Literature DB >> 29187644

Nanoparticle targeting to the endothelium during normothermic machine perfusion of human kidneys.

Gregory T Tietjen1, Sarah A Hosgood2, Jenna DiRito1, Jiajia Cui1, Deeksha Deep1, Eric Song1, Jan R Kraehling3, Alexandra S Piotrowski-Daspit1, Nancy C Kirkiles-Smith4, Rafia Al-Lamki2, Sathia Thiru5, J Andrew Bradley2, Kourosh Saeb-Parsy2, John R Bradley2, Michael L Nicholson2, W Mark Saltzman1, Jordan S Pober6.   

Abstract

Ex vivo normothermic machine perfusion (NMP) is a new clinical strategy to assess and resuscitate organs likely to be declined for transplantation, thereby increasing the number of viable organs available. Short periods of NMP provide a window of opportunity to deliver therapeutics directly to the organ and, in particular, to the vascular endothelial cells (ECs) that constitute the first point of contact with the recipient's immune system. ECs are the primary targets of both ischemia-reperfusion injury and damage from preformed antidonor antibodies, and reduction of perioperative EC injury could have long-term benefits by reducing the intensity of the host's alloimmune response. Using NMP to administer therapeutics directly to the graft avoids many of the limitations associated with systemic drug delivery. We have previously shown that polymeric nanoparticles (NPs) can serve as depots for long-term drug release, but ensuring robust NP accumulation within a target cell type (graft ECs in this case) remains a fundamental challenge of nanomedicine. We show that surface conjugation of an anti-CD31 antibody enhances targeting of NPs to graft ECs of human kidneys undergoing NMP. Using a two-color quantitative microscopy approach, we demonstrate that targeting can enhance EC accumulation by about 5- to 10-fold or higher in discrete regions of the renal vasculature. In addition, our studies reveal that NPs can also nonspecifically accumulate within obstructed regions of the vasculature that are poorly perfused. These quantitative preclinical human studies demonstrate the therapeutic potential for targeted nanomedicines delivered during ex vivo NMP.
Copyright © 2017 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.

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Year:  2017        PMID: 29187644      PMCID: PMC5931373          DOI: 10.1126/scitranslmed.aam6764

Source DB:  PubMed          Journal:  Sci Transl Med        ISSN: 1946-6234            Impact factor:   17.956


  43 in total

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