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Transcript 
GLP-vaatimukset ATMP-valmisteiden
turvallisuustutkimuksille
Tiina Palomäki
Fimea
2.9.2015
Advanced therapy medicinal products (ATMPs)
• Somatic cell therapy medicinal products
• Tissue engineered products
• Gene therapy medicinal products
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
2
Advanced therapy medicinal products
Innovative therapies for diseases and conditions for which limited or no
treatment options exist
 Degenerative diseases
Alzheimer’s disease, Parkinson’s disease, macular degeneration, diabetes
 Autoimmune diseases
Chron’s disease
 Cancer
 Tissue defects
bone, cartilage, skin, myocardial infarction, spinal cord injury
 Organ replacement
artificial liver, bladder
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
3
Cell-based medicinal products
• Somatic cell therapy medicinal products
• Tissue engineered products
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
4
Somatic cell therapy medicinal products
 cells or tissues that have been subjected to substantial manipulation so that biological
characteristics, physiological functions or structural properties relevant for the intended
clinical use have been altered, or
 cells or tissues that are not intended to be used for the same essential function(s) in
the recipient and the donor
 to treat, prevent or diagnose a disease through the pharmacological, immunological or
metabolic action
Annex I, Part IV of Dir 2001/83/EC
Tissue engineered products
 engineered cells or tissues (see above)
 to regenerate, repair or replace a human tissue
Regulation EC (No) 1394/2007
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
5
IgG ~1500 Da (~1400 aa)
Eukaryotic cell 10 μm
Aspirin MW 180
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
6
Non-clinical requirements for cell-based products
 Proof-of-concept
•
Relevant animal model(s)
 Pharmacological and toxicological effects
•
•
•
•
•
Biodistribution
Unintended differentiation
Ectopic engraftment
Tumourigenicity
Immune related effects
 Provide estimate for selection of safe and efficacious
dose in clinical studies
 Support the route of administration and feasibility of
application procedure
 Identify target organs for toxicity
 Identify parameters to be monitored in clinical
studies
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
7
Gene therapy medicinal products
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
8
Gene therapy medicinal products
 active substance contains or consists of a recombinant nucleic acid which
therapeutic, prophylactic or diagnostic effect relates directly to the recombinant
nucleic acid sequence, or to the product of genetic expression of this sequence
 to regulate, repair, replace, add or delete a genetic sequence
Part IV of Annex I to Directive 2001/83/EC
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
9
IgG ~1500 Da (~1400 aa)
Eukaryotic cell 10 μm
Aspirin MW 180
Virus particle 20-300 nm
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
10
Non-clinical requirements for gene therapy products
 Proof-of-concept
•
Relevant animal model(s)
 Pharmacological and toxicological effects
•
•
•
•
•
•
•
•
•
Biodistribution
Persistence
Ectopic transgene expression
Recombination and mobilisation of a vector
Induced cellular changes
Insertional mutagenesis
Germline transmission
Immune related effects of a transgene and a vector
Virus shedding
 Provide estimate for selection of safe and efficacious dose
in clinical studies
 Support the route of administration and feasibility of
application procedure
 Identify target organs for toxicity
 Identify parameters to be monitored in clinical studies
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
11
GLP requirements
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
12
Legal background
ATMP (advanced therapy medicinal products) are medicinal products the
marketing of which necessitates a Marketing Authorisation recommended by
the European Medicines Agency (EMA) and issued by the European
Commission.
