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Extracorporeal
liver support: waiting for the deciding vote.
Adham
M.
ASAIO J. 2003
Nov-Dec;49(6):621-32.
Department of General, Digestive Surgery and Liver Transplantation,
Croix
Rousse
Hospital,
Lyon,
France.
Because
acute liver cell failure is associated with an exceedingly high mortality, liver
support has been proposed since the 1950s to improve patient outcome. Early
devices, including hemodialysis, hemofiltration, exchange transfusion,
plasmapheresis, hemoperfusion, plasma and cross-hemodialysis or
cross-circulation, appeared inefficient. Meanwhile, documented results of
extracorporeal liver perfusion (ECLP) suggested its superiority over
conventional treatment. These devices were abandoned with the development of
liver transplantation (LT), which allowed a better outcome and longer survival
rate. In the present day, the fact that patients die while waiting for LT
because of organ shortage led to a renewed interest in liver support as bridge
to LT or regeneration. These devices can be classified according to the presence
or lack of hepatocytes, whereas biologic devices refers
to the presence of cells or other organic and biochemical component. The absence
of individual success of early models led to the development of combined
hepatocyte free devices, or artificial liver, which are based upon the
hemodiabsorption principle (Biologic-DT) or on the "albumin bound toxin
hypothesis" (Molecular Adsorbents Recirculating System) with encouraging
results. Meanwhile, hepatocyte based bioartificial liver devices (BLD) were
conceived for a global "metabolic support." BLD were developed with the use of
human hepatoma cell line (C3A) or primary or cryopreserved porcine hepatocytes.
Preliminary experience gave promising results bridging patients to LT. Based
upon the same principle of global hepatocyte metabolic support, ECLP regained
interest, particularly with the development of transgenic pigs. Several concerns
were raised about these devices. Artificial livers lacked any metabolic
synthetic activity, the use of human liver for ECLP seems hardly acceptable
because of organ shortage, and the accepted use of borderline livers for
transplantation is pending trials for the use of xenogenic livers. For BLD, the
concerns were the low hepatocyte mass, the absence of accessory liver cells, and
the potential risk of seeding tumor cells into patient with the use of human
hepatoma cell line. The use of porcine hepatocytes (BLD or ECLP) raised
physiologic and immunologic concerns and particularly the fear of a possible
transfer of porcine viral material. Although recent studies clearly demonstrate
clinical improvement of patients with the use of recently developed liver
support devices, most of reported prospective, controlled, or randomized trials
had a small number of patients. To give the deciding vote and avoid previous
pitfalls, trials need to be developed with a larger number of patients based
upon statistically significant models with the following characteristics: 1)
comprehensive understanding of the acute liver cell failure mechanisms, 2) world
wide classification of conditions that require liver support, and 3) a clear
definition of treatment success pending patients to LT or recovery without
transplantation. There has not yet been conclusive evidence to support the
benefits of extracorporeal liver support. We are still waiting for
the deciding vote.
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