Piccinino F, Felaco F M, Sagnelli E, Aprea L, Messina V, Pasquale G, Filippini P, Scolastico C
Istituto di Malattie Infettive, II Università di Napoli, Italy.
Res Virol. 1998 Sep-Oct;149(5):283-91. doi: 10.1016/s0923-2516(99)89007-4.
The aims of the study were to evaluate the long-term efficacy and tolerability of different doses of interferon-alpha (IFN alpha) and different durations of treatment in chronic hepatitis C by comparing 3 or 6 mega units (MUs) three times weekly given for either 12 or 24 months, and the possibility of obtaining a response in non-responder patients by increasing the dose or by administering IFN daily. A total of 504 patients with non-cirrhotic chronic hepatitis C enrolled in a multicentre study were consecutively assigned to receive either 3 (255 patients) or 6 MU (249 patients) of lymphoblastoid IFN alpha 3 times a week (tiw). At the 12th month of therapy, patients with normal aminotransferase (AMT) in both groups were either given IFN for an additional 12 months with an unmodified or halved dose, or else discontinued therapy. For patients with unmodified AMT levels after 6 months of therapy, the IFN dose was doubled in the 3-MU group, while it was administered at 3 MU daily in the 6-MU group. When no improvement was achieved, therapy was discontinued; otherwise it was prolonged until the 18th month. Patients were followed up for 12 months after discontinuing IFN. Of the 255 patients enrolled at 3 MU, therapy was stopped during the first 6 months in 36 patients (14.1%) because of side effects, and in 24 (9.4%) because of lack of cooperation. Of the remaining 195 patients at the 6th month of therapy, 119 (61%) had normal and 76 (39%) unmodified AMT levels; 14 of the 76 normalized AMT after doubling the dose of IFN, but only 5 (6.6%) had a sustained response. Of the 119 patients with normal AMT, 40 discontinued IFN at the 12th month (schedule A), 39 remained at 3 MU tiw (schedule B) and 40 were given a dose of 1.5 MU tiw (schedule C) for an additional 12 months. At the end of follow-up, 23/40 (57.5%) patients in schedule A, 31/39 (79.5%) on schedule B and 29/40 (72.5%) on schedule C still had normal AMT (A vs. B p = 0.04). In an intention-to-treat analysis, the sustained response rate for patients enrolled at 3 MUs, including the 5 initial non-responders, was 34.5%. Of the 249 patients enrolled at 6 MU, therapy was discontinued during the first 6 months for 39 (15.7%) because of side effects, and for 27 (10.8%) because of lack of cooperation. Of the remaining 183 patients at the 6th month of therapy, 110 (60%) had normal and 73 (40%) unmodified AMT levels. Of the 73 patients, 55 accepted the daily regimen and 8 of them (14.5%) showed a sustained response. Of the 110 patients with normal AMT, 32 (29.1%), despite normalization of AMT, spontaneously discontinued IFN