formulation TD

Question 1

skin anatomy

Answer 1

• Stratum corneum
  
  • Top 10um layer of skin
• epidermis
  
  • Cells flatter, more keratinised moving up through layers
• Dermis
  
  • Blood vessels, macrophages, mast cells
  • Sebaceous glands, hair glands

Question 2

stratum corneum (main barrier)

Answer 2

• Top 10um layer of skin
• 10-20 layers of flattened, stratified, fully keratinised dead cells
• Primary barrier to drug crossing the skin
  
  • Brick and mortar structure
    ○ Ordered, rigid bilayer structure
    ○ Access primarily via: intracellular lipidic domains
  • Lipids, cholesterol, fatty acids, ceramides

Question 3

skin delivery 2 ways

Answer 3

topical
transdermal

Question 4

topical

Answer 4

• Shallow skin penetration
• Local delivery
• Cosmetics, antiseptics (local wound that affects only surface layer), anti-inflammatories

Question 5

transdermal

Answer 5

• Deep skin penetration (across stratum –> epidermis –> adipose tissue –> dermis –> blood vessels)
• Systemic delivery
  - Nicotine, pain relief, hormonal regulation
  - Protects pdt + retain on surface of skin

Question 6

adv of TD

Answer 6

• Controlled release
  ○ Reservoir: (amt of drug + conc loaded into reservoir)
  ○ Duration of conTDtact: (size of patch, duration)
  ○ Decr dosing freq
• No GI degradation/ irritation
  ○ More local skin irritation
• Bypass hepatic 1st pass effect
• Easy termination of input
  ○ Peel off and admin of drug stops, not high plasma conc left
• Non-invasive
  ○ Painless, no skin breeched

Question 7

disadv of TD

Answer 7

• Variability b. people and location of admin on body
  ○ Thickness of skin differs
• SC
  ○ Slows absorption, barrier
  ○ Rate limiting step
• Skin irritation
  ○ Adhesive layer – removal
  ○ Drug int on skin surface
• Easily removed by pt
• Metabolic enzymes (specific chemical functional grps?)
• BBB (via systemic delivery)
• Systemic SE

Question 8

8 factors that affect delivery

Answer 8

• Skin condition: age, disease, injury, site
• Skin thickness (diffusion layer)
• Hydration of skin (stratum corneum)
• Stimulation of skin
  
  • Phonophoresis/ ultrasound – vibration
  • Iontophoresis – heat
• Physicochemical properties of drug
  
  • Lipophilicity, diffusion coefficient – LogP, size
• Permeation enhancers (eg ethanol)
  
  • Reversible reduction in barrier resistance of SC w/o damaging viable cells
• Conc gradient
  
  • Patch reservoir –> skin
  • 50% of Drug left in patch as there must be FLUX
• Area of contact b. formulation & skin (SIZE)

Question 9

hydration by

Answer 9

• Natural: hydration, humidity
• Manufactured:
  ○ Chemically (moisturise)
  ○ Physically (occlusive layer to trap water at site)

Question 10

hydration affects

Answer 10

Water absorbed by lipid channels in between
Lipid channel widens, facilitate flow/ permeation of drug
- Size of corneocytes remain the same
- The gaps between WIDENS, better permeation

Question 11

brain access via TD

Answer 11

Skin (barrier) –> blood –> (barrier) brain

* Drug sol flows through circ system 
	○ Reticuloendothelial system (RES) 
	○ Unless active targeting, drug is distributed everywhere =unwanted SE  
* Drug bypass BBB to access the brain 
	○ Blocks ~98% of small mole drug candidates 
	○ Paracellular (tight junctions) << transcellular transport

Question 12

transcellular transport via

Answer 12

1) Active efflux transporters (REMOVE from organs into lumen)
○ P-gP, BCRP (breast cancer resistance protein), MRP (multi-drug resistance protein)

2) Endocytosis mediated transporters (INTO by Specific molecules/ functional grp binding)
○ Carrier-mediated transporters (LAT1, GLUT1, MCT1, OCTN2)
○ Receptor-mediated transporters (IR, TfR)

Question 13

TD drug candidate lipinski

Answer 13

• logP 1-3
  if too hydrophobic: repelled, still needs to be transported systemically
• unionised

Question 14

TD formulations

Answer 14

• Topical: gel, creams (w-based/ oil-based), ointment
• TD: patches
  ○ Sol/ susp in reservoirs
  ○ Polymer matrix

Question 15

TD excipients

Answer 15

• Preservatives - reduce microbial growth
• Solvent, co-solv - dissolve drug
• Viscosity modifier - flow of formulation in reservoir
• Permeation enhancer - in contact w/ SC
  ○ Bioadhesive (stick to mucus layer)
  ○ SR agent (complex matrix)
• Adhesives - stick to skin
  ○ May have properties: viscosity enhancers, matrix polymer
• Polymer matrices (SR)

Question 16

polymer matrices and Drug release depends on:

Answer 16

• Diffusion coefficient of drug
• SA
• Conc of polymer > dilute (more crosslink)
• Porosity/ tortuosity of polymer matrix
  * Intramolecular interactions (crosslink, H bonds)

drug encapsulated between matrix, diffuse out slowly

Question 17

permeation enhancers
- interaction with intercellular protein
- improve partition of the drug into stratum corneum

