L2

Question 1

QbA

Answer 1

Judge quality of a medicine by its appearance

Question 2

QbT

Answer 2

Test quality into a product (quality by testing of finished product)

• product tested at the end of batch manufacturing process
• if product passes test(s), it was deemed to be of good quality

Question 3

Limitations of conventional product testing

Answer 3

• you test only on a ‘representative’ sample size (most testings are destructive in nature)
• you can test only if you know the analyte (ingredients: APIs, excipients) and you have a test method
• you can test only if test method is specific, accurate and reliable ie. if it is validated

Question 4

Historical development of pharmaceutical product quality

Answer 4

QbA -> QbT -> QbD

Question 5

QbD

Answer 5

Design and build quality into a product

Question 6

Limitations/Disadvantages of Sterility Testing

Answer 6

• high (statistical) probability of passing sterility test, even when contamination level is relatively high
• sterility test is not cheap, several hundred SGD
• 2 weeks of incubation period needed for sterility test
• sterilised product cannot be released in real time: expensive cost of storage space during quarantine of bulky products eg. large volume parenterals (LVP)

Question 7

Limitations of sterility testing led to develpment of

Answer 7

Parametric release of terminally-sterilised LVPs (annex 17)

Question 8

parametric release

Answer 8

annex 17: release of a batch of injectable product which has been terminally sterilised (by dry/moist heat sterilisation), without the need to conduct batch sterility testing
- release of a batch of injection based on CPPs (critical process parameters eg. autoclaving - moist heat) which has been rigorously validated (sterilisation assurance level <= 10^-6)

Question 9

examples of CPPs

Answer 9

temperature, pressure, sterilisation time/cycle, bioburden of pre-sterilised parenteral product

Question 10

What is the QRM and what is its objective?

Answer 10

annex 20: systemic framework to manage quality risk in a stepwise approach comprising risk identification, analysis, reduction and communication
- objective: assess risks to product qulity/patient, and then manage these risks to an acceptable level

Question 11

quality should be the concern and business of:

Answer 11

(1) manufacturer
- product and manufacturer’s licence holder
- distributer and advertiser
- r&d scientists
- production/QC experts

(2) regulator ie. HSA
- product quality reviewers
- GMP inspectors
- analytical scientists

^ hard skills set, knowledge and equipment to assure good quality medicines

Question 12

hard skills and knowledge required: (7)

Answer 12

• pharmacology/pharmacotherapy (drug actions, drug treatments)
• medicinal chemistry (including drug synthesis and analysis)
• pharmaceutics (incl dosage from design, mfg processes)
• pharmaceutical microbiology (especially sterilisation and disinfection)
• pharmaceutical laws (ie MA, HPA)
• GMP and quality standards (including validation and stability studies)
• statistics eg. ANOVA, SPC ie. statistical process control

Question 13

what is a contaminated medicinal product?

Answer 13

defined as a product that contains undesirable foreign matters

• of chemical or microbiological nature (for non-specific in nature)
• may be present in a starting material, intermediate, bulk product
• introduced during manufacturing: procurement, sampling, processing, packaging, re-packaging, storage or transportation (cross-contamination)

Question 14

How is homogenity demonstrated?

Answer 14

Through process validation

Question 15

What is process validation?

Answer 15

US FDA, UK MHRA, EMA, Australia TGA PIC/S, WHO

• means of ensuring and providing documentary evidence
• that manufacturing processes are capable of consistently produce a finished product of required quality
• carried out on at lesat 3 consecutive full-scale batches