Role of circulating neurotoxins in the pathogenesis of hepatic encephalopathy: potential for improvement following their removal by liver assist devices

被引：36

作者：

Butterworth, RF ^{[1
]}

机构：

[1] Univ Montreal, CHUM, Hop St Luc, Neurosci Res Unit, Montreal, PQ H2X 3J4, Canada

来源：

LIVER INTERNATIONAL | 2003年 / 23卷

关键词：

ammonia; manganese; hepatic encephalopathy; benzodiazepines; acute liver failure; aromatic amino acids; glutamine; neuropathology;

D O I：

10.1034/j.1478-3231.23.s.3.1.x

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

Both acute and chronic liver failure result in impaired cerebral function known as hepatic encephalopathy (HE). Evidence suggests that HE is the consequence of the accumulation in brain of neurotoxic and/or neuroactive substance including ammonia, manganese, aromatic amino acids, mercaptans, phenols, short-chain fatty acids, bilirubin and a variety of neuroactive medications prescribed as sedatives to patients with liver failure. Brain ammonia concentrations may attain levels in excess of 2 mM, concentrations which are known to adversely affect both excitatory and inhibitory neurotransmission as well as brain energy metabolism. Manganese exerts toxic effects on dopaminergic neurones. Prevention and treatment of HE continues to rely heavily on the reduction of circulation ammonia either by reduction of gut production using lactulose or antibiotics or by increasing its metabolism using L-ornithine-L-aspartate. No specific therapies have so far been designed to reduce circulation concentrations of other toxins. Liver assist devices offer a potential new approach to the reduction of circulating neurotoxins generated in liver failure. In this regard, the Molecular Absorbents Recirculating System (MARS) appears to offer distinct advantages over hepatocyte-based systems.

引用

页码：5 / 9

页数：5

共 32 条

[1] BASILE AS, 1991, PHARMACOL REV, V43, P27
[2] AROMATIC AND BRANCHED-CHAIN AMINO-ACIDS IN AUTOPSIED BRAIN-TISSUE FROM CIRRHOTIC-PATIENTS WITH HEPATIC-ENCEPHALOPATHY
BERGERON, M
LAYRARGUES, GP
BUTTERWORTH, RF
[J]. METABOLIC BRAIN DISEASE, 1989, 4 (03) : 169 - 176
[3] EFFECT OF AMMONIA ON BRAIN-SEROTONIN METABOLISM IN RELATION TO FUNCTION IN THE PORTACAVAL SHUNTED RAT
BERGERON, M
SWAIN, MS
READER, TA
GRONDIN, L
BUTTERWORTH, RF
[J]. JOURNAL OF NEUROCHEMISTRY, 1990, 55 (01) : 222 - 229
[4] AMMONIA - KEY FACTOR IN THE PATHOGENESIS OF HEPATIC-ENCEPHALOPATHY
BUTTERWORTH, RF
GIGUERE, JF
MICHAUD, J
LAVOIE, J
LAYRARGUES, GP
[J]. NEUROCHEMICAL PATHOLOGY, 1987, 6 (1-2): : 1 - 12
[5] Molecular Adsorbent Recirculating System: clinical experience in patients with liver failure based on hepatitis B in China
Chen, SB
Zhang, LL
Shi, YF
Yang, XL
Wang, MM
[J]. LIVER, 2002, 22 : 48 - 51
[6] Cerebral herniation in patients with acute liver failure is correlated with arterial ammonia concentration
Clemmesen, JO
Larsen, FS
Kondrup, J
Hansen, BA
Ott, P
[J]. HEPATOLOGY, 1999, 29 (03) : 648 - 653
[7] BIOCHEMISTRY AND PHYSIOLOGY OF BRAIN AMMONIA
COOPER, AJL
PLUM, F
[J]. PHYSIOLOGICAL REVIEWS, 1987, 67 (02) : 440 - 519
[8] REVERSIBLE TOXIC MANIFESTATIONS IN PATIENTS WITH CIRRHOSIS OF THE LIVER GIVEN CATION-EXCHANGE RESINS
GABUZDA, GJ
PHILLIPS, GB
DAVIDSON, CS
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1952, 246 (04) : 124 - 130
[9] BRAIN HISTOLOGY AND BEHAVIOR OF MICE INJECTED WITH UREASE
GIBSON, GE
ZIMBER, A
KROOK, L
RICHARDSON, EP
VISEK, WJ
[J]. JOURNAL OF NEUROPATHOLOGY AND EXPERIMENTAL NEUROLOGY, 1974, 33 (02) : 201 - 211
[10] AMINO-ACID CHANGES IN REGIONS OF THE CNS IN RELATION TO FUNCTION IN EXPERIMENTAL PORTAL-SYSTEMIC ENCEPHALOPATHY
GIGUERE, JF
BUTTERWORTH, RF
[J]. NEUROCHEMICAL RESEARCH, 1984, 9 (09) : 1309 - 1321

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