Persistent replication of human immunodeficiency virus type 1 despite treatment of pulmonary tuberculosis in dually infected subjects.

Harriet Mayanja Kizza, Benigno Rodriguez, Miguel Quinones-Mateu, Muneer Mirza, Htin Aung, Belinda Yen-Lieberman, Colleen Starkey, Libby Horter, Pierre Peters, Joy Baseke, John L Johnson, Zahra Toossi
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引用次数: 30

Abstract

Tuberculosis (TB) is the most common life-threatening infection in human immunodeficiency virus (HIV)-infected persons and frequently occurs before the onset of severe immunodeficiency. Development of TB is associated with increased HIV type 1 (HIV-1) viral load, a fall in CD4 lymphocyte counts, and increased mortality. The aim of this study was to examine how treatment of pulmonary TB affected HIV-1 activity in HIV-1/TB-coinfected subjects with CD4 cell counts of >100 cells/mul. HIV-1/TB-coinfected subjects were recruited in Kampala, Uganda, and were monitored over time. Based upon a significant (0.5 log10 copies/ml) decrease in viral load by the end of treatment, two patient groups could be distinguished. Responders (n = 17) had more rapid resolution of anemia and pulmonary lesions on chest radiography during TB treatment. This group had a significant increase in viral load to levels not different from those at baseline 6 months after completion of TB treatment. HIV-1 viral load in nonresponders (n = 10) with TB treatment increased and at the 6 month follow-up was significantly higher than that at the time of diagnosis of TB. Compared to baseline levels, serum markers of macrophage activation including soluble CD14 decreased significantly by the end of TB treatment in responders but not in nonresponders. These data further define the impact of pulmonary TB on HIV-1 disease. HIV-1 replication during dual HIV-1/TB infection is not amenable to virologic control by treatment of TB alone. Concurrent institution of highly active antiretroviral treatment needs to be evaluated in patients dually infected with pulmonary TB and HIV-1.

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尽管在双重感染的受试者中治疗肺结核,人类免疫缺陷病毒1型持续复制。
结核病(TB)是人类免疫缺陷病毒(HIV)感染者中最常见的危及生命的感染,通常发生在严重免疫缺陷发病之前。结核病的发展与艾滋病毒1型(HIV-1)病毒载量增加、CD4淋巴细胞计数下降和死亡率增加有关。本研究的目的是研究治疗肺结核如何影响CD4细胞计数>100细胞/多例HIV-1/TB共感染患者的HIV-1活性。在乌干达坎帕拉招募了HIV-1/ tb合并感染的受试者,并对其进行了长期监测。根据治疗结束时病毒载量显著下降(0.5 log10拷贝/ml),可以区分两组患者。有反应者(n = 17)在结核病治疗期间的胸片上有更快的贫血和肺部病变的消退。该组在完成结核病治疗6个月后,病毒载量显著增加,达到与基线水平无差异的水平。在接受结核病治疗的无应答者(n = 10)中,HIV-1病毒载量在6个月的随访中显著高于诊断为结核病时的水平。与基线水平相比,在结核病治疗结束时,应答者中巨噬细胞激活的血清标志物(包括可溶性CD14)显著下降,而在无应答者中则没有。这些数据进一步确定了肺结核对HIV-1疾病的影响。在HIV-1/TB双重感染期间,HIV-1复制无法通过单独治疗结核病进行病毒学控制。需要对双重感染肺结核和HIV-1的患者同时进行高活性抗逆转录病毒治疗进行评估。
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