学术探索
学术期刊
新闻热点
数据分析
智能评审

Use of hepatic lidocaine metabolism to monitor patients with chronic liver disease

被引:22
作者
Shiffman, ML
Luketic, VA
Sanyal, AJ
Thompson, EB
机构
来源
THERAPEUTIC DRUG MONITORING | 1996年 / 18卷 / 04期
关键词
hepatitis; cirrhosis; lidocaine; monoethylglycinexylodide;
D O I
10.1097/00007691-199608000-00010
中图分类号
R446 [实验室诊断]; R-33 [实验医学、医学实验];
学科分类号
1001 ;
摘要
Lidocaine is converted to its primary metabolic product monoethylglycinexylodide (MEGX) via cytochrome P-4503A4 within the liver. A steady-state concentration of MEGX appears in serum within 15 min following the intravenous administration of lidocaine. The present article reviews some of the data suggesting that this MEGX value can be utilized to assess hepatic function. MEGX production declines stepwise with the severity of chronic hepatitis. In patients with cirrhosis, MEGX declines further with worsening Child class. Nearly all persons with MEGX of <20 ng/ml had cirrhosis confirmed upon histologic evaluation. Severe life-threatening complications of cirrhosis were observed only in patients with MEGX production below 20 ng/ml. One-year survival for patients with an MEGX value of <10 ng/ml was only 50%. In contrast, 1-year survival for patients with MEGX of >10 ng/ml was similar to 80%. These data suggest that MEGX could be utilized as an accurate test of hepatic function and to predict morbidity and mortality related to complications of chronic liver disease. However, this test does have several limitations. There is wide interpatient variability between MEGX and hepatic histology, which severely impairs the ability of this test to accurately predict hepatic histology. In addition, MEGX is affected by gender and several medications. However, since MEGX does decline stepwise with advancing histology in any given patient, the available data suggest that serial monitoring of MEGX could be utilized to track hepatic metabolic capacity in patients with chronic hepatitis and cirrhosis.
引用
收藏
页码:372 / 377
页数:6
相关论文
共 19 条
  • [11] OELLERICH M, 1987, J CLIN CHEM CLIN BIO, V25, P845
  • [12] A RANDOMIZED, CONTROLLED TRIAL OF INTERFERON ALFA-2B ALONE AND AFTER PREDNISONE WITHDRAWAL FOR THE TREATMENT OF CHRONIC HEPATITIS-B
    PERRILLO, RP
    SCHIFF, ER
    DAVIS, GL
    BODENHEIMER, HC
    LINDSAY, K
    PAYNE, J
    DIENSTAG, JL
    OBRIEN, C
    TAMBURRO, C
    JACOBSON, IM
    SAMPLINER, R
    FEIT, D
    LEFKOWITCH, J
    KUHNS, M
    MESCHIEVITZ, C
    SANGHVI, B
    ALBRECHT, J
    GIBAS, A
    [J]. NEW ENGLAND JOURNAL OF MEDICINE, 1990, 323 (05) : 295 - 301
  • [13] MONOETHYLGLYCINEXYLIDE FORMATION IN ASSESSING PEDIATRIC DONOR LIVER-FUNCTION
    ROSSI, SJ
    SCHROEDER, TJ
    VINE, WH
    AKADER, HH
    GREMSE, DA
    RYCKMAN, FC
    PEDERSEN, SH
    PESCE, AJ
    BALISTRERI, WF
    [J]. THERAPEUTIC DRUG MONITORING, 1992, 14 (06) : 452 - 456
  • [14] SCHROEDER TJ, 1989, TRANSPLANT P, V21, P2299
  • [15] HEPATIC LIDOCAINE METABOLISM AND COMPLICATIONS OF CIRRHOSIS - IMPLICATIONS FOR ASSESSING PATIENT PRIORITY FOR HEPATIC TRANSPLANTATION
    SHIFFMAN, ML
    FISHER, RA
    SANYAL, AJ
    EDINBORO, LE
    LUKETIC, VA
    PURDUM, PP
    RAYMOND, P
    POSNER, MP
    RYCKMAN
    POLLAK
    [J]. TRANSPLANTATION, 1993, 55 (04) : 830 - 834
  • [16] SHIFFMAN ML, 1994, HEPATOLOGY, V19, P933, DOI 10.1016/0270-9139(94)90294-1
  • [17] TALIANI G, 1995, HEPATOLOGY, V21, P1760, DOI 10.1002/hep.1840210646
  • [18] ERYTHROMYCIN BREATH TEST AS AN ASSAY OF GLUCOCORTICOID-INDUCIBLE LIVER CYTOCHROMES P-450 - STUDIES IN RATS AND PATIENTS
    WATKINS, PB
    MURRAY, SA
    WINKELMAN, LG
    HEUMAN, DM
    WRIGHTON, SA
    GUZELIAN, PS
    [J]. JOURNAL OF CLINICAL INVESTIGATION, 1989, 83 (02) : 688 - 697
  • [19] MULTIPLE BOLUS TECHNIQUE FOR LIDOCAINE ADMINISTRATION DURING 1ST HOURS OF AN ACUTE MYOCARDIAL-INFARCTION
    WYMAN, MG
    LALKA, D
    HAMMERSMITH, L
    CANNOM, DS
    GOLDREYER, BN
    [J]. AMERICAN JOURNAL OF CARDIOLOGY, 1978, 41 (02) : 313 - 317
12