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HIV-1感染患者中GBV-C感染的特征分析。

Characterization of GBV-C infection in HIV-1 infected patients.

作者信息

Canducci F, Uberti Foppa C, Boeri E, Racca S, Gallotta G, Grasso M A, Calori G, Lazzarin A, Clementi M

机构信息

San Raffaele Microbiology and Virology, Diagnostics and Research, Milan, Italy.

出版信息

J Biol Regul Homeost Agents. 2003 Apr-Jun;17(2):191-4.

Abstract

BACKGROUND

GB virus C, a positive-stranded RNA virus, is classified in the family Flaviviridae. It is currently believed that persistent infection occurs in 25-50% of infected individuals, however, it still remains an "orphan" virus in search of a role in human pathology. Molecular epidemiological studies have demonstrated that GBV-C infection is present in about 1-1.4% of the healthy population in developed countries, that it shares routes of transmission with HIV and HCV and that the prevalence of GBV-C in these populations is higher than in blood donors. On the basis of the sequence variation among the isolates, GBV-C is classified into at least four major genotypes. Preliminary evidence has suggested that GBV-C is a lymphotropic virus that replicates mainly in the spleen and bone marrow. Recently, several reports have investigated the possible beneficial effect of GBV-C co-infection on HIV disease progression to AIDS, reduced mortality in HIV infected individuals and lower HIV viral loads, not leading to a definitive conclusion yet.

AIM

To investigate the role of GBV virus C co-infection in two different subsets of HIV-infected patients, and to evaluate the prevalence of GBV-C genotypes in Northern Italy.

METHODS

A total of 86 HIV positive patients were examined for GBV-C viremia (years after HIV sera conversion: 12 +/- 5). Control population (Group A): 46 patients (mean age 42 years) with <200CD4/ml during the observation period. Longterm non progressor population (Group B): 40 patients, (mean age 40 years) with >500 CD4/ml for at least 8 years and never treated with HAART. After extraction of viral RNA from plasma samples, amplification of a highly conserved region of 5'UTR was performed by nested RT-PCR. All positive samples were genotyped by sequencing, alignment with published sequences and phylogenetic analysis. CD4 cell count, HIV plasma levels were also evaluated.

RESULTS

9 out of 46 (19.56%) in Group A and 15 out of 40 (37.5%) in Group B had detectable GBV-C viremia (p=0.064, OR 2.47, percent confidence interval 0.94 to 6.51). No statistical difference was observed when disease stage was evaluated between the two groups. In Group B, after regression analysis for CD4 cell count decrease over the period observed, no significant difference was detected between GBV-C positive and negative patients. No significant difference was observed in Group B in HIV viremia and CD4 cell count at time of GBV-C detection between GBV-C infected patients and GBV-C negative patients. All Italian patients were genotype 2, the only African patient carried GBV-C genotype 1.

CONCLUSIONS

Although previous results suggest that GBV-C virus may be a favorable marker for long term non progression of HIV disease, whether it plays a direct anti-HIV role or just takes advantage of non progessors' higher CD4 cell count to replicate more efficiently, still remains to be answered. Follow up of untreated patients and further evaluation of virological interactions, between the viruses and the host immune system, will be helpful to shed some light on these observations, offering new prognostic and eventually therapeutical tools for the management of HIV patients.

摘要

背景

GB病毒C是一种正链RNA病毒,归类于黄病毒科。目前认为,25%至50%的感染者会发生持续性感染,然而,它在人类病理学中仍为一种“孤儿”病毒,尚未明确其作用。分子流行病学研究表明,发达国家约1%至1.4%的健康人群存在GBV-C感染,它与HIV和HCV的传播途径相同,且这些人群中GBV-C的流行率高于献血者。根据分离株之间的序列变异,GBV-C至少可分为四种主要基因型。初步证据表明,GBV-C是一种嗜淋巴细胞病毒,主要在脾脏和骨髓中复制。最近,有几份报告研究了GBV-C合并感染对HIV疾病进展至艾滋病的可能有益影响、降低HIV感染者的死亡率以及降低HIV病毒载量,但尚未得出明确结论。

目的

研究GB病毒C合并感染在两类不同HIV感染患者亚组中的作用,并评估意大利北部GBV-C基因型的流行情况。

方法

共对86例HIV阳性患者进行GBV-C病毒血症检测(HIV血清转化后的年份:12±5)。对照组(A组):46例患者(平均年龄42岁),观察期内CD4细胞计数<200/ml。长期非进展者组(B组):40例患者(平均年龄40岁),CD4细胞计数>500/ml至少8年,且从未接受过高效抗逆转录病毒治疗(HAART)。从血浆样本中提取病毒RNA后,通过巢式逆转录聚合酶链反应(RT-PCR)扩增5'非翻译区(UTR)的高度保守区域。所有阳性样本通过测序、与已发表序列比对及系统发育分析进行基因分型。同时评估CD4细胞计数和HIV血浆水平。

结果

A组46例中有9例(19.56%)、B组40例中有15例(37.5%)检测到GBV-C病毒血症(p=0.064,比值比2.47,可信区间0.94至6.51)。两组间评估疾病阶段时未观察到统计学差异。在B组中,对观察期内CD4细胞计数下降情况进行回归分析后,GBV-C阳性和阴性患者之间未检测到显著差异。在GBV-C检测时,B组中GBV-C感染患者与GBV-C阴性患者的HIV病毒血症和CD4细胞计数未观察到显著差异。所有意大利患者均为2型基因型,唯一的非洲患者携带GBV-C 1型基因型。

结论

尽管先前的结果表明GBV-C病毒可能是HIV疾病长期不进展的有利标志物,但它是发挥直接抗HIV作用,还是仅仅利用非进展者较高的CD4细胞计数更有效地复制,仍有待解答。对未治疗患者的随访以及对病毒与宿主免疫系统之间病毒学相互作用的进一步评估,将有助于阐明这些观察结果,为HIV患者的管理提供新的预后工具并最终提供治疗工具。

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