Abstract

Lung transplantation (LTx) is still limited by organ shortage. To expand the donor pool, lung retrieval from non-heart-beating donors (NHBD) was introduced into clinical practice recently. However, primary graft dysfunction with inactivation of endogenous surfactant due to ischemia/reperfusion-injury is a major cause of early mortality. Furthermore, donor-derived human mesenchymal stem cell (hMSC) expansion and fibrotic differentiation in the allograft results in bronchiolitis obliterans syndrome (BOS), a leading cause of post-LTx long-term mortality. Therefore, pretreatment of NHBD with recipient-specific bone-marrow-(BM)-derived hMSC might have the potential to both improve the postischemic allograft function and influence the long-term development of BOS by the numerous paracrine, immunomodulating and tissue-remodeling properties especially on type-II-pneumocytes of hMSC.Asystolic pigs (n = 5/group) were ventilated for 3 h of warm ischemia (groups 2-4). 50x106 mesenchymal-stem-cells (MSC) were administered in the pulmonary artery (group 3) or nebulized endobronchially (group 4) before lung preservation. Following left-lung-transplantation, grafts were reperfused, pulmonary-vascular-resistance (PVR), oxygenation and dynamic-lung-compliance (DLC) were monitored and compared to control-lungs (group 2) and sham-controls (group 1). To prove and localize hMSC in the lung, cryosections were counter-stained. Intra-alveolar edema was determined stereologically. Statistics comprised ANOVA with repeated measurements.Oxygenation (p = 0.001) and PVR (p = 0.009) following endovascular application of hMSC were significantly inferior compared to Sham controls, whereas DLC was significantly higher in endobronchially pretreated lungs (p = 0.045) with overall sham-comparable outcome regarding oxygenation and PVR. Stereology revealed low intrapulmonary edema in all groups (p > 0.05). In cryosections of both unreperfused and reperfused grafts, hMSC were localized in vessels of alveolar septa (endovascular application) and alveolar lumen (endobronchial application), respectively.Preischemic deposition of hMSC in donor lungs is feasible and effective, and endobronchial application is associated with significantly better DLC as compared to sham controls. In contrast, transvascular hMSC delivery results in inferior oxygenation and PVR. In the long term perspective, due to immunomodulatory, paracrine and tissue-remodeling effects on epithelial and endothelial restitution, an endobronchial NHBD allograft-pretreatment with autologous mesenchymal-stem-cells to attenuate limiting bronchiolitis-obliterans-syndrome in the long-term perspective might be promising in clinical lung transplantation. Subsequent work with chronic experiments is initiated to further elucidate this important field.

Highlights

  • Thorsten Wittwer1,2*, Parwis Rahmanian1, Yeong-Hoon Choi1,2, Mohamed Zeriouh1, Samira Karavidic1, Klaus Neef1,2, Astrid Christmann3, Tanja Piatkowski3, Anke Schnapper3, Matthias Ochs3,4, Christian Mühlfeld3,4, Anja Sterner-Kock5, Maria Guschlbauer5, Florian Hofmaier5, Alexandra C Maul5 and Thorsten Wahlers1,2. Following publication of this manuscript [1] it was discovered that several authors were inadvertently omitted from the author list

  • SK assisted in the surgical animal procedures, performed data management and prepared lung procurement for histological analysis

  • Germany 2Center of Molecular Medicine, University of Cologne, Cologne, Germany

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Summary

Introduction

Following publication of this manuscript [1] it was discovered that several authors were inadvertently omitted from the author list. Erratum: Mesenchymal stem cell pretreatment of non-heart-beating-donors in experimental lung transplantation Thorsten Wittwer1,2*, Parwis Rahmanian1, Yeong-Hoon Choi1,2, Mohamed Zeriouh1, Samira Karavidic1, Klaus Neef1,2, Astrid Christmann3, Tanja Piatkowski3, Anke Schnapper3, Matthias Ochs3,4, Christian Mühlfeld3,4, Anja Sterner-Kock5, Maria Guschlbauer5, Florian Hofmaier5, Alexandra C Maul5 and Thorsten Wahlers1,2

Results
Conclusion

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