Śmierć osobnicza (mózgowa) jako przesłanka dopuszczalności przeszczepu ex mortuo

W artykule przedstawiono problematykę śmierci osobniczej (mózgowej) jako przesłanki dopuszczalności przeszczepu ex mortuo. W pierwszej kolejności zostały opisane podstawowe zagadnienia dotyczące pojęcia transplantacji oraz jej rodzajów występujących w piśmiennictwie medycznym. Dalej poruszono tematykę śmierci i jej rodzajów w kontekście transplantacji, podkreślono również występującą w doktrynie różnicę utożsamiania śmierci klinicznej ze śmiercią pozorną, a także przedstawiono występujący w literaturze sztuczny podział śmierci ze względu na narządy, tj. mózg, płuca i serce. Głównym punktem pracy jest zagadnienie śmierci mózgowej (osobniczej). Wskazano wątpliwości natury prawnej, medycznej i społecznej odnośnie do tej przesłanki. Wskazano na metodykę pracy przy ustaleniu śmierci mózgowej. Zwrócono uwagę na fakt zmiany definicji na gruncie obowiązującej ustawy transplantacyjnej. W dalszej kolejności zostało poruszone zagadnienie śmierci wskutek nieodwracalnego zatrzymania krążenia. W podsumowaniu zebrano w sposób ścisły wątki omawiane przez całą pracę i wspominano o innych przesłankach dopuszczalności przeszczepu ex mortuo.

Sialologia historico-medica, h.e. Salivae humanae consideratio physico-medico-forensis, qua ejus natura & usus insimulque morsus brutorum & hominis, rabies & hydrophobia, demorsorum delicta & defensio, item: signa vitalitatis ex spuma oris in foetu mortuo desumenda et alia huc spectantia quaestionibus medico-forensibus perpenduntur /

Mode of access: Internet.

A brief history of haemotopoietic stem cell Ex vivo expansion

Haematopoiesis is the process by which a hierarchy of mature and progenitor blood cells are formed. These cell populations are all derived from multipotent haematopoietic stem cells (HSC), which reside in the bone marrow ‘niche’ of adult humans. Over the lifetime of a healthy individual, this HSC population replenishes between 1010-1011 blood cells on a daily basis. Dysregulation of this system can lead to a number of haematopoietic diseases, including aplastic anaemias and leukaemias, which result in, or require for disease resolution, bone marrow cell depletion. In 1956, E. Donnall Thomas demonstrated that haematopoiesis could be restored by transplanting bone marrow-derived cells from one man into his identical twin brother, who was suffering from advanced leukaemia. His success drew significant interest in academic research and medicine communities, and 12 years later, the first successful allogeneic transplant was performed. To this day, HSCs remain the most studied and characterised stem cell population. In fact, HSCs are the only stem cell population routinely utilised in the clinic. As such, HSCs function as a model system both for the biological investigation of stem cells, as well as for their clinical application. Herein, we briefly review HSC transplantation, strategies for the ex vivo cultivation of HSCs, recent clinical outcomes, and their impact on the future direction of HSC transplantation therapy.

Técnica in útero vs ex útero para recolección de sangre de cordón umbilical como fuente de células madres

La técnica de recolección es el primer paso para obtener una muestra de sangre de cordón umbilical de óptima calidad. Dicho proceso es esencial en los eventos que conducen al éxito del trasplante de células madre. Aunque no existe consenso internacional sobre el procedimiento de recolección, dos técnicas son las principales: la técnica in utero y la técnica ex utero. La técnica in utero aporta ventajas en cuanto al volumen sanguíneo y conteo celular. El parto por cesárea, si se realiza por razones obstétricas es benéfico para la recolección con técnica in utero. Es necesaria la realización de estudios que permitan mayor nivel de evidencia.

