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Microencapsulation for Cosmetic Application
Kelompok III
Fransisca Arvianty, Janur Malasari, Yusafrina Dewi, Khairunnisa Irwan,
Devi Silitonga, Hernando Manalu, Maulana Sakti
Microencapsulation
Conventional microencapsulation can be described as
surrounding either a liquid droplet or a solid particle
core with a defined, solid shell. It is used to deliver,
protect, stabilize or control the release of the core.
Ingredients that can be encapsulated include adhesives,
drug substances, colors, fragrances, flavors, agricultural
chemicals, solvents and oils.
Especially in the cosmetic industry such capsules are
designed to release the core by fracture of the shell.
Although the earliest application by the cosmetic
industry was probably for “scratch and sniff ” fragrance
samplers, the first commercial use of
microencapsulation was in carbonless paper. Schematic comparing
microcapsules with SLNs
Microencapsulation
Traditional microencapsulation capsules are typically larger than 1 μm in diameter, the
normal range being 50–500 μm.
Capsule size is determined, in part, by limitations of the methods used to produce them
and by the fact that a large size is necessary for the capsule to be ruptured by either
pressure or by shear of use.
As capsule size decreases the capsules become less susceptible to the forces that can cause
rupture of the shell. Such capsules are normally supplied in a dry powder form that,
subsequently, often needs to be incorporated (dispersed) into the cosmetic or
pharmaceutical formulation.
Microencapsulation capsules are produced by:
1. Chemical processes
2. Physical processes
Chemical Production
The chemical methods used are
categorized as coacervation, condensation
or interfacial polymerization and
generally involve dispersing the active
core material in a non-solvent continuous
phase to form an emulsion or dispersion
(the continuous phase must be a non-
solvent for the dispersed phase).
The shell is created by a chemical reaction,
and subsequent precipitation, of one or
more shell-precursor materials that are
dissolved in the continuous or
discontinuous, phase at the interface of
the core material and the continuous
phase.
It is possible to have different components
of the shell dissolved in both phases.
Optical micrograph of gelatin-acacia
microcapsule
prepared by coacervation
SEM of fractured poly(4-vinylpyridine) microcapsule
Physical Production
These methods entail co-extrusion of a solution, melting the shell material
over a droplet, or particle, of the core material, or spray-coating the shell
over a solid particle where fluidized beds are often employed to ensure
uniform coating of cores by shell forming solutions.
The Wurster Process is the classic example, in which particles are fluidized
in an air stream within a vertical chamber and coating material solution is
injected from below into the fluidized particles. Such physical methods
typically produce larger capsules, and are especially suited to particles with
solid cores.
SLN (Solid-Lipid Nanoparticles)
The purpose is encapsulation of ethylhexyl methoxycinnamate (EHMC;
Octinoxate) for dermal sunscreens.
The goal was to encapsulate the organic sunscreen in a benign matrix and
effectively turn them into particulates in order to decrease the irritant/allergic
sensitization potential.
A low pressure proprietary melt-emulsify-chill (MEC) process was used. This
encapsulation method is general and can be applied to many water- or oil-
soluble cosmetic and pharmaceutical actives. The process is cost-effective,
reproducible, robust and scalable. For economic and technical (processing)
reasons, it is very desirable to have a high solids content particle dispersion;
stable, concentrated aqueous dispersions (up to 60% w/w) of SLN’s can be
prepared by the MEC method.
SLN (Solid-Lipid Nanoparticles)
The particle size and distribution is controlled by the rate of initial mixing,
degree of shear and rate of cooling.
These particles are a homogeneous mixture of matrix and active; the active can
be present at concentrations as high as 30% by weight of the total dispersion. The
matrix is typically a wax (or mixture of waxes) but may be an organic polymer or
a silicone.
In principle, the MEC process allows systems to be custom-designed to fit
specific applications.
The SLN is not a wall-and-core particle; the particles are stable to mechanical
agitation as well as storage—unlike many liposomal systems. Release is
accomplished via diffusion or particle breakdown. Diffusion is dependent on
particle/surrounding medium interaction. Breakdown can be accomplished
through exploitation of melting points.
Schematic of the Melt-Emulsify-Chill process
SEM of a typical SLN
Note that the particles are spherical but
polydisperse
Experimental Methods
Solid lipid nanoparticles were prepared by the MEC process.
In essence, a molten wax is dispersed into a hot aqueous emulsifier
solution under controlled shear and then cooled to yield a stable
dispersion of solid-lipid nanoparticles.
