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A clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death

BACKGROUND: Heart transplantation (HTx) from brainstem dead (BSD) donors is the gold-standard therapy for severe/end-stage cardiac disease, but is limited by a global donor heart shortage. Consequently, innovative solutions to increase donor heart availability and utilisation are rapidly expanding....

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Autores principales: See Hoe, Louise E., Wildi, Karin, Obonyo, Nchafatso G., Bartnikowski, Nicole, McDonald, Charles, Sato, Kei, Heinsar, Silver, Engkilde-Pedersen, Sanne, Diab, Sara, Passmore, Margaret R., Wells, Matthew A., Boon, Ai-Ching, Esguerra, Arlanna, Platts, David G., James, Lynnette, Bouquet, Mahe, Hyslop, Kieran, Shuker, Tristan, Ainola, Carmen, Colombo, Sebastiano M., Wilson, Emily S., Millar, Jonathan E., Malfertheiner, Maximillian V., Reid, Janice D., O’Neill, Hollier, Livingstone, Samantha, Abbate, Gabriella, Sato, Noriko, He, Ting, von Bahr, Viktor, Rozencwajg, Sacha, Byrne, Liam, Pimenta, Leticia P., Marshall, Lachlan, Nair, Lawrie, Tung, John-Paul, Chan, Jonathan, Haqqani, Haris, Molenaar, Peter, Li Bassi, Gianluigi, Suen, Jacky Y., McGiffin, David C., Fraser, John F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer International Publishing 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8702587/
https://www.ncbi.nlm.nih.gov/pubmed/34950993
http://dx.doi.org/10.1186/s40635-021-00425-4
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author See Hoe, Louise E.
Wildi, Karin
Obonyo, Nchafatso G.
Bartnikowski, Nicole
McDonald, Charles
Sato, Kei
Heinsar, Silver
Engkilde-Pedersen, Sanne
Diab, Sara
Passmore, Margaret R.
Wells, Matthew A.
Boon, Ai-Ching
Esguerra, Arlanna
Platts, David G.
James, Lynnette
Bouquet, Mahe
Hyslop, Kieran
Shuker, Tristan
Ainola, Carmen
Colombo, Sebastiano M.
Wilson, Emily S.
Millar, Jonathan E.
Malfertheiner, Maximillian V.
Reid, Janice D.
O’Neill, Hollier
Livingstone, Samantha
Abbate, Gabriella
Sato, Noriko
He, Ting
von Bahr, Viktor
Rozencwajg, Sacha
Byrne, Liam
Pimenta, Leticia P.
Marshall, Lachlan
Nair, Lawrie
Tung, John-Paul
Chan, Jonathan
Haqqani, Haris
Molenaar, Peter
Li Bassi, Gianluigi
Suen, Jacky Y.
McGiffin, David C.
Fraser, John F.
author_facet See Hoe, Louise E.
Wildi, Karin
Obonyo, Nchafatso G.
Bartnikowski, Nicole
McDonald, Charles
Sato, Kei
Heinsar, Silver
Engkilde-Pedersen, Sanne
Diab, Sara
Passmore, Margaret R.
Wells, Matthew A.
Boon, Ai-Ching
Esguerra, Arlanna
Platts, David G.
James, Lynnette
Bouquet, Mahe
Hyslop, Kieran
Shuker, Tristan
Ainola, Carmen
Colombo, Sebastiano M.
Wilson, Emily S.
Millar, Jonathan E.
Malfertheiner, Maximillian V.
Reid, Janice D.
O’Neill, Hollier
Livingstone, Samantha
Abbate, Gabriella
Sato, Noriko
He, Ting
von Bahr, Viktor
Rozencwajg, Sacha
Byrne, Liam
Pimenta, Leticia P.
Marshall, Lachlan
Nair, Lawrie
Tung, John-Paul
Chan, Jonathan
Haqqani, Haris
Molenaar, Peter
Li Bassi, Gianluigi
Suen, Jacky Y.
