Husa Petr, Slesinger Pavel, Stroblová Hana, Svobodník Adam, Husová Libuse
Department of Infectious Diseases, Medical Faculty, Masaryk University and Faculty Hospital Brno, Czech Republic.
Klin Mikrobiol Infekc Lek. 2008 Apr;14(2):67-73.
The aim of the study was to compare efficacy and viral kinetics during antiviral treatment in different chronic hepatitis C patients--naïve, relapsers and non-responders to previous pegylated interferon alpha (PEG-IFN) and ribavirin treatment, with different genotypes, baseline viremia, body weight, age and gender--and to find some baseline parameters which can predict Sustained Virological Response (SVR; negative serum HCV RNA 24 weeks after treatment).
216 chronic hepatitis C patients were treated with PEG-IFN alpha-2a 180 mg/wk and ribavirin 1 000 or 1 200 mg/day. There were 140 men and 76 women, mean age 40, range 19-70 years; 142 (66 %) naïve, 37 (17 %) relapsers after previous PEG-IFN and ribavirin treatment, and 37 (17 %) non-responders to this treatment. 172 (79,6%) has genotype 1 infection, 4 (1,9 %) genotype 2, 34 (15,6 %) genotype 3, 1 (0,5 %) genotype 4 or 6 infection, and 4 (1,9 %) were infected by unknown viral genotype. Quantitative detection of HCV RNA was done at baseline (216 pts.), 24 hours (83 pts.), 14 days (85 pts.), 28 days (88 pts.), and 84 days (211 pts.) after the first dose of PEG-IFN.
195 patients have completed the treatment period and 179 patients the 24-week follow-up period. The probability of SVR was significantly higher (P < 0,001) in naïve patients (74/114, 64,9 %) and relapsers (22/30, 73,3 %) than in non-responders (9/35, 25,7 %) and in genotype 3 patients (23/28, 82,1%) than genotype 1 patient (77/143, 53,8 %) (P = 0,002). The patients with SVR comparing those without SVR have significantly lower weight (mean 72,8 kg vs. 79,1, P = 0,008(, were younger (mean 36,2, vs. 45,5, P > 0,001), and had lower baseline viremia (mean 1,014 3 106 IU/mL vs. 2,415 3 106 IU/mL, P > 0,001). SVR was more frequent in women than in men (43/63, 62,8 % vs. 62/116, 53,4 %) but difference was not significant (P = 0,059). Undetectable serum HCV RNA at week 12 was more predictive of SVR than early viral response (minimum 2 log decrease of serum HCV RNA during the first 12 weeks of treatment)--98/122 (80,3 %) versus 104/141 (73,1 %) of SVR.
本研究旨在比较不同慢性丙型肝炎患者(初治患者、复发患者以及既往聚乙二醇化干扰素α[PEG-IFN]和利巴韦林治疗无应答者)在抗病毒治疗期间的疗效和病毒动力学,这些患者具有不同的基因型、基线病毒血症、体重、年龄和性别,并寻找一些能够预测持续病毒学应答(SVR;治疗后24周血清HCV RNA阴性)的基线参数。
216例慢性丙型肝炎患者接受180mg/周的PEG-IFNα-2a和1000或1200mg/天的利巴韦林治疗。其中男性140例,女性76例,平均年龄40岁,范围为19 - 70岁;142例(66%)为初治患者,37例(17%)为既往PEG-IFN和利巴韦林治疗后的复发患者,37例(17%)为该治疗的无应答者。172例(79.6%)感染基因型1,4例(1.9%)感染基因型2,34例(15.6%)感染基因型3,1例(0.5%)感染基因型4或6,4例(1.9%)病毒基因型未知。在基线(216例患者)、首剂PEG-IFN后24小时(83例患者)、14天(85例患者)、28天(88例患者)和84天(211例患者)进行HCV RNA定量检测。
195例患者完成治疗期,179例患者完成24周随访期。初治患者(74/114,6 A4.9%)和复发患者(22/30,73.3%)的SVR概率显著高于无应答者(9/35,25.7%),基因型3患者(23/28,82.1%)的SVR概率高于基因型1患者(77/143,53.8%)(P = 0.002)。与无SVR的患者相比,有SVR的患者体重显著更低(平均72.8kg对79.1kg,P = 0.008),年龄更小(平均年龄36.2岁对45.5岁,P > 0.001),且基线病毒血症更低(平均1.014×10⁶IU/mL对2.415×10⁶IU/mL,P > 0.001)。女性的SVR比男性更常见(43/63,62.8%对62/116,53.4%),但差异无统计学意义(P = 0.059)。治疗第12周时血清HCV RNA不可测比早期病毒应答(治疗前12周血清HCV RNA至少下降2个对数)更能预测SVR - SVR患者中98/122(80.3%)对104/141(73.1%)。
1)丙型肝炎患者抗病毒治疗前12周的病毒动力学监测对SVR具有重要预测价值。2)治疗第12周时血清HCV RNA阴性比早期病毒应答更能预测SVR。3)基线病毒血症较低、体重较轻和年龄较小的患者SVR概率显著更高。4)性别对治疗疗效无显著影响。
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