The effect of a hydrogen sulfide releasing molecule (Na2S) on the cold storage of livers from cardiac dead donor rats. A study in an ex vivo model

Autor: Claudio Tiribelli, Edgardo E. Guibert, Joaquín V. Rodríguez, Cecilia Lucía Balaban
Přispěvatelé: Balaban, Cecilia Lucía, Rodríguez, Joaquín Valentín, Tiribelli, Claudio, Guibert, Edgardo Elvio
Jazyk: angličtina
Rok vydání: 2015
Předmět:
Male
medicine.medical_treatment
Liver transplantation
Isolated perfused rat liver
Potassium Chloride
Liver disease
Ischemia
Malondialdehyde
Mannitol
Warm Ischemia
Hydrogen sulfide
Otras Medicina Básica
General Medicine
Organ Preservation
Gaseous transmitter
Medicina Básica
Real-time polymerase chain reaction
Liver
Proto-Oncogene Proteins c-bcl-2
Anesthesia
Reperfusion Injury
General Agricultural and Biological Sciences
CIENCIAS MÉDICAS Y DE LA SALUD
Donation after cardiac death
Organ Preservation Solutions
Cold storage
Sulfides
General Biochemistry
Genetics and Molecular Biology

Microcirculation
Andrology
medicine
Animals
Organ donation
RNA
Messenger

Rats
Wistar

Cryopreservation
business.industry
Tumor Necrosis Factor-alpha
medicine.disease
Liver Transplantation
Rats
Glucose
Cytoprotection
business
Ex vivo
Heme Oxygenase-1
Procaine
Popis: Liver transplantation is currently the preferred treatment option for end-stage liver disease. Donation after cardiac death was a common practice in the early years of organ donation before brain death criteria were established. Those organs were subjected to variable periods of warm ischemia that might intensify cold ischemia/reperfusion injuries. In the present, shortage of brain dead donors has led to the reassessment of organ donation after cardiac death. Since many cytoprotective roles have been describe for H2S during ischemia/reperfusion on a variety of tissues, we hypothesized that graft exposure to this bioactive gas might improve preservation of non-heart beating donated organs. Therefore, to establish a rat model of donation post-cardiac arrest and using this approach to judge H2S delivery effects on graft hypothermic preservation, were the main objectives of this investigation. Cardiopulmonary arrest was induced in sedated rats by overload of potassium (K+ ). Livers were surgically removed and subsequently stored in HTK Solution (Histidine–tryptophan–ketoglutarate) at 0–4 C. After 24 h of hypothermic preservation, livers were rewarmed in an ex vivo model. Three experimental groups were established as follows: I – Livers procured before cardiac death and cold stored 24 h in HTK (BCD); II – Livers procured after cardiac death (45 min) and cold stored 24 h in HTK (ACD); III – Livers procured after cardiac death (45 min) and cold stored 24 h in HTK + 10 lM Sodium Sulfide (Na2S) (ACD-SS). Data suggest that after 45 min of warm ischemia, viability parameters assessed during reperfusion in the ex vivo model were significantly impaired. Real time PCR revealed that after ex vivo reperfusion there is an increased expression of HO-1 and TNF-a and a modest drop in Bcl-2 mRNA, which could be interpreted as the cellular response to the hypoxic insult sustained during warm ischemia. On the other hand, warm ischemic livers exposed to H2S during cold storage, improved microcirculation, morphology and viability parameters during ex vivo reperfusion and showed significant modulation of HO-1 mRNA expression. In conclusion, HTK supplementation with Na2S arose as a potential treatment to recover non-heart beating harvested organs. Furthermore, an appropriate model of cardiac dead liver donors was successfully developed. Fil: Balaban, Cecilia Lucía. Universidad Nacional de Rosario. Secretaria de Ciencia y Tecnica. Centro Binacional de Investigación en Criobiologia Clinica y Aplicada; Argentina Fil: Rodriguez, Joaquin Valentin. Universidad Nacional de Rosario. Secretaria de Ciencia y Tecnica. Centro Binacional de Investigación en Criobiologia Clinica y Aplicada; Argentina Fil: Tiribelli, Claudio. Centro Studi Fegato; Italia Fil: Guibert, Edgardo Elvio. Universidad Nacional de Rosario. Secretaria de Ciencia y Tecnica. Centro Binacional de Investigación en Criobiologia Clinica y Aplicada; Argentina
Databáze: OpenAIRE