Identification of pharmacological inducers of a reversible hypometabolic state for whole organ preservation
Author:
Sperry Megan M12ORCID, Charrez Berenice1ORCID, Fotowat Haleh1, Gardner Erica1, Pilobello Kanoelani1, Izadifar Zohreh1, Lin Tiffany1ORCID, Kuelker Abigail1, Kaki Sahith1, Lewandowski Michael1, Lightbown Shanda1, Martinez Ramses1, Marquez Susan1, Moore Joel1, Plaza-Oliver Maria13, Sesay Adama M1ORCID, Shcherbina Kostyantyn1, Sheehan Katherine1, Takeda Takako1, Del Campo Daniela1, Andrijauskaite Kristina4ORCID, Cisneros Exal4, Lopez Riley4, Cano Isabella4, Maxwell Zachary4, Jessop Israel4, Veraza Rafael J4ORCID, Bunegin Leon4ORCID, Percival Thomas J5, Yracheta Jaclyn5, Pena Jorge5, Wood Diandra5, Homas Zachary5, Hinshaw Cody5, Cox-Hinshaw Jennifer5, Parry Olivia G5, Sleeter Justin J5, Weitzel Erik K5ORCID, Levin Michael126ORCID, Super Michael1ORCID, Novak Richard1ORCID, Ingber Donald E178ORCID
Affiliation:
1. Wyss Institute for Biologically Inspired Engineering at Harvard University 2. Department of Biology, Tufts University, 3. DEVANA group, Faculty of Pharmacy, University of Castilla-La Mancha 4. Vascular Perfusion Solutions, Inc 5. RESTOR™, 59th Medical Wing, JBSA 6. Allen Center, Tufts University 7. Vascular Biology Program & Department of Surgery, Boston Children’s Hospital and Harvard Medical School 8. Harvard John A. Paulson School of Engineering and Applied Sciences
Abstract
Drugs that induce reversible slowing of metabolic and physiological processes would have great value for organ preservation, especially for organs with high susceptibility to hypoxia-reperfusion injury, such as the heart. Using whole-organism screening of metabolism, mobility, and development in
Xenopus
, we identified an existing drug, SNC80, that rapidly and reversibly slows biochemical and metabolic activities while preserving cell and tissue viability. Although SNC80 was developed as a delta opioid receptor activator, we discovered that its ability to slow metabolism is independent of its opioid modulating activity as a novel SNC80 analog (WB3) with almost 1,000 times less delta opioid receptor binding activity is equally active. Metabolic suppression was also achieved using SNC80 in microfluidic human organs-on-chips, as well as in explanted whole porcine hearts and limbs, demonstrating the cross-species relevance of this approach and potential clinical relevance for surgical transplantation. Pharmacological induction of physiological slowing in combination with organ perfusion transport systems may offer a new therapeutic approach for tissue and organ preservation for transplantation, trauma management, and enhancing patient survival in remote and low-resource locations.
Publisher
eLife Sciences Publications, Ltd
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