No organic solvents are required in this process, and the nanoparticles
are hydrolytically.
The results clearly demonstrate a substantial increase in SPF when using
encapsulated sunscreen active compared with the control products
containing regular sunscreen active at the same levels.
The exact reason for this initially rather unexpected result could arise
from several factors.
Importantly, the molecules of the organic sunscreen are well dispersed
within the microcapsules and the microcapsules themselves form a more
uniform film on the skin (compared with the non-encapsulated material)
thus improving the UV photon collection and absorption efficiency. Path
length and additional scattering of radiation also increase.
Further, the encapsulation may also help to reduce photodegradation.
1. Formulation
Result and Discussion
The results clearly demonstrate a substantial increase in SPF when using
encapsulated sunscreen active compared with the control products
containing regular sunscreen active at the same levels.
The exact reason for this initially rather unexpected result could arise
from several factors.
Importantly, the molecules of the organic sunscreen are well dispersed
within the microcapsules and the microcapsules themselves form a more
uniform film on the skin (compared with the non-encapsulated material)
thus improving the UV photon collection and absorption efficiency. Path
length and additional scattering of radiation also increase.
Further, the encapsulation may also help to reduce photodegradation.
2. Result
The SLN suspensions used in the study all had solid contents of 50% by
weight.
No change occurred in viscosity of a typical suspension after 12 months
storage at room temperature.
3. Stability
Conclusions
The MEC process can easily, and cheaply, produce a range of solid lipid nanoparticles
(SLNs) that offer flexibility in formulation, increased efficacy and decreased
formulation complexity.
The method is general and can be applied to many water- or oil-soluble cosmetic and
pharmaceutical actives. Multiple actives can be co-encapsulated. The process is cost-
effective, reproducible, robust and scalable.
The bulk physical characteristics and surface chemical properties can be varied to
allow systems to be custom designed to fit specific applications; use can be made of
this in the targeting of encapsulated actives, botanicals and therapeutics to skin and
hair.
Fairhurst, D., and Andrew L. 2008. Micro- and Nano-encapsulation of Water- and Oil-
soluble Actives for Cosmetic and Pharmaceutical Applications. Bethlehem, PA,
USA: Particle Sciences Inc.

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Microencapsulation for Cosmetic Application

  • 1. Microencapsulation for Cosmetic Application Kelompok III Fransisca Arvianty, Janur Malasari, Yusafrina Dewi, Khairunnisa Irwan, Devi Silitonga, Hernando Manalu, Maulana Sakti
  • 2. Microencapsulation Conventional microencapsulation can be described as surrounding either a liquid droplet or a solid particle core with a defined, solid shell. It is used to deliver, protect, stabilize or control the release of the core. Ingredients that can be encapsulated include adhesives, drug substances, colors, fragrances, flavors, agricultural chemicals, solvents and oils. Especially in the cosmetic industry such capsules are designed to release the core by fracture of the shell. Although the earliest application by the cosmetic industry was probably for “scratch and sniff ” fragrance samplers, the first commercial use of microencapsulation was in carbonless paper. Schematic comparing microcapsules with SLNs
  • 3. Microencapsulation Traditional microencapsulation capsules are typically larger than 1 μm in diameter, the normal range being 50–500 μm. Capsule size is determined, in part, by limitations of the methods used to produce them and by the fact that a large size is necessary for the capsule to be ruptured by either pressure or by shear of use. As capsule size decreases the capsules become less susceptible to the forces that can cause rupture of the shell. Such capsules are normally supplied in a dry powder form that, subsequently, often needs to be incorporated (dispersed) into the cosmetic or pharmaceutical formulation. Microencapsulation capsules are produced by: 1. Chemical processes 2. Physical processes
  • 4. Chemical Production The chemical methods used are categorized as coacervation, condensation or interfacial polymerization and generally involve dispersing the active core material in a non-solvent continuous phase to form an emulsion or dispersion (the continuous phase must be a non- solvent for the dispersed phase). The shell is created by a chemical reaction, and subsequent precipitation, of one or more shell-precursor materials that are dissolved in the continuous or discontinuous, phase at the interface of the core material and the continuous phase. It is possible to have different components of the shell dissolved in both phases. Optical micrograph of gelatin-acacia microcapsule prepared by coacervation SEM of fractured poly(4-vinylpyridine) microcapsule
  • 5. Physical Production These methods entail co-extrusion of a solution, melting the shell material over a droplet, or particle, of the core material, or spray-coating the shell over a solid particle where fluidized beds are often employed to ensure uniform coating of cores by shell forming solutions. The Wurster Process is the classic example, in which particles are fluidized in an air stream within a vertical chamber and coating material solution is injected from below into the fluidized particles. Such physical methods typically produce larger capsules, and are especially suited to particles with solid cores.
