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Long-term implant fibrosis prevention in rodents and non-human primates using crystallized drug formulations.

Citation
Farah, S., et al. “Long-Term Implant Fibrosis Prevention In Rodents And Non-Human Primates Using Crystallized Drug Formulations.”. Nature Materials, pp. 892-904.
Center Joslin Diabetes Center
Author Shady Farah, Joshua C Doloff, Peter Müller, Atieh Sadraei, Hye Jung Han, Katy Olafson, Keval Vyas, Hok Hei Tam, Jennifer Hollister-Lock, Piotr S Kowalski, Marissa Griffin, Ashley Meng, Malia McAvoy, Adam C Graham, James McGarrigle, Jose Oberholzer, Gordon C Weir, Dale L Greiner, Robert Langer, Daniel G Anderson
Abstract

Implantable medical devices have revolutionized modern medicine. However, immune-mediated foreign body response (FBR) to the materials of these devices can limit their function or even induce failure. Here we describe long-term controlled-release formulations for local anti-inflammatory release through the development of compact, solvent-free crystals. The compact lattice structure of these crystals allows for very slow, surface dissolution and high drug density. These formulations suppress FBR in both rodents and non-human primates for at least 1.3 years and 6 months, respectively. Formulations inhibited fibrosis across multiple implant sites-subcutaneous, intraperitoneal and intramuscular. In particular, incorporation of GW2580, a colony stimulating factor 1 receptor inhibitor, into a range of devices, including human islet microencapsulation systems, electrode-based continuous glucose-sensing monitors and muscle-stimulating devices, inhibits fibrosis, thereby allowing for extended function. We believe that local, long-term controlled release with the crystal formulations described here enhances and extends function in a range of medical devices and provides a generalized solution to the local immune response to implanted biomaterials.

Year of Publication
2019
Journal
Nature materials
Volume
18
Issue
8
Number of Pages
892-904
Date Published
12/2019
ISSN Number
1476-1122
DOI
10.1038/s41563-019-0377-5
Alternate Journal
Nat Mater
PMID
31235902
PMCID
PMC7184801
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