| Literature DB >> 35922421 |
William Whyte1, Debkalpa Goswami1, Sophie X Wang1,2, Yiling Fan3, Niamh A Ward1,4, Ruth E Levey5, Rachel Beatty5, Scott T Robinson5,6, Declan Sheppard7, Raymond O'Connor5, David S Monahan1,5, Lesley Trask4, Keegan L Mendez8, Claudia E Varela8, Markus A Horvath8, Robert Wylie5, Joanne O'Dwyer1,4, Daniel A Domingo-Lopez5, Arielle S Rothman1, Garry P Duffy5,6, Eimear B Dolan9, Ellen T Roche10,11,12.
Abstract
Fibrous capsule (FC) formation, secondary to the foreign body response (FBR), impedes molecular transport and is detrimental to the long-term efficacy of implantable drug delivery devices, especially when tunable, temporal control is necessary. We report the development of an implantable mechanotherapeutic drug delivery platform to mitigate and overcome this host immune response using two distinct, yet synergistic soft robotic strategies. Firstly, daily intermittent actuation (cycling at 1 Hz for 5 minutes every 12 hours) preserves long-term, rapid delivery of a model drug (insulin) over 8 weeks of implantation, by mediating local immunomodulation of the cellular FBR and inducing multiphasic temporal FC changes. Secondly, actuation-mediated rapid release of therapy can enhance mass transport and therapeutic effect with tunable, temporal control. In a step towards clinical translation, we utilise a minimally invasive percutaneous approach to implant a scaled-up device in a human cadaveric model. Our soft actuatable platform has potential clinical utility for a variety of indications where transport is affected by fibrosis, such as the management of type 1 diabetes.Entities:
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Year: 2022 PMID: 35922421 PMCID: PMC9349266 DOI: 10.1038/s41467-022-32147-w
Source DB: PubMed Journal: Nat Commun ISSN: 2041-1723 Impact factor: 17.694