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Extremely short bioavailability and fast pharmacodynamic effects of pMHC-based nanomedicines

J Control Release. 2021-08; 
Yang Yang, Kristofor K Ellestad, Santiswarup Singha, Muhammad Myn Uddin, Robert Clarke, Debajyoti Mondal, Nahir Garabatos, Patricia Solé, Cesar Fandos, Pau Serra, Pere Santamaria
Products/Services Used Details Operation
Catalog Antibody anti-PEG mAb (Clone AGP4, anti-PEG); and 4) anti-His mAb (Clone 6G2A9, Genscript) Get A Quote

摘要

Nanoparticles (NPs) coated with autoimmune disease-relevant peptide-major histocompatibility complexes (pMHCs) can blunt autoimmune diseases by re-programming cognate effector T-lymphocytes into disease-suppressing regulatory T-cells, followed by massive expansion. Here, a method to quantify the absolute amounts of the active drug product is developed, to understand the relationship between bioavailability and pharmacodynamics. Incubation with plasma results in the formation of a protein corona that stabilizes the directional pMHC coat, shielding it from proteolysis or anti-drug antibody recognition, without any appreciable loss in biological potency. A quantitative method that harnesses these features indicate... More

關鍵詞

Anti-drug antibodies (ADAs), Autoimmune disease, Peptide-major histocompatibility complex (pMHC), Pharmacodynamics (PD), Pharmacokinetics (PK), Protein corona, iron oxide nanoparticles
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