A Hyperbaric Warm Perfusion System Preserves Tissue Composites Ex vivo and Delays the Onset of Acute Rejection

Author:

Villamaria Carole12,Spencer Jerry13,Lawson Shari1,Wang Lin1,Raj Thomas4,Wolf E.5,Parida Bijaya13,Gorantla Vijay1,Rickard Rory6,Davis Michael13,Fries Charles16

Affiliation:

1. Department of Reconstructive Surgery, U.S. Army Institute of Surgical Research, Fort Sam Houston, Texas, United States

2. Department of Surgery, University of Texas Health Science Center at San Antonio, San Antonio, Texas, United States

3. 59 MDW/Science and Technology, Joint Base San Antonio, Texas

4. Department of Pathology, Brooke Army Medical Center, San Antonio, Texas, United States

5. Hyperbaric Oxygen Organ Preservation Systems, San Antonio, Texas

6. Academic Department of Military Surgery and Trauma, Royal Centre for Defence Medicine, ICT Centre, Birmingham, United Kingdom

Abstract

Background Ischemia–reperfusion injury (IRI) precipitates acute rejection of vascularized composite allografts (VCA). Hyperbaric preservation of tissues ex vivo, between harvest and revascularization, may reduce IRI and mitigate acute rejection of VCA. Methods A porcine heterotopic musculocutaneous gracilis flap model was used. In phase 1, control autografts (n = 5) were infused with University of Wisconsin Solution (UWS) and stored at 4°C for 3 hours. Intervention autografts (n = 5) were placed in a hyperbaric oxygen organ preservation system for 5 hours and infused with hyperoxygenated UWS at 20°C and 3 atm. Grafts were replanted into the animals' necks. In phase 2, similarly treated control (n = 8) and intervention grafts (n = 8) were allotransplanted into the necks of animals separated by a typed and standardized genetic mismatch. No systemic immunosuppression was given. Systemic markers of IRI, and clinical and histopathological assessments of necrosis and rejection were performed. Results Autotransplanted tissue composites preserved in the hyperbaric chamber showed histopathological evidence of less muscle necrosis at 3 hours (p = 0.05). Despite a longer period of ischemia, no evidence was found of a difference in systemic markers of IRI following revascularization in these groups. Allotransplanted tissues supported ex vivo within the hyperbaric perfusion device experienced acute rejection significantly later than corresponding controls. Conclusion Hyperbaric warm perfusion preserves musculocutaneous tissue composites ex vivo for longer than standard cold preservation in this model. This translates into a delay in acute rejection of allotransplanted tissue composites.

Publisher

Georg Thieme Verlag KG

Subject

Surgery

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