McGiffin, David C.
Fraser, John F.
author_sort See Hoe, Louise E.
collection PubMed
description BACKGROUND: Heart transplantation (HTx) from brainstem dead (BSD) donors is the gold-standard therapy for severe/end-stage cardiac disease, but is limited by a global donor heart shortage. Consequently, innovative solutions to increase donor heart availability and utilisation are rapidly expanding. Clinically relevant preclinical models are essential for evaluating interventions for human translation, yet few exist that accurately mimic all key HTx components, incorporating injuries beginning in the donor, through to the recipient. To enable future assessment of novel perfusion technologies in our research program, we thus aimed to develop a clinically relevant sheep model of HTx following 24 h of donor BSD. METHODS: BSD donors (vs. sham neurological injury, 4/group) were hemodynamically supported and monitored for 24 h, followed by heart preservation with cold static storage. Bicaval orthotopic HTx was performed in matched recipients, who were weaned from cardiopulmonary bypass (CPB), and monitored for 6 h. Donor and recipient blood were assayed for inflammatory and cardiac injury markers, and cardiac function was assessed using echocardiography. Repeated measurements between the two different groups during the study observation period were assessed by mixed ANOVA for repeated measures. RESULTS: Brainstem death caused an immediate catecholaminergic hemodynamic response (mean arterial pressure, p = 0.09), systemic inflammation (IL-6 - p = 0.025, IL-8 - p = 0.002) and cardiac injury (cardiac troponin I, p = 0.048), requiring vasopressor support (vasopressor dependency index, VDI, p = 0.023), with normalisation of biomarkers and physiology over 24 h. All hearts were weaned from CPB and monitored for 6 h post-HTx, except one (sham) recipient that died 2 h post-HTx. Hemodynamic (VDI - p = 0.592, heart rate - p = 0.747) and metabolic (blood lactate, p = 0.546) parameters post-HTx were comparable between groups, despite the observed physiological perturbations that occurred during donor BSD. All p values denote interaction among groups and time in the ANOVA for repeated measures. CONCLUSIONS: We have successfully developed an ovine HTx model following 24 h of donor BSD. After 6 h of critical care management post-HTx, there were no differences between groups, despite evident hemodynamic perturbations, systemic inflammation, and cardiac injury observed during donor BSD. This preclinical model provides a platform for critical assessment of injury development pre- and post-HTx, and novel therapeutic evaluation. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1186/s40635-021-00425-4.
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spelling pubmed-87025872022-01-10 A clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death See Hoe, Louise E. Wildi, Karin Obonyo, Nchafatso G. Bartnikowski, Nicole McDonald, Charles Sato, Kei Heinsar, Silver Engkilde-Pedersen, Sanne Diab, Sara Passmore, Margaret R. Wells, Matthew A. Boon, Ai-Ching Esguerra, Arlanna Platts, David G. James, Lynnette Bouquet, Mahe Hyslop, Kieran Shuker, Tristan Ainola, Carmen Colombo, Sebastiano M. Wilson, Emily S. Millar, Jonathan E. Malfertheiner, Maximillian V. Reid, Janice D. O’Neill, Hollier Livingstone, Samantha Abbate, Gabriella Sato, Noriko He, Ting von Bahr, Viktor Rozencwajg, Sacha Byrne, Liam Pimenta, Leticia P. Marshall, Lachlan Nair, Lawrie Tung, John-Paul Chan, Jonathan Haqqani, Haris Molenaar, Peter Li Bassi, Gianluigi Suen, Jacky Y. McGiffin, David C. Fraser, John F. Intensive Care Med Exp Methodologies BACKGROUND: Heart transplantation (HTx) from brainstem dead (BSD) donors is the gold-standard therapy for severe/end-stage cardiac disease, but is limited by a global donor heart shortage. Consequently, innovative solutions to increase donor heart availability and utilisation are rapidly expanding. Clinically relevant preclinical models are essential for evaluating interventions for human