HJ Schlitt scite author profile

Liver transplantation represents a successful and well-established therapeutic concept for patients with advanced liver diseases. Organ donor shortage continues to pose a significant problem. To ensure fair and transparent allocation of too few post-mortem grafts, the model of end-stage liver disease (MELD)-based allocation was implemented in December 2006. This has decreased waiting list mortality from 20 to 10 % but at the same time has reduced post OLT survival (1-year survival from almost 90% to below 80%), which is largely due to patients with a labMELD score > 30. Following MELD introduction the regular allocation threshold has increased from a matchMELD of initially 25 to meanwhile 34. At the same time the quality of donor organs has seen a continuous deterioration over the last 10 - 15 years: 63% of organs are "suboptimal" with a donor risk index of > 1.5. Moreover, the numbers of living-related liver transplantations have decreased. In Germany incentives for transplant centres are inappropriate: patients with decompensated cirrhosis, high MELD scores and high post-transplant mortality as well as marginal liver grafts are accepted for transplantation without the necessary consideration of outcomes, and against a background of the still absent publication and transparency of outcome results. The outlined development calls for measures for improvement: (i) the increase of donor grafts (e. g., living donation, opt-out solutions, non-heart beating donors), (ii) the elimination of inappropriate incentives for transplant centres, (iii) changes of allocation guidelines, that take the current situation and suboptimal donor grafts into account, and (iv) the systematic and complete collection of transplant-related data in order to allow for the development of improved prognostic scores.

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Recurrent Immunoglobulin A Nephropathy After Renal Transplantation

Ohmacht¹,

Kliem²,

Burg³

et al. 1997

Transplantation

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Expression of augmenter of liver regeneration (ALR) in human liver cirrhosis and carcinoma

Thasler

Schlott²,

Thelen

et al. 2005

Histopathology

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Development, Stability, and Clinical Correlations of Allogeneic Microchimerism After Solid Organ Transplantation1

Hisanaga¹,

Hundrieser²,

Böker

et al. 1996

Transplantation

109

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To assess the development, stability, and clinical relevance of donor-type microchimerism, skin and blood were analyzed in heart (n = 53) and liver (n = 18) transplant recipients by nested polymerase chain reaction. Microchimerism was detectable in 40 (75%) and 13 (72%) patients after heart and liver transplantation, respectively. In heart transplantation, chimerism-positive patients showed a lower frequency of acute rejection as compared with negative patients, although this was only of borderline statistical significance. Repeated intraindividual analyses demonstrated variable patterns of microchimerism over time, but changes did not correlate to the clinical state. In liver transplantation, chimeric state showed no clear correlation with the patients' immunological situation. Our results demonstrate that peripheral microchimerism frequently develops after different types of organ transplantation and represents a dynamic process but without diagnostic value to predict the immunological risk for individual patients.

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HJ Schlitt

Aktuelle Entwicklungen der Lebertransplantation in Deutschland: MELD-basierte Organallokation und „incentives” für Transplantationszentren

Recurrent Immunoglobulin A Nephropathy After Renal Transplantation

Expression of augmenter of liver regeneration (ALR) in human liver cirrhosis and carcinoma

Development, Stability, and Clinical Correlations of Allogeneic Microchimerism After Solid Organ Transplantation1

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