Injectables 2 Past Paper PDF

Summary

This document provides lecture notes on injectables, focusing on formulation aspects, biopharmaceutics, and the production of long-acting injectables. It also includes examples, case studies, and discussions about the process of producing injectables.

Full Transcript

PR5217:
Injectables 2
Associate Professor Matthias G. Wacker, PhD
Department of Pharmacy | Faculty of Science
[email protected]

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 Learning outcomes
To learn about formulation aspects relevant to biologics and
biosimilars
To understand the biopharmaceutics and production of long-
acting injectables.

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 Written
Questions
in PR5217

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 Aseptic Production

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 Aseptic Production
A clean environment with different cleanroom grades, depending
on the risk associated with operations. Typically, process steps
that involve working with an open product for parenteral
administration require cleanroom grade A standard.

Sterile materials are being used.
Operators are not allowed to contaminate the product.
Stringent cleaning and disinfection protocols are being
conducted.

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 Aseptic Filtration
Terminal sterilization is the safest
method, but aseptic filtration (often
referred to as “sterile filtration”) is
also applicable to:

Thermolabile liquids Conditions according to Ph. Eur.
To remove pyrogens 0.22 µm pore size

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 Aseptic Manufacture

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 Cleanroom
Sinovac

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Source: https://www.youtube.com/watch?v=cZRMTF3yQeA
 Biologics

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 Biologics and Biosimilars

Biologics are at least partially manufactured by living
organisms. Their synthesis does not follow conventional
chemical processes and their composition is usually more
complex. Biosimilars are biologics that show very similar
clinical performance as compared to a an already approved
reference product.

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 Formulation Science
Biosimilars
Biosimilars should use the same dosage
form and the excipients are widely
identical.
Small differences in certain excipients
(e.g., human serum albumin) may not
preclude a finding of biosimilarity if data
and information provided show that the
proposed product is highly similar to the
reference product.

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 Injection Sites
Injection sites for subcutnaoeus
tissue can be arm, abdomen, or
thigh.
Injection site differences matter
more for large molecules.

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Source: Zuo et al. 2021, J Control Rel (https://doi.org/10.1016/j.jconrel.2021.06.038)
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Source: Li et al. 2021, J Pharm Sci (https://doi.org/10.1016/j.xphs.2021.10.031)
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 Protein Formulation
Biologics commonly require formulations improving their
chemical stability (shelf life).
Common stabilizers are surfactants and buffers that keep
the pH at a constant level and lower interactions in highly
concentrated protein solutions
(IgG antibodies ~2-150 mg/mL).
Lyophilization requires specific ingredients such as
lyoprotectants and cryoprotectants.

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 Case studies:
Antibodies

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 Pharmaceutical Development

Route of administration Physical form Functional requirements

Oral Sterility
Solid
Topical
Viscosity
Semisolid
Parenteral
Particle size
Rectal
Liquid
Release behavior
Inhalation
Gas Stability
Ophthalmic

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 Erbitux®
Erbitux (Cetuximab) is an antibody indicated
for the treatment of patients with recurrent
or metastatic squamous cell carcinoma
of the head and neck for whom prior
platinum-based therapy has failed.

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 Regulatory Requirements
European Pharmacopeia
Parenteral preparations are sterile preparations
intended for administration by injection, infusion or
implantation […]. Containers for parenteral
preparations […] are sufficiently transparent to permit
the visual inspection […].

Injections are sterile solutions, emulsions or
suspensions. They are prepared by dissolving,
emulsifying or suspending the active substance(s) […]
in water for injections […].

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 Excipients
Erbitux®
Formulation type: Solution for injection

Inactive ingredients:
Glycine
Polysorbate 80
Sodium chloride
Citric acid monohydrate
Sodium hydroxide
Water for injections

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 Antibody solutions are typically highly concentrated
Excipients in parenterals.
Antibody Sodium chloride and aminoacids are typically used.
Solutions Buffers adjust the pH and differ between lyophilized and
non-lyophilized products.

Viscosity reduction Buffers Tonicity
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Source: Strickley and Lambert 2011, J Pharm Sci (https://doi.org/10.1016/j.xphs.2021.03.017)
 Excipients
Erbitux®
Adsorption to various materials reduces due
to the presence of polysorbate.
Steric stabilization decreases the occurrence
of larger agglomerates in antibody solutions.