Answer 17

cyclodextrin
glyceryl monoleate
ethanol
propylene glycol

Question 18

solvent

Answer 18

ethanol
propylene glycol

Question 19

viscosity modifier

Answer 19

carboxymethyl cellulose, HPMC
hyaluronate sodium
calcium alginate
carbomer
poly(methyl vinyl ester/ maleic anhydride)

Question 20

matrix polymer

Answer 20

glyceryl monooleate (SR agent)
carboxymethyl cellulose, HPMC
hyaluronate sodium
calcium alginate
povidone (SR)

Question 21

adhesive

Answer 21

calcium alginate
carbomer
povidone
poly(methyl vinyl ester/ maleic anhydride)

glyceryl monooleate (bioadhesive)
silicone, rubber, adhesives

Question 22

humectant

Answer 22

hyaluronate sodium

hydrates skin, better permeation (brick, mortar)

Question 23

packaging and storage

Answer 23

• Patches sealed in indiv pouches
  ○ Plastic/ polymer lining (maintain hydration in patch)
  ○ Al lining (protect from light degradation)
• Sealed packaging
  ○ Maintain integrity of adhesive
  ○ Maintain integrity of pdt (oxidation, reduction, temp)
  ○ Maintain hydration

Question 24

designs of patches (3)

Answer 24

1) membrane patch (bulky, reservoir, matrix, adhesive separate)

2) matrix patch (drug in matrix, no reservoir)

3) drug-in-adhesive matrix patch (drug+polymer+adhesive)

• calcium alginate
• povidone

Question 25

parts of a patch

Answer 25

• backing layer (ontop, impermeable)
• membrane (polmer matrix)
• adhesive
• liner (protects adhesive, remove just before admin)

Question 26

backing layer

Answer 26

○ Impermeable layer (plastic/ polymer lining, additional Al lining)
○ Protects drug and contents
○ Maintain patch: hydration, stability (light, Oxidation)
○ support and protection of drug-loaded adhesive from environ

Question 27

membrane, polymer layer

Answer 27

○ Polymer matrix
○ Release rate depends on:
* Composition/ chemistry, thickness and porosity/ tortuosity (channels in matrix)

Question 28

adhesive

Answer 28

silicone, rubber, adhesives

permeatiion enhancers (prime skin for better permeation)

Question 29

special considerations of TD patch

Answer 29

• release rate of drug
  * toxicity/ ADR/ ineffectiveness
  * temp (no heated blankets, incr SE)
  * crystallinity of drug over time
• strength of adhesion
  * b. clothes layers, influence of sweat, hair
• disposal of patch
  * high conc left in patch –> needed to create a flux (release)

Question 30

release rate of drug affected by

Answer 30

• potential for leaching, extraction of drug from backing
  * drug remains in reservoir, not fluxed/ released
  * substances from backing layer (may be toxic) leached
• temp (not use heated blankets, incr SE)
• crystallinity of drug over time (crystal/ amorphous – melting point)

Question 31

rotigotine/ neupro

Answer 31

• drug in adhesive
• dopamine receptor agonist (PD)

backing film, drug matrix, protective liner

Question 32

admin of patch

Answer 32

• Apply on skin that was not used previously
  ○ Adhered skin is more tender, rate of drug penetration affected
  ○ rotate sites, not repeat in 14d
  ○ shave hairy site 3d before apply
• Immediately apply to skin after peeling protective layer from adhesive
  ○ Exposed to microbials
  ○ Affect adhesiveness of patch
• 30s Warm up area to activate adhesion
  ○ Better adhere to skin

Question 33

rotigotine API

Answer 33

• MW: 315.48 g/mol
• logP: 4.7
• Hydrogen bond donor (1)
• Hydrogen bond acceptor (3)
• Ionisable –yes 3*amine & OH
  ○ pKa is weak, affected by pH of body + formulation
  ○ Usually uncharged to have higher LogP, better partition into lipo layer of skin
  ○ may become ionised for systemic circulation

Question 34

rotigotine composition

Answer 34

• Ascorbyl palmitate – antioxidant
• Sodium metabisulfite – antioxidant
• DL-alpha tocopherol vit E – anti oxidant
• Povidone – polymer, SR, adhesive
• Silicone adhesive

Question 35

PK/PD of rotigotine

Answer 35

• ~45% released in 24hrs (0.2mg/cm2)
  ○ Cmax dependent on patch dose
• repeated daily use to maintain steady state conc
• After removing patch,
  ○ Plasma lvl decr with t1/2: 5-7hrs

Question 36

fentanyl/ duragesic

Answer 36

• opioid agonist – pain relief (repeat 72h application)
• drug in membrane (bulky: reservoir, release mem, adhesive – separated)
• dose depeds on conc in patch + size of patch

backing layer, drug reservoir,mem, silicone, protective liner

• rotate sites, do not shave (clipped)

Question 37

fentanyl API

Answer 37

• MW: 336.5g/mol
• logP: 4.05
• Hydrogen bond donor (0)
• Hydrogen bond acceptor (2)

Ionisable, +ve charged

Question 38

fentanyl composition

Answer 38

• Alcohol *– permeation enhancer (found on adhesive)
  ○ Minute amounts, less irritation to skin
• Ethylene-vinyl acetate copolymer – matrix
• Hydroxyethyl cellulose – matrix
• Polyester – backing layer (no water passes through)
• Silicone – adhesive

Question 39

PK/PD of fentanyl

Answer 39

• SS plasma conc after ~ 3days
  ○ Large variability (pt)
• Plasma conc depend on patch dose
• large conc variability even at maintenance
• After removing patch
  ○ t1/2 ~ 7hrs