translation, yet few exist that accurately mimic all key HTx components, incorporating injuries beginning in the donor, through to the recipient. To enable future assessment of novel perfusion technologies in our research program, we thus aimed to develop a clinically relevant sheep model of HTx following 24 h of donor BSD. METHODS: BSD donors (vs. sham neurological injury, 4/group) were hemodynamically supported and monitored for 24 h, followed by heart preservation with cold static storage. Bicaval orthotopic HTx was performed in matched recipients, who were weaned from cardiopulmonary bypass (CPB), and monitored for 6 h. Donor and recipient blood were assayed for inflammatory and cardiac injury markers, and cardiac function was assessed using echocardiography. Repeated measurements between the two different groups during the study observation period were assessed by mixed ANOVA for repeated measures. RESULTS: Brainstem death caused an immediate catecholaminergic hemodynamic response (mean arterial pressure, p = 0.09), systemic inflammation (IL-6 - p = 0.025, IL-8 - p = 0.002) and cardiac injury (cardiac troponin I, p = 0.048), requiring vasopressor support (vasopressor dependency index, VDI, p = 0.023), with normalisation of biomarkers and physiology over 24 h. All hearts were weaned from CPB and monitored for 6 h post-HTx, except one (sham) recipient that died 2 h post-HTx. Hemodynamic (VDI - p = 0.592, heart rate - p = 0.747) and metabolic (blood lactate, p = 0.546) parameters post-HTx were comparable between groups, despite the observed physiological perturbations that occurred during donor BSD. All p values denote interaction among groups and time in the ANOVA for repeated measures. CONCLUSIONS: We have successfully developed an ovine HTx model following 24 h of donor BSD. After 6 h of critical care management post-HTx, there were no differences between groups, despite evident hemodynamic perturbations, systemic inflammation, and cardiac injury observed during donor BSD. This preclinical model provides a platform for critical assessment of injury development pre- and post-HTx, and novel therapeutic evaluation. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1186/s40635-021-00425-4. Springer International Publishing 2021-12-24 /pmc/articles/PMC8702587/ /pubmed/34950993 http://dx.doi.org/10.1186/s40635-021-00425-4 Text en © The Author(s) 2021 https://creativecommons.org/licenses/by/4.0/Open AccessThis article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Methodologies
See Hoe, Louise E.
Wildi, Karin
Obonyo, Nchafatso G.
Bartnikowski, Nicole
McDonald, Charles
Sato, Kei
Heinsar, Silver
Engkilde-Pedersen, Sanne
Diab, Sara
Passmore, Margaret R.
Wells, Matthew A.
Boon, Ai-Ching
Esguerra, Arlanna
Platts, David G.
James, Lynnette
Bouquet, Mahe
Hyslop, Kieran
Shuker, Tristan
Ainola, Carmen
Colombo, Sebastiano M.
Wilson, Emily S.
Millar, Jonathan E.
Malfertheiner, Maximillian V.
Reid, Janice D.
O’Neill, Hollier
Livingstone, Samantha
Abbate, Gabriella
Sato, Noriko
He, Ting
von Bahr, Viktor
Rozencwajg, Sacha
Byrne, Liam
Pimenta, Leticia P.
Marshall, Lachlan
Nair, Lawrie
Tung, John-Paul
Chan, Jonathan
Haqqani, Haris
Molenaar, Peter
Li Bassi, Gianluigi
Suen, Jacky Y.
McGiffin, David C.
Fraser, John F.
A clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death
title A clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death
title_full A clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death
title_fullStr A clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death
title_full_unstemmed A clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death
title_short A clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death
title_sort clinically relevant sheep model of orthotopic heart transplantation 24 h after donor brainstem death
topic Methodologies
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8702587/
https://www.ncbi.nlm.nih.gov/pubmed/34950993
http://dx.doi.org/10.1186/s40635-021-00425-4
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