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Source: Mahler et al. 2010, J Pharm Sci (https://www.doi.org/10.1002/jps.22045); Kiese et al. 2008, J Pharm Sci (https://doi.org/10.1002/jps.21328)
 Excipients
Erbitux®
Glycin weakly interacts with proteins, leading to a certain steric
stabilization.
Competition for water between the unfolding protein and
glycine increases stability.
All amino acids have a certain buffer capacity.

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© Copyright National University of Singapore. All Rights Reserved.
Source: Li et al. 2021, J Pharm Sci (https://doi.org/10.1016/j.xphs.2021.10.031)
 Injection Site
Absorption of larger molecules
(antibodies) depends on injection site.
Bioavailibility differences
Abdomen 64%
Arm 75%
Thigh 71%
Muscle 81%
IV 100%

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Source: Li et al. 2014, Clin. Pharmacol. Drug. Dev. (https://doi.org/10.1002/cpdd.60)
 Case study:
Long-acting injectable

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 Pharmaceutical Development

Route of administration Physical form Functional requirements

Oral Sterility
Solid
Topical
Viscosity
Semisolid
Parenteral
Particle size
Rectal
Liquid
Release behavior
Inhalation
Gas Stability
Ophthalmic

© Copyright National University of Singapore. All Rights Reserved. 28
 European Pharmacopeia
Parenteral preparations are sterile preparations
intended for administration by injection, infusion or
implantation […]. Containers for parenteral
preparations […] are sufficiently transparent to permit
the visual inspection […].

Injections are sterile solutions, emulsions or
suspensions. They are prepared by dissolving,
emulsifying or suspending the active substance(s) […]
in Water for injections […].

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 Medroxyprogesterone acetate
Medroxyprogesterone acetate (MPA) is a drug substance used
as birth control.

Molecular weight 386.52 g/mol
Peroral bioavailability 99%

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 Dosage Form
MPA has an aqueous solubility
of approx. 1.54 ± 0.60 μg/mL
and is formulated at 160 mg/mL.
Micronized suspension for
subcutaneous injection into
abdomen or thigh (no clear
instruction).

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Source: Gao et al. 2020, Int. J. Pharm. (https://dx.doi.org/10.2165/00044011-199714010-00005)
 Biopharmaceutics
Low blood levels of MPA are
required for the pharmacological
effect.
Intramuscular administration
guarantees a long duration of
action after a single injection.

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Source: Gao et al. 2020, Int. J. Pharm. (https://dx.doi.org/10.2165/00044011-199714010-00005)
 Selected Target Requirements
Safety
Sterile
Non-pyrogenic preparations

Efficacy
Stable with controlled particle size
Optimized dissolution rate for long-term absorption
Syringable

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 Injection Site
Small molecules are typically less
affected by differences in the injection
site.
Long-acting injectables are more
susceptible as they have a longer
absorption process.

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Source: Gao et al. 2020, Int. J. Pharm. (https://dx.doi.org/10.2165/00044011-199714010-00005)
 Depo-SubQ Provera®
Formulation type: Suspension for injection

Inactive ingredients:
Medroxyprogesterone acetate
Methylparaben
Propylparaben
Sodium Chloride
Polyethylene Glycol
Polysorbate 80
Monobasic Sodium Phosphate

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 Process Technologies

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 Formulation Technologies
Sterilization Technologies (Injectables 1 lecture)
Hot Melt Extrusion (Injectables 1 lecture)
Homogenization Technologies
Lyophilization (Lyophilization lecture)

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 High Pressure Homogenization
High pressure homogenization uses high shear forces to mill
particles down to the lower micrometer scale.
Milling process occurs in a closed batch production process
that makes it easy to keep the product sterile.
Stability of the product can be a critical issue (e.g., hardly
suitable for proteins).

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 High pressure homogenization

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Source: https://www.youtube.com/watch?v=E-C7DXzAKZM
 Wet Bead Milling
Wet bead milling produces particles by grinding and shearing
the product.
Friction is achieved by using the milling medium composed of
ultra-crosslinked milling beads.

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 Wet bead milling

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Source: https://www.youtube.com/watch?v=jxmujqREj50
 Summary
Type of injection is often selected based on the desired
pharmacokinetics.
Parenterals come with specific requirements with regards to
chemical, physical and microbiological contamination.
Protein formulations are challenging because of the stability
issues arising from the structure.
Long-acting injectables are developed when there is medical
need; the release behavior plays an important role.

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 Questions in
PR5217
Answers provided
twice a week

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 Thank you!

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