  • 6. SLN (Solid-Lipid Nanoparticles) The purpose is encapsulation of ethylhexyl methoxycinnamate (EHMC; Octinoxate) for dermal sunscreens. The goal was to encapsulate the organic sunscreen in a benign matrix and effectively turn them into particulates in order to decrease the irritant/allergic sensitization potential. A low pressure proprietary melt-emulsify-chill (MEC) process was used. This encapsulation method is general and can be applied to many water- or oil- soluble cosmetic and pharmaceutical actives. The process is cost-effective, reproducible, robust and scalable. For economic and technical (processing) reasons, it is very desirable to have a high solids content particle dispersion; stable, concentrated aqueous dispersions (up to 60% w/w) of SLN’s can be prepared by the MEC method.
  • 7. SLN (Solid-Lipid Nanoparticles) The particle size and distribution is controlled by the rate of initial mixing, degree of shear and rate of cooling. These particles are a homogeneous mixture of matrix and active; the active can be present at concentrations as high as 30% by weight of the total dispersion. The matrix is typically a wax (or mixture of waxes) but may be an organic polymer or a silicone. In principle, the MEC process allows systems to be custom-designed to fit specific applications. The SLN is not a wall-and-core particle; the particles are stable to mechanical agitation as well as storage—unlike many liposomal systems. Release is accomplished via diffusion or particle breakdown. Diffusion is dependent on particle/surrounding medium interaction. Breakdown can be accomplished through exploitation of melting points.
  • 8. Schematic of the Melt-Emulsify-Chill process SEM of a typical SLN Note that the particles are spherical but polydisperse
  • 9. Experimental Methods Solid lipid nanoparticles were prepared by the MEC process. In essence, a molten wax is dispersed into a hot aqueous emulsifier solution under controlled shear and then cooled to yield a stable dispersion of solid-lipid nanoparticles. No organic solvents are required in this process, and the nanoparticles are hydrolytically.
  • 10. The results clearly demonstrate a substantial increase in SPF when using encapsulated sunscreen active compared with the control products containing regular sunscreen active at the same levels. The exact reason for this initially rather unexpected result could arise from several factors. Importantly, the molecules of the organic sunscreen are well dispersed within the microcapsules and the microcapsules themselves form a more uniform film on the skin (compared with the non-encapsulated material) thus improving the UV photon collection and absorption efficiency. Path length and additional scattering of radiation also increase. Further, the encapsulation may also help to reduce photodegradation. 1. Formulation Result and Discussion
  • 11.
  • 12. The results clearly demonstrate a substantial increase in SPF when using encapsulated sunscreen active compared with the control products containing regular sunscreen active at the same levels. The exact reason for this initially rather unexpected result could arise from several factors. Importantly, the molecules of the organic sunscreen are well dispersed within the microcapsules and the microcapsules themselves form a more uniform film on the skin (compared with the non-encapsulated material) thus improving the UV photon collection and absorption efficiency. Path length and additional scattering of radiation also increase. Further, the encapsulation may also help to reduce photodegradation. 2. Result
  • 13.
  • 14. The SLN suspensions used in the study all had solid contents of 50% by weight. No change occurred in viscosity of a typical suspension after 12 months storage at room temperature. 3. Stability
  • 15.
  • 16. Conclusions The MEC process can easily, and cheaply, produce a range of solid lipid nanoparticles (SLNs) that offer flexibility in formulation, increased efficacy and decreased formulation complexity. The method is general and can be applied to many water- or oil-soluble cosmetic and pharmaceutical actives. Multiple actives can be co-encapsulated. The process is cost- effective, reproducible, robust and scalable. The bulk physical characteristics and surface chemical properties can be varied to allow systems to be custom designed to fit specific applications; use can be made of this in the targeting of encapsulated actives, botanicals and therapeutics to skin and hair.
  • 17. Fairhurst, D., and Andrew L. 2008. Micro- and Nano-encapsulation of Water- and Oil- soluble Actives for Cosmetic and Pharmaceutical Applications. Bethlehem, PA, USA: Particle Sciences Inc.