2 QC laboratories near to PQ
12 QC laboratories audited, corrective measures proposed
8 QC laboratories expressed interest, but not send LIF yet– Not audited yet, information not complete or recent interest
expression
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 17 |
Frequent deficiencies and weak points (1)Frequent deficiencies and weak points (1)
Quality system– SOPs not covering, not properly maintained– No quality responsible– No or not enough internal audits
Personnel– No qualification system– Not enough training, no training programmes– Responsibilities and tasks not clearly defined on personal level,
vague organization
Premises– Too small and unfit– Limited and unfit storage areas– No regular environmental (at least temperature) monitoring– Archives not good, nor secured
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Frequent deficiencies and weak points (2)Frequent deficiencies and weak points (2)
Maintenance of the equipment – No proper or only partial qualifications– Documentation in general very deficient– Not adequate training by the suppliers in the beginning– No pre-maintenance programme
Reference materials and reagents – Maintenance system and records not efficient, nor clear– No working standards system
Instructions / methods – No clear system as to which pharmacopoeial or manufacturers'
method to use– Validations/ verifications of methods not sufficient or non-
existing
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Frequent deficiencies and weak points (3)Frequent deficiencies and weak points (3)
Waste management – Not properly organized
Safety – Fume hoods lacking or few– No or insufficient protection of the personnel
(e.g. insufficient protective garments, no training, no safety sheets of the chemicals)
– No classification nor proper storage of dangerous chemical materials (e.g. toxics, caustic / volatile reagents etc.)
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 20 |
Technical assistanceTechnical assistance
Capacity building and technical assistance provided to national QC laboratories
– Out of the scope of prequalification procedure
Technical assistance provided to 5 national medicines quality control laboratories
– Assistance in implementation of quality system
– Assistance in microbiological testing
– 1 – 3 weeks
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TrainingTraining
Participation in Quality Assurance training of OMCLs organized by EDQM
– October 2005, 5 participants from AFRO and EMRO
– September 2007, 12 participants from AFRO, EMRO and EURO
Trainings in Quality Assurance, Quality Control and Ph.Int. under preparation
– November 2007, Morocco, 47 participants from Francophone countries (AFRO, EMRO), cooperation with EDQM
– December 2007, Tanzania, 50 participants from Anglophone countries (AFRO, EMRO, AMRO/PAHO)
Trainings planned in 2008– Market surveillance projects, Networking of African laboratories
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Sampling and testing of medicinesSampling and testing of medicines
Policy
– To monitor quality of supplied prequalified products• Required by the procedure for products prequalification
– To contribute to quality control of other products procured by UN agencies
– To contribute to quality control of products, if requested by Member States
Prequalified laboratories used for testing, if available
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Survey of the quality of antiretroviral medicines circulating in selected African countries (1)
Survey of the quality of antiretroviral medicines circulating in selected African countries (1)
Carried out in June-December 2005, report finalized this year
42 collection sites in 7 countries– Cameroon, DR of Congo, Kenya, Nigeria, Tanzania, Uganda and
Zambia
Monocomponent products (didanosine, efavirenz, lamivudine, nevirapine, stavudine, zidovudine) and FDCs (lamivudine/zidovudine, stavudine/lamivudine, stavudine/lamivudine/nevirapine)
394 samples from official procurement and treatment centres, both private and public, around capital cities
– Good logistic organization, no deterioration of samples, no expired sample sent for testing
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Testing
– Samples tested in Swissmedic – official medicines control laboratory of Switzerland
– According to Ph.Int., USP, Indian Pharmacopoeia, validated in-house Swissmedic methods
– Tests performed• Appearance• Labelling• Identification• Uniformity of mass (capsules/tablets)
Survey of the quality of antiretroviral medicines circulating in selected African countries (2)
Survey of the quality of antiretroviral medicines circulating in selected African countries (2)
• Dissolution/disintegration• pH (oral solutions-depending
upon the matrix)• Related substances• Content of each active ingredient
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Survey of the quality of antiretroviral medicines circulating in selected African countries (3)
Survey of the quality of antiretroviral medicines circulating in selected African countries (3)
