Immunoregulatory cytokines in chronic hepatitis C virus infection: Pre- and posttreatment with interferon alfa

被引：182

作者：

Cacciarelli, TV

Martinez, OM

Gish, RG

Villanueva, JC

Krams, SM

机构：

[1] CALIF PACIFIC MED CTR,DEPT TRANSPLANTAT,SAN FRANCISCO,CA

[2] CALIF PACIFIC MED CTR,TRANSPLANTAT IMMUNOBIOL LAB,SAN FRANCISCO,CA

来源：

HEPATOLOGY | 1996年 / 24卷 / 01期

关键词：

D O I：

10.1002/hep.510240102

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

T lymphocytes and immunoregulatory cytokines may be important in the host response to hepatitis C virus (HCV) infection. T-helper type 1 (Th1) cytokines (interleukin [IL]-2, interferon gamma [IFN-gamma]) are required for host antiviral immune responses, including cytotoxic T-cell generation and natural killer cell activation, while T-helper type 2 (Th2) cytokines (IL-4, IL-10) can inhibit the development of these effector mechanisms. in this study, the serum levels of Th1 and Th2 cytokines in patients (n = 23) infected with HCV were measured and compared with biochemical (alanine transaminase [ALT]) and viral (HCV RNA) indicators of infection. Serial cytokine levels were measured in a subset of 11 patients at 1 and 12 weeks during and at 1 week after interferon alfa (IFN-alpha) therapy (n = 33 samples). Levels of circulating IL-2, IL-4, IL-10, and IFN-gamma were significantly elevated in HCV patients versus normal controls (128 vs. 25 pg/mL, 3,045 vs. 29 pg/mL, 2,949 vs. 18 pg/mL, and 307 vs. 24 pg/mL, respectively; P < .01). Treatment with IFN-alpha decreased the levels of IL-4 (321 +/- 224 pg/mL) and IL-10 (1,011 +/- 344 pg/mL), which paralleled a decrease in HCV RNA (114 +/- 27 vs. 25 +/- 20 Eq/mL x 10(5), pre- vs. post-IFN-alpha [12 weeks]; P < .05). These findings indicate that an activated T cell response, as manifest by increased circulating immunoregulatory cytokines, is present in patients with HCV liver disease. Furthermore, treatment with IFN-alpha diminishes the Th2 cytokine response. Thus, modulation of T-cell function and cytokine production may be one mechanism whereby IFN-alpha therapy results in reduced viral burden.

引用

页码：6 / 9

页数：4

共 31 条

[11] INTERFERON IN VIRAL-HEPATITIS - ROLE IN PATHOGENESIS AND TREATMENT
DAVIS, GL
HOOFNAGLE, JH
[J]. HEPATOLOGY, 1986, 6 (05) : 1038 - 1041
[12] RECOMBINANT INTERFERON-ALFA THERAPY FOR CHRONIC HEPATITIS-C - A RANDOMIZED, DOUBLE-BLIND, PLACEBO-CONTROLLED TRIAL
DIBISCEGLIE, AM
MARTIN, P
KASSIANIDES, C
LISKERMELMAN, M
MURRAY, L
WAGGONER, J
GOODMAN, Z
BANKS, SM
HOOFNAGLE, JH
[J]. NEW ENGLAND JOURNAL OF MEDICINE, 1989, 321 (22) : 1506 - 1510
[13] FIORENTINO DF, 1991, J IMMUNOL, V146, P3444
[14] QUANTITATIVE-ANALYSIS OF HEPATITIS-C VIRUS-RNA IN SERUM DURING INTERFERON ALFA THERAPY
HAGIWARA, H
HAYASHI, N
MITA, E
TAKEHARA, T
KASAHARA, A
FUSAMOTO, H
KAMADA, T
[J]. GASTROENTEROLOGY, 1993, 104 (03) : 877 - 883
[15] EVIDENCE FOR A DEFICIENCY OF INTERFERON-PRODUCTION IN PATIENTS WITH CHRONIC HEPATITIS-B VIRUS-INFECTION ACQUIRED IN ADULT LIFE
IKEDA, T
LEVER, AML
THOMAS, HC
[J]. HEPATOLOGY, 1986, 6 (05) : 962 - 965
[16] KAKUMU S, 1989, HEPATO-GASTROENTEROL, V36, P97
[17] ABILITY OF PROLONGED INTERFERON TREATMENT TO SUPPRESS RELAPSE AFTER CESSATION OF THERAPY IN PATIENTS WITH CHRONIC HEPATITIS-C - A MULTICENTER RANDOMIZED CONTROLLED TRIAL
KASAHARA, A
HAYASHI, N
HIRAMATSU, N
OSHITA, M
HAGIWARA, H
KATAYAMA, K
KATO, M
MASUZAWA, M
YOSHIHARA, H
KISHIDA, Y
SHIMIZU, Y
INOUE, A
FUSAMOTO, H
KAMADA, T
[J]. HEPATOLOGY, 1995, 21 (02) : 291 - 297
[18] KERN DE, 1981, J IMMUNOL, V127, P1323
[19] SIGNIFICANCE OF SERUM HEPATITIS-C VIRUS-RNA LEVELS IN CHRONIC HEPATITIS-C
LAU, JYN
DAVIS, GL
KNIFFEN, J
QIAN, KP
URDEA, MS
CHAN, CS
MIZOKAMI, M
NEUWALD, PD
WILBER, JC
[J]. LANCET, 1993, 341 (8859) : 1501 - 1504
[20] MALEFYT RD, 1991, J EXP MED, V174, P915

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