Thermogels have the ability to dissolve in cold water and form solid, gel structures when heated to body temperature. This allows them to deliver delicate molecules, like antibodies, which typically break down under normal processing conditions to form microparticles. Researchers at the Polish Academy of Sciences used PLGA-PEG-PLGA (AK012, AK024, AK088, AK091) and PLCL-PEG-PLCL (AK108) from PolySciTech Division of Akina, Inc. (www.polyscitech.com) to create a gel to deliver antibodies. This research holds promise to provide for improved biotherapy techniques in the future. Read more: Lipowska-Kur, Daria, Łukasz Otulakowski, Urszula Szeluga, Katarzyna Jelonek, and Alicja Utrata-Wesołek. "Diverse Strategies to Develop Poly (ethylene glycol)-Polyester Thermogels for Modulating the Release of Antibodies." Materials 17, no. 18 (2024): 4472. www.mdpi.com/1...
“Abstract: In this work, we present basic research on developing thermogel carriers containing high amounts of model antibody immunoglobulin G (IgG) with potential use as injectable molecules. The quantities of IgG loaded into the gel were varied to evaluate the possibility of tuning the dose release. The gel materials were based on blends of thermoresponsive and degradable ABA-type block copolymers composed of poly(lactide-co-glycolide)-b-poly(ethylene glycol)-b-poly(lactide-co-glycolide) (PLGA-PEG-PLGA) or poly(lactide-co-caprolactone)-b-poly(ethylene glycol)-b-(lactide-co-caprolactone) (PLCL-PEG-PLCL). Primarily, the gels with various amounts of IgG were obtained via thermogelation, where the only factor inducing gel formation was the change in temperature. Next, to control the gels’ mechanical properties, degradation rate, and the extent of antibody release, we have tested two approaches. The first one involved the synergistic physical and chemical crosslinking of the copolymers. To achieve this, the hydroxyl groups located at the ends of the PLGA-PEG-PLGA chain were modified into acrylate groups. In this case, the thermogelation was accompanied by chemical crosslinking through the Michael addition reaction. Such an approach increased the dynamic mechanical properties of the gels and simultaneously prolonged their decomposition time. An alternative solution was to suspend crosslinked PEG-polyester nanoparticles loaded with IgG in a PLGA-PEG-PLGA gelling copolymer. We observed that loading IgG into thermogels lowered the gelation temperature (TGEL) value and increased the storage modulus of the gels, as compared with gels without IgG. The prepared gel materials were able to release the IgG from 8 up to 80 days, depending on the gel formulation and on the amount of loaded IgG. The results revealed that additional, chemical crosslinking of the thermogels and also suspension of particles in the polymer matrix substantially extended the duration of IgG release. With proper matching of the gel composition, environmental conditions, and the type and amount of active substances, antibody-containing thermogels can serve as effective IgG delivery materials. Keywords: thermogels; sol-gel transition; tandem gelation; polymer degradation; nanoparticles; antibody”
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29 сен 2024
