Almasio P L, Di Marco V, Bonura C, Fuschi P, Camma C, Lo Iacono O, Artini M, Natoli C, Di Stefano R, Levrero M, Craxi A
Dipartimento di Igiene e Microbiologia, Università di Palermo, Italy.
Dig Dis Sci. 1999 May;44(5):1013-9. doi: 10.1023/a:1026625001168.
In chronic hepatitis C the rate of relapse after an end-of-treatment response to interferon may exceed 50%. The usefulness of retreatment of relapsers with interferon in obtaining a complete sustained response and the role of clinical, virological and immunological features in determining long-term efficacy of retreatment are unclear. We aimed to assess the efficacy of interferon retreatment in obtaining a complete sustained response, to evaluate whether increasing the dose may enhance responsiveness, and to identify possible predictors of sustained response. We enrolled 42 patients with biopsy-proven chronic hepatitis C without cirrhosis who had previously responded to a six-month course of Interferon-alpha2b (total dose: group A, 22 patients, 234 MU; group B, 20 patients, 468 MU) and then relapsed. All, except one, were HCV-RNA negative at the end of first cycle of interferon; most (31/42, 74%) were infected by HCV 1b. Subjects were randomly allocated to receive another cycle of interferon either at the original dose (group A1: 234 MU, 11 patients; group B1 468 MU, 10 patient) or twice the original dose (group A2: 468 MU, 11 patients; group B2: 936 MU, 10 patients). At the end of the second cycle of interferon, 24 subjects (57%) had normal ALT and were HCV-RNA negative, and 16 (39%) had normal ALT, but were HCV-RNA positive. A complete sustained response was obtained in eight patients (19%), at a similar rate in all treatment groups. Complete sustained responders were different from the other patients in terms of age (35.9 +/- 10.4 vs 44.1 +/- 8.8, P = 0.027), rate of infection with non-1b HCV (6/8 vs 5/34, P = 0.0005), serum HCV-RNA (74,016 vs 321,428 median copies/ml, P = 0.037) and serum levels of 90K/MAC-2 BP (5.76 +/- 3.01 vs 10.25 +/- 5.16 units/ml, P = 0.02), an N-glycoprotein implicated in cellular defense functions. Multivariate logistic analysis validated age and HCV genotype as independent predictors of CSR. Among noncirrhotic relapsers who received a total interferon dose > or = 234 MU in the first cycle, retreatment usually induced end-of-treatment response. A complete sustained response was obtained in only one of every five subjects. Increasing the dose of interferon above that of the first cycle did not enhance the rate of sustained response. In conclusion we might assert that young subjects infected by non-1b HCV and with low levels of HCV-RNA and of 90K/MAC-2 BP are the best candidates for retreatment.
在慢性丙型肝炎中,对干扰素治疗产生治疗结束反应后复发的比率可能超过50%。对复发者再次使用干扰素以获得完全持续反应的有效性,以及临床、病毒学和免疫学特征在确定再次治疗的长期疗效中的作用尚不清楚。我们旨在评估再次使用干扰素获得完全持续反应的疗效,评估增加剂量是否可增强反应性,并确定持续反应的可能预测因素。我们纳入了42例经活检证实为无肝硬化的慢性丙型肝炎患者,这些患者先前对为期6个月的α-2b干扰素疗程有反应(总剂量:A组,22例患者,234MU;B组,20例患者,468MU),随后复发。除1例患者外,所有患者在干扰素第一个疗程结束时HCV-RNA均为阴性;大多数(31/42,74%)感染的是HCV 1b型。受试者被随机分配接受另一个疗程的干扰素,剂量为原剂量(A1组:234MU,11例患者;B1组468MU,10例患者)或原剂量的两倍(A2组:468MU,11例患者;B2组:936MU,10例患者)。在干扰素第二个疗程结束时,24例受试者(57%)ALT正常且HCV-RNA阴性,16例(39%)ALT正常但HCV-RNA阳性。8例患者(19%)获得了完全持续反应,所有治疗组的发生率相似。完全持续反应者与其他患者在年龄(35.9±10.4对44.1±8.8,P=0.027)、非1b型HCV感染率(6/8对5/34,P=0.0005)、血清HCV-RNA(中位数拷贝/ml分别为74,016对321,428,P=0.037)以及血清90K/MAC-2 BP水平(5.76±3.01对10.25±5.16单位/ml,P=0.02)方面存在差异,90K/MAC-2 BP是一种与细胞防御功能有关的N-糖蛋白。多因素逻辑分析证实年龄和HCV基因型是完全持续反应的独立预测因素。在第一个疗程中接受的干扰素总剂量≥234MU的非肝硬化复发者中,再次治疗通常会诱导治疗结束反应。每五名受试者中只有一人获得完全持续反应。将干扰素剂量增加至超过第一个疗程的剂量并不能提高持续反应率。总之,我们可以断言,感染非1b型HCV、HCV-RNA水平低且90K/MAC-2 BP水平低的年轻受试者是再次治疗的最佳人选。
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