| Literature DB >> 27479756 |
Takashi K Kishimoto1, Joseph D Ferrari1, Robert A LaMothe1, Pallavi N Kolte1, Aaron P Griset1, Conlin O'Neil1, Victor Chan1, Erica Browning1, Aditi Chalishazar1, William Kuhlman1, Fen-Ni Fu1, Nelly Viseux1, David H Altreuter1, Lloyd Johnston1, Roberto A Maldonado1.
Abstract
The development of antidrug antibodies (ADAs) is a common cause for the failure of biotherapeutic treatments and adverse hypersensitivity reactions. Here we demonstrate that poly(lactic-co-glycolic acid) (PLGA) nanoparticles carrying rapamycin, but not free rapamycin, are capable of inducing durable immunological tolerance to co-administered proteins that is characterized by the induction of tolerogenic dendritic cells, an increase in regulatory T cells, a reduction in B cell activation and germinal centre formation, and the inhibition of antigen-specific hypersensitivity reactions. Intravenous co-administration of tolerogenic nanoparticles with pegylated uricase inhibited the formation of ADAs in mice and non-human primates and normalized serum uric acid levels in uricase-deficient mice. Similarly, the subcutaneous co-administration of nanoparticles with adalimumab resulted in the durable inhibition of ADAs, leading to normalized pharmacokinetics of the anti-TNFα antibody and protection against arthritis in TNFα transgenic mice. Adjunct therapy with tolerogenic nanoparticles represents a novel and broadly applicable approach to prevent the formation of ADAs against biologic therapies.Entities:
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Year: 2016 PMID: 27479756 DOI: 10.1038/nnano.2016.135
Source DB: PubMed Journal: Nat Nanotechnol ISSN: 1748-3387 Impact factor: 39.213