or reduced the dose because of a poor quality of life, while 78 continued with 6 MU until the 12th month, when therapy was discontinued for 28 (schedule A1); 24 patients were given an unmodified dose (schedule B1) and 26 a halved dose (schedule C1) for an additional 12 months. At the end of follow-up, 18/28 (64.3%) patients on schedule A1, 19/24 (79.2%) on schedule B1 and 19/26 (73.1%) on C1 still had normal AMT (p = NS). In an intention-to-treat evaluation, the sustained response rate for patients enrolled at 6 MU, including the 8 from the daily treatment, was 25.7% (64/249). HCV viraemia was undetectable 1 year after discontinuation of IFN in 72.6% of patients with a sustained response. Sustained response was observed in 36.4% of patients with minimal, 46.6% of those with mild, and 33.3% with moderate or severe histological activity (p = NS). The rate of sustained response was lower in patients with genotype 1b (23.6%) than in those with genotype 2a (67.8%, p = 0.002) or genotype 3 (50%, p = 0.03), irrespective of the histological activity. In conclusion, 6 MU IFN alpha are no more effective than 3 MU in inducing a sustained response in treatments of both 12 and 24 months. A 24-month treatment is more effective than a 12-month treatment in maintaining a biochemical response after discontinuation of IFN. In terms of efficacy, compliance and cost, 3 MU for 24 months app
本研究的目的是通过比较每周三次给予12个月或24个月的3或6百万单位(MU)干扰素-α(IFNα),评估不同剂量的IFNα和不同疗程在慢性丙型肝炎中的长期疗效和耐受性,以及通过增加剂量或每日给予IFN在无反应患者中获得反应的可能性。一项多中心研究纳入了504例非肝硬化慢性丙型肝炎患者,连续分配接受每周三次(tiw)3(255例患者)或6 MU(249例患者)的淋巴母细胞IFNα治疗。在治疗的第12个月,两组中氨基转移酶(AMT)正常的患者,要么给予IFN再治疗12个月,剂量不变或减半,要么停止治疗。对于治疗6个月后AMT水平未改变的患者,3-MU组的IFN剂量加倍,而6-MU组则每日给予3 MU。若未取得改善,则停止治疗;否则延长至第18个月。停止IFN治疗后对患者随访12个月。在纳入3 MU治疗的255例患者中,36例(14.1%)在最初6个月内由于副作用停止治疗,24例(9.4%)由于缺乏合作停止治疗。在治疗第6个月时,其余195例患者中,119例(61%)AMT正常,76例(39%)AMT未改变;76例中14例在IFN剂量加倍后AMT恢复正常,但只有5例(6.6%)获得持续反应。119例AMT正常的患者中,40例在第12个月停止IFN治疗(方案A),39例继续每周三次给予3 MU(方案B),40例给予每周三次1.5 MU的剂量(方案C)再治疗12个月。随访结束时,方案A组40例患者中的23例(57.5%)、方案B组39例中的31例(79.5%)和方案C组40例中的29例(72.5%)AMT仍正常(A组与B组比较,p = 0.04)。在意向性治疗分析中,纳入3 MU治疗的患者,包括最初5例无反应者,持续反应率为34.5%。在纳入6 MU治疗的249例患者中,39例(15.7%)在最初6个月内由于副作用停止治疗,27例(10.8%)由于缺乏合作停止治疗。在治疗第6个月时,其余183例患者中,110例(60%)AMT正常,73例(40%)AMT未改变。73例患者中,55例接受每日治疗方案,其中8例(14.5%)获得持续反应。110例AMT正常的患者中,32例(29.1%)尽管AMT恢复正常,但由于生活质量差自行停止IFN治疗或减少剂量,而78例继续给予6 MU直至第12个月,此时28例停止治疗(方案A1);24例给予未改变的剂量(方案B1),26例给予减半剂量(方案C1)再治疗12个月。随访结束时,方案A1组28例患者中的18例(64.3%)、方案B1组24例中的19例(79.2%)和方案C1组26例中的19例(73.1%)AMT仍正常(p =无显著性差异)。在意向性治疗评估中,纳入6 MU治疗的患者,包括每日治疗的8例,持续反应率为25.7%(64/249)。在获得持续反应的患者中,72.6%在停止IFN治疗1年后HCV病毒血症检测不到。在组织学活动程度为轻微的患者中,36.4%获得持续反应;轻度患者中为46.6%;中度或重度患者中为33.3%(p =无显著性差异)。无论组织学活动程度如何,1b基因型患者的持续反应率(23.6%)低于2a基因型患者(67.8%,p = 0.002)或3基因型患者(50%,p = 0.03)。总之,在12个月和24个月的治疗中,6 MU IFNα在诱导持续反应方面并不比3 MU更有效。24个月的治疗在停止IFN治疗后维持生化反应方面比12个月的治疗更有效。在疗效、依从性和成本方面,24个月给予3 MU……