Findings– Very low failure of 1.8%, no critical deficiencies
• 1 sample broken tablets, 2 samples insufficiently labelled, 1 sample higher API content, 1 sample failed to disintegrate in 30', 2 samples lower dissolution
• 53% prequalified products• In 3 countries found non-registered products, mostly in private
sector (12% of 394 samples)
– Positive effect of common efforts of NDRAs, WHO and others involved in prequalification and purchase policies
– Limited to official distribution points and treatment centres around the capital cities
• Positive outcome cannot be generalized to the entire territories of the countries surveyed
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Current sampling and testing activities (1)Current sampling and testing activities (1)
Comparative dissolution study of Coartem tablets– Artemether / lumefantrine innovator - problems with dissolution reported from
various sides
– 5 batches manufactured in different manufacturing sites and collected in Tanzania tested in RIIP, South Africa
– Dissolution profiles of compared to the mean of all data SIMILAR
Generic products containing nelfinavir– Test on EMS/MMS impurity using Roche method
– Search for manufacturers placing product on markets – 2 in India, 1 in Thailand
– Samples collected from manufacturers, as well as from markets
– For the purposes of Ph.Int. monograph dissolution study added
– Testing on-going in Swissmedic
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 27 |
Current sampling and testing activities (2)Current sampling and testing activities (2)
Testing samples on request from countries– Arsuamoon tablets (co-blistered artesunate+amodiaquine), Guilin
Pharma, China• Request from Indonesia, local procurement by donors, concerns about
authenticity• 2 batches tested in RIIP, South Africa artesunate tablets compliant with
Ph.Int., amodiaquine tablets compliant with USP
– Diethylcarbamazine citrate tablets, Asian Pharmaceutical Company, Nepal
• Request from Nepal, serious adverse events reported, MoH asked for independent testing before distribution of further batches
• 4 batches tested in RIVM, Netherlands compliant with USP
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 28 |
Current sampling and testing activities (3)Current sampling and testing activities (3)
Quality survey of antimalarials
– Most sold and recommended by national guidelines ACTs (co-packed and FDCs) and sulfadoxine-pyrimethamine, oral dosage forms
– In 9 African countries (Cameroon, Ethiopia, Ghana, Kenya, Madagascar, Nigeria, Senegal, Tanzania, Uganda)
– Covering whole distribution chain (private and public) and informal market throughout the country
– First testing using GPHF-Minilab, part of samples then tested in a laboratory (identification, dissolution/disintegration, content of APIs)
– Collection of samples in countries being prepared in extensive cooperation with WHO country offices and NDRAs
– Assessment of quality of product information (Labelling and PIL)
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 29 |
Current sampling and testing activities (4)Current sampling and testing activities (4)
Quality monitoring within UNITAID projects
– Strengthening of quality control of products as close to patients as possible, in close cooperation with NDRAs (capacity building)
– Pilot phase under preparation - paediatric ARV FDCs, cotrimoxazol, second line ARVs in Kenya, Tanzania, Uganda and Zambia
– Framework protocol supplemented by country specific sampling and testing plans
– Assessment of quality of product information (Labelling and PIL)
Monitoring of quality of WHO prequalified products– Verification that WHO-prequalified products procured by agencies comply
with the specifications approved within PQ process
– In cooperation with NDRAs
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Systematic approach to sampling and testing of medicines
Systematic approach to sampling and testing of medicines
Objectives– Products which are prequalified and procured using international
funding are subject to systematic risk based quality testing• Probability of poor quality, severity of health risk, size of exposed population, …
– Urgent testing is organized, if needed– Member States are supported in quality testing, if requested– Outcomes of testing are reflected in appropriate measures
Quality team– Assessor/s, inspector/s, PhV expert, pharmacopoeial expert, QCL
coordinator, external expert/s (if needed)– Discussion of project proposals and immediate signals, application of
risk analysis, projects outcomes, actions needed
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 31 |
Sampling and testing projectsSampling and testing projects
Conduct of projects
Commitments)PQ procedure,
Agreements(
Plan+updates
P1 P1-out P2-out P3-outP2 P3
ReportsActions
InspectionsAssessment
PhV
Entryinformation
)Quality concerns,complaints/defects ,
signals(
QCL Training | 5-7 December 2007, Dar es Salaam, Tanzania 32 |
Thanks for your attentionThanks for your attentionThanks for your attentionThanks for your attention
www.who.int/[email protected]