Development of solid lipid
nanoparticles is one of the emerging fields of lipid nanotechnology (for a review on lipid nanotechnology, see ) with several potential applications in drug delivery,
clinical medicine and
research, as well as in other disciplines. Due to their unique size-dependent properties, lipid nanoparticles can possibly develop new therapeutics. The ability to incorporate drugs into nanocarriers offers a new prototype in drug delivery that could hold great promise for attaining
bioavailability enhancement along with controlled and site-specific drug delivery. SLNs are also considered to be well tolerated in general, due to their composition from physiologically similar lipids. The conventional approaches such as use of
permeation enhancers, surface modification, prodrug synthesis, complex formation and colloidal lipid carrier-based strategies have been developed for the delivery of drugs to intestinal lymphatics. In addition, polymeric nanoparticles, self-emulsifying delivery systems,
liposomes,
microemulsions, micellar solutions and recently, solid lipid nanoparticles (SLN) have been exploited as probable possibilities as carriers for oral intestinal lymphatic delivery.
Drug delivery Solid lipid nanoparticles can function as the basis for oral and parenteral
drug delivery systems. SLNs combine the advantages of lipid emulsion and polymeric nanoparticle systems while overcoming the temporal and
in vivo stability issues that troubles the conventional as well as
polymeric nanoparticles drug delivery approaches. or thiol groups for adhesion via disulfide bond formation can be immobilized on their surface. A recent study has demonstrated the use of solid lipid nanoparticles as a platform for oral delivery of the nutrient mineral
iron, by incorporating the hydrophilic molecule
ferrous sulfate (FeSO4) in a lipid matrix composed of
stearic acid.
Carvedilol-loaded solid lipid nanoparticles were prepared using
hot-homogenization technique for oral delivery with
compritol and
poloxamer 188 as the lipid and surfactant, respectively. Many nano-structured systems have been employed for
ocular drug delivery. SLNs have been looked at as a potential drug carrier system since the 1990s. SLNs do not show biotoxicity as they are prepared from physiological lipids. SLNs are useful in ocular drug delivery as they can enhance the
corneal absorption of drugs and improve the ocular bioavailability of both
hydrophilic and
lipophilic drugs. SLNs have another advantage of allowing
autoclave sterilization, a necessary step towards formulation of ocular preparations. Advantages of SLNs include the use of physiological lipids (which decreases the danger of acute and chronic toxicity), the avoidance of organic solvents, a potential wide application spectrum (
dermal,
per os,
intravenous) and the high pressure homogenization as an established production method. Additionally, improved
bioavailability, protection of sensitive drug molecules from the outer environment (e.g. water, light), and even controlled release characteristics were claimed by the incorporation of poorly water-soluble drugs in the solid lipid matrix. Moreover, SLNs can carry both lipophilic and hydrophilic drugs, and are more affordable compared to polymeric/surfactant-based carriers.
Nucleic acids A significant obstacle to using LNPs as a delivery vehicle for
nucleic acids is that in nature, lipids and nucleic acids both carry a negative
electric charge—meaning they do not easily mix with each other. While working at
Syntex in the mid-1980s,
Philip Felgner pioneered the use of artificially-created cationic lipids (positively-charged lipids) to bind lipids to nucleic acids in order to
transfect the latter into cells. However, by the late 1990s, it was known from
in vitro experiments that this use of cationic lipids had undesired side effects on
cell membranes. During the late 1990s and 2000s,
Pieter Cullis, while at the
University of British Columbia, developed ionizable cationic lipids which are "positively charged at an acidic pH but neutral in the blood." As of 2021, the current understanding of LNPs formulated with such ionizable cationic lipids is that they enter cells through
receptor-mediated endocytosis and end up inside
endosomes. In 2018, the FDA approved Alnylam's siRNA drug Onpattro (
patisiran), the first drug to use LNPs as the drug delivery system. Several researchers have shown the enhancement of oral
bioavailibility of poorly water-soluble drugs when encapsulated in solid lipid
nanoparticle. This enhanced
bioavailibility is achieved via
lymphatic delivery. To elucidate the absorption mechanism, from solid lipid
nanoparticle, human excised
Caco-2 cell monolayer could be alternative tissue for development of an in-vitro model to be used as a screening tool before animal studies are undertaken. The results obtained in this model suggested that the main absorption mechanism of carvedilol loaded solid lipid
nanoparticle could be
endocytosis and, more specifically, clathrin-mediated
endocytosis. == See also ==