Histologic and functional evaluation of lungs reconditioned by ex vivo lung perfusion

BACKGROUND: Only about 15% of donor lungs are considered suitable for transplantation (LTx). Ex vivo lung perfusion (EVLP) has been developed as a method to reassess and repair damaged lungs. We report our experience with EVLP in non-acceptable donor lungs and evaluate its ability to recondition these lungs. METHODS: We studied lungs from 16 brain-dead donors rejected for LTx. After harvesting, the lungs were stored at 4 degrees C for 10 hours and subjected to normothermic EVLP with Steen Solution (Vitro life, Goteborg, Sweden) for 60 minutes. For functional evaluation, the following variables were assessed: partial pressure of arterial oxygen (Pao(2)), pulmonary vascular resistance (PVR), and lung compliance (LC). For histologic assessment, lung biopsy was done before harvest and after EVLP. Tissue samples were examined under light microscopy. To detect and quantify apoptosis, terminal deoxynucleotide transferase-mediated deoxy uridine triphosphate nick-end labeling assay was used. RESULTS: Thirteen lima donors were refused for having impaired lung function. The mean Pao(2) obtained in the organ donor at the referring hospital was 193.7 mm Hg and rose to 489 mm Hg after EVLP. During EVLP, the mean PVR was 652.5 dynes/sec/cm(5) and the mean LC was 48 ml/cm H2O. There was no significant difference between the mean Lung Injury Score before harvest and after EVLP. There was a trend toward a reduction in the median number of apoptotic cells after EVLP. CONCLUSIONS: EVLP improved lung function (oxygenation capacity) of organs considered unsuitable for transplantation. Lung tissue structure did not deteriorate even after 1 hour of normothermic perfusion. J Heart Lung Transplant 2012;31:305-9 (C) 2012 International Society for Heart and Lung Transplantation. All rights reserved.

Paediatric population pharmacokinetics of itraconazole and its active metabolite hydroxy-itraconazole in cystic fibrosis and bone marrow transplant patients

Objectives: The aim of the study was to characterise the population pharmacokinetics (popPK) properties of itraconazole (ITRA) and its active metabolite hydroxy-ITRA in a representative paediatric population of cystic fibrosis (CF) and bone marrow transplant (BMT) patients. The goals were to determine the relative bioavailability between the two oral formulations, and to explore improved dosage regimens in these patients. Methods: All paediatric patients with CF taking oral ITRA for the treatment of allergic bronchopulmonary aspergillosis and patients undergoing BMT who were taking ITRA for prophylaxis of any fungal infection were eligible for the study. A minimum of two blood samples were drawn after the capsules and also after switching to oral solution, or vice versa. ITRA and hydroxy-ITRA plasma concentrations were measured by HPLC[1]. A nonlinear mixed-effect modelling approach (NONMEM 5.1.1) was used to describe the PK of ITRA and hydroxy-ITRA simultaneously. Simulations were used to assess dosing strategies in these patients. Results: Forty-nine patients (29CF, 20 BMT) were recruited to the study who provided 227 blood samples for the population analysis. A 1-compartment model with 1st order absorption and elimination best described ITRA kinetics, with 1st order conversion to hydroxy-ITRA. For ITRA, the apparent clearance (ClItra/F) and volume of distribution (Vitra/F) was 35.5L/h and 672L, respectively; the absorption rate constant for the capsule formulation was 0.0901 h-1 and for the oral solution formulation it was 0.959 h-1. The capsule comparative bioavailability (vs. solution) was 0.55. For hydroxy-ITRA, the apparent volume of distribution and clearance were 10.6 L and 5.28 L/h, respectively. Of several screened covariates only allometrically scaled total body weight significantly improved the fit to the data. No difference between the two populations was found. Conclusion: The developed popPK model adequately described the pharmacokinetics of ITRA and hydroxy-ITRA in paediatric patients with CF and patients undergoing BMT. High inter-patient variability confirmed previous data in CF[2], leukaemia and BMT[3] patients. From the population model, simulations showed the standard dose (5 mg/kg/day) needs to be doubled for the solution formulation and even 4 times more given of the capsules to achieve an adequate target therapeutic trough plasma concentration of 0.5 mg/L[4] in these patients.