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Liver
support by extracorporeal blood purification: a clinical observation.
Stange
J, Mitzner SR, Klammt S, Freytag J, Peszynski P, Loock J, Hickstein H, Korten G,
Schmidt R, Hentschel J, Schulz M, Lohr M, Liebe S, Schareck W, Hopt
UT.
Liver
Transpl 2000; 6(5):603-613.
Abstract:
Liver failure associated with excretory insufficiency and jaundice results in an
endogenous accumulation of toxins involved in the impairment of cardiovascular,
kidney, and cerebral function. Moreover, these toxins have been shown to damage
the liver itself by inducing hepatocellular apoptosis and necrosis, thus
creating a vicious cycle of the disease. We report a retrospective cohort study
of 26 patients with acute or chronic liver failure with intrahepatic cholestasis
(bilirubin level > 20 mg/dL) who underwent a new extracorporeal blood
purification treatment. A synthetic hydrophilic/hydrophobic domain-presenting
semipermeable membrane (pore size < albumin size, 100-nm thick) was used for
extracorporeal blood detoxification using dialysis equipment. The opposite side
was rinsed with ligandin-like proteins as molecular adsorbents that were
regenerated online using a chromatography-like recycling system (molecular
adsorbent recirculating system [MARS]). Bile acid and bilirubin levels,
representing the previously described toxins, were reduced by 16% to 53% and 10%
to 90% of the initial concentration by a single treatment of 6 to 8 hours,
respectively. Toxicity testing of patient plasma onto primary rat hepatocytes by
live/dead fluorescence microscopy showed cell-damaging effects of jaundiced
plasma that were not observed after treatment. Patients with a worsening of
Child-Turcotte-Pugh (CTP) index before the treatments showed a significant
improvement of this index during a period of 2 to 14 single treatments with an
average of 14 days. After withdrawal of MARS treatment, this improvement was
sustained in all long-term survivors. Ten patients represented a clinical status
equivalent to the United Network for Organ Sharing (UNOS) status 2b (group A1),
and all survived. Sixteen patients represented a clinical status equivalent to
UNOS status 2a, and 7 of these patients survived (group A2), whereas 9 patients
(group B) died. We conclude that in acute excretory failure caused by a chronic
liver disease, this treatment provides a therapy option to remove toxins
involved in multiorgan dysfunction secondary to liver failure
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