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HCV RNA viral load is independent from CD4 cell count and plasma HIV RNA viral load in immunocompetent HIV-HCV co-infected patients: a 3-years follow-up study

机译:在具有免疫能力的HIV-HCV合并感染患者中,HCV RNA病毒载量与CD4细胞计数和血浆HIV RNA病毒载量无关:为期3年的随访研究

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Background HCV RNA viral load is an important predictor of sustained virological response and, recently, a significant correlation with liver fibrosis was described. We investigated on possible influence of clinical and viro-immunological variables on HCV viral load in HIV-HCV co-infected patients over a study time of three years (2009-2012). Methods We retrospectively enrolled 98 adult patients with a diagnosis of chronic HIV infection in 2009, a diagnosis of chronic HCV infection with a detectable plasma HCV RNA in 2009 and 2012, HCV therapy-na?ve or with failed and stopped antiviral treatment before June 2008. The following variables were recorded: age, gender, HCV genotype, IL28B rs12979860 CC genotype, HCV treatment status, advanced liver fibrosis diagnosis, antiretroviral therapy, CD4+ cell count, HCV viral load, HIV RNA (plasma HIV-1 RNA levels were measured from blood samples every three months at least). The correlation was established using linear regression analysis, analysis of variance and Fisher’s exact test. Comparisons between groups were performed using Fisher’s exact test, the independent samples t-test and the t-test for paired data, as appropriate, for continuous variables. A mixed mode (ME) maximum likelihood linear regression model was constructed to evaluate the dependence of HCV viral load. Results HCV RNA levels did not change significantly from 2009 to 2012 (from 3924650?±?5320177?IU/ml to 3085128?±?3372347?IU/ml, p?=?0.13); the CD4+ count increased significantly (from a mean of 576 to a mean of 654, p?=?0.003). Using linear regression, a positive correlation was observed for HCV load and genotype 1 (p?=?0.002), nonresponder status (p?=?0.04) and with interleukin 28B CC allele (p?=?0.05). Other studied covariates failed to reach a significant correlation. Conclusions The HCV RNA load, a known pretreatment predictor of response to antiviral therapy, was independent of the two main parameters of HIV disease, plasma HIV RNA and CD4 cell count, over an observation time of 3?years in patients with recovered or spontaneously maintained immunocompetence.
机译:背景HCV RNA病毒载量是持续病毒学应答的重要预测指标,最近,它与肝纤维化有显着相关性。我们调查了在三年(2009-2012年)的研究时间内,临床和病毒免疫学变量对HIV-HCV合并感染患者中HCV病毒载量的可能影响。方法我们回顾性研究了2009年诊断为慢性HIV感染的98名成年患者,2009年和2012年诊断为慢性HCV感染并具有可检测的血浆HCV RNA,未进行过HCV治疗或抗病毒治疗失败和停止治疗的患者。记录以下变量:年龄,性别,HCV基因型,IL28B rs12979860 CC基因型,HCV治疗状态,晚期肝纤维化诊断,抗逆转录病毒疗法,CD4 +细胞计数,HCV病毒载量,HIV RNA(测定血浆HIV-1 RNA水平至少每三个月从血液样本中提取一次)。使用线性回归分析,方差分析和Fisher精确检验来建立相关性。使用费舍尔精确检验,独立样本t检验和配对数据的t检验(适用时,连续变量)进行组之间的比较。构建了混合模式(ME)最大似然线性回归模型,以评估HCV病毒载量的依赖性。结果HCV RNA水平从2009年至2012年没有显着变化(从3924650?±?5320177?IU / ml到3085128?±?3372347?IU / ml,p?=?0.13); CD4 +计数显着增加(从576平均值增加到654,平均值p = 0.003)。使用线性回归,观察到HCV负荷和基因型1(p≥0.002),无反应者状态(p≥0.04)和白介素28B CC等位基因(p≥0.05)呈正相关。其他研究的协变量未能达到显着的相关性。结论HCV RNA负荷是已知的抗病毒治疗反应的预处理指标,在3年的观察时间内,恢复或自发维持的患者独立于HIV疾病的两个主要参数,血浆HIV RNA和CD4细胞计数免疫能力。

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