 Dir 2001/83/EC as amended
• Annex I Part IV (Dir 2003/63/EC)
• Reg 1394/2007
 General requirements for all medicinal products
 Non-clinical (fpharmacological-toxicological) studies should be conducted
according to the good laboratory practise (GLP
• Annex I Part I (Dir 2003/63/EC)
 Additional specific requirements for ATMP products
• Annex I Part IV (Dir 2009/120/EC)
Lääkealan turvallisuus- ja kehittämiskeskus
2012-04-03
ATMP-tuotteiden GLP-vaatimukset Tiina Palomäki
13
Legal requirements
Proteins
Cell-based products
Gene therapy products
(EC) No 726/2004 laying down Community procedures for the authorisation and
supervision of medicinal products for human and veterinary use and establishing a
European Medicines Agency
Biotech and advanced therapy products to be authorised by the EMA
Directive 2001/83/EC Community code relating to all medicinal products for human use
Directive 2003/63/EC (Annex I of 2001/83/EC)
Analytical, pharmaco-toxicological and clinical requirements
(EC) No 1394/2007 on advanced therapy medicinal products
and amending Directive 2001/83/EC and Regulation 726/2004
Directive 2009/120/EC (Annex I, part IV of 2001/83/EC)
Technical requirements for testing of ATMPs
Dir 2004/23/EC setting
standards of quality and safety
for donation, procurement,
testing, processing,
preservation, storage and
distribution of human
tissues/cells,
Technical requirements in Dir
2006/17/EC and Dir 2006/86/EC
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
14
Clinical trials
• Regulation 536/2014 on clinical trials on medicinal products for
human use, and repealing Directive 2001/20/EC
“Non-clinical information submitted in an application dossier shall be
based on data derived from studies complying with Union law on the
principles of good laboratory practice”
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
15
Non-clinical pharmaco-toxicological requirements
Pharmacodynamics
• Primary pharmacodynamics (PD)
• Secondary PD
• Safety pharmacology
• PD drug interactions
Pharmacokinetics
• ADME
• PK drug interactions
Toxicology
• General toxicity: single and repeat-dose
• Genotoxicity
• Carcinogenicity
• Developmental and reproductive toxicity
• Local tolerance
• Immunotoxicity
• Immunogenicity
• Environmental risk assessment
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
16
Where does the drug
end-up in the body
How long does it stay there
PK
PK
Toxicokinetics
Persistence
Clearance
Longevity
Shedding
Toxicokinetics
Biodistribution
Migration
Germ line transmission
What does it do there
PD
Prim PD
Sec PD
Safety pharmacology
Differentiation
Proliferation/growth
Ectopic engraftment
TOX
General toxicity
Tumourigenicity
Genomic integration
Repro-dev toxicity
Immunogenicity
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
17
General
requirements
Special requirements for biologicals and ATMPs
Proteins
Gene therapy
Cell-based therapies
Pharmacology
Proof-of-concept
Prim PD
Sec PD
Safety pharmacology
Proof-of-concept
Tropism
(Safety pharmacology)
Proof-of-concept
Tissue integration
Tissue interaction
Bioactive molecules
(Safety pharmacology)
Absorption
Biodistribution
(Excretion)
Biodistribution, persistence,
clearance, mobilisation,
germ line transmission
viability, longevity,
distribution, growth,
differentiation and
migration
Single and repeat-dose
toxicity
Can be included in POC
studies
Can be included in POC
studies
Genotoxicity
(-)
(-)
(-)
Carcinogenicity
Included in chronic tox
studies
Insertional mutagenesis
Tumourigenic potential
Repro-dev toxicity
Repro- dev toxicity
Fertility, reproductive
potential
(-)
Other toxicity
Immunogenicity
(Immunotoxicity)
Immunogenicity
shedding
Immunogenicity,
immunotoxicity,
xenopathogen transmission
(-)
GMO ERA
(-)
Prim PD
Sec PD
Safety pharmacology
Pharmacokinetics
ADME
TK
Toxicology
Single and
repeat-dose toxicity
ERA
Lääkealan turvallisuus- ja kehittämiskeskus
18
GLP requirements
 GLP requirements the same regardless of the product class!
 Nonclinical studies according to the GLP requirements
• All pivotal studies to which nonclinical safety is based on
• Safety pharmacology and toxicology studies
 Pharmacological characterisation and proof-of-concept studies generally nonGLP
• When pivotal safety end-points are included in a POC study the study
should be conducted under GLP
 Full GLP compliance may not always feasible
• Deviation may be justified due to product related issues
• GLP principles must be followed to the extent possible
• Non-GLP and possible impact to the overall safety assessment need to
be justified
• Acceptance on a case by case basis
Lääkealan turvallisuus- ja kehittämiskeskus
4.5.2017
GLP seminar
19
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