| Literature DB >> 25542803 |
Lucas L Falke1, Stefan H van Vuuren1, Filis Kazazi-Hyseni2, Farshad Ramazani2, Tri Q Nguyen1, Gert J Veldhuis3, Erik M Maarseveen4, Jurjen Zandstra5, Johan Zuidema6, Luisa F Duque6, Rob Steendam6, Eliane R Popa5, Robbert Jan Kok2, Roel Goldschmeding7.
Abstract
Kidney injury triggers fibrosis, the final common pathway of chronic kidney disease (CKD). The increase of CKD prevalence worldwide urgently calls for new therapies. Available systemic treatment such as rapamycin are associated with serious side effects. To study the potential of local antifibrotic therapy, we administered rapamycin-loaded microspheres under the kidney capsule of ureter-obstructed rats and assessed the local antifibrotic effects and systemic side effects of rapamycin. After 7 days, microsphere depots were easily identifiable under the kidney capsule. Both systemic and local rapamycin treatment reduced intrarenal mTOR activity, myofibroblast accumulation, expression of fibrotic genes, and T-lymphocyte infiltration. Upon local treatment, inhibition of mTOR activity and reduction of myofibroblast accumulation were limited to the immediate vicinity of the subcapsular pocket, while reduction of T-cell infiltration was widespread. In contrast to systemically administered rapamycin, local treatment did not induce off target effects such as weight loss. Thus subcapsular delivery of rapamycin-loaded microspheres successfully inhibited local fibrotic response in UUO with less systemic effects. Therapeutic effect of released rapamycin was most prominent in close vicinity to the implanted microspheres.Entities:
Keywords: Chronic kidney disease; Fibrosis; Microsphere; Rapamycin; Subcapsular delivery; mTOR
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Year: 2014 PMID: 25542803 DOI: 10.1016/j.biomaterials.2014.11.042
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479