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在没有强化抗病毒治疗的情况下,丙戊酸对静息CD4+ T细胞的持续性HIV感染影响有限。

Valproic acid without intensified antiviral therapy has limited impact on persistent HIV infection of resting CD4+ T cells.

作者信息

Archin Nancy M, Eron Joseph J, Palmer Sarah, Hartmann-Duff Anne, Martinson Jeffery A, Wiegand Ann, Bandarenko Nicholas, Schmitz John L, Bosch Ronald J, Landay Alan L, Coffin John M, Margolis David M

机构信息

University of North Carolina at Chapel Hill, Chapel Hill, North Carolina, USA.

出版信息

AIDS. 2008 Jun 19;22(10):1131-5. doi: 10.1097/QAD.0b013e3282fd6df4.

Abstract

OBJECTIVES

Valproic acid and intensified antiretroviral therapy may deplete resting CD4+ T-cell HIV infection. We tested the ability of valproic acid to deplete resting CD4+ T-cell infection in patients receiving standard antiretroviral therapy.

METHODS

Resting CD4+ T-cell infection was measured in 11 stably aviremic volunteers twice prior to, and twice after Depakote ER 1000 mg was added to standard antiretroviral therapy. Resting CD4+ T-cell infection frequency was measured by outgrowth assay. Low-level viremia was quantitated by single copy plasma HIV RNA assay.

RESULTS

A decrease in resting CD4+ T-cell infection was observed in only four of the 11 patients. Levels of immune activation and HIV-specific T-cell response were low and stable. Valproic acid levels ranged from 26 to 96 microg/ml when measured near trough. Single copy assay was performed in nine patients. In three patients with depletion of resting CD4+ T-cell infection following valproic acid, single copy assay ranged from less than 1-5 copies/ml. Continuous low-level viremia was observed in three patients with stable resting CD4+ T-cell infection (24-87, 8-87, and 1-7 copies/ml respectively) in whom multiple samples were analyzed.

CONCLUSION

The prospective addition of valproic acid to stable antiretroviral therapy reduced the frequency of resting CD4+ T-cell infection in a minority of volunteers. In patients in whom resting CD4+ T-cell infection depletion was observed, viremia was rarely detectable by single copy assay.

摘要

目的

丙戊酸和强化抗逆转录病毒疗法可能会清除静息CD4+ T细胞中的HIV感染。我们测试了丙戊酸在接受标准抗逆转录病毒疗法的患者中清除静息CD4+ T细胞感染的能力。

方法

在11名病毒血症稳定的志愿者中,在将1000毫克缓释德巴金添加到标准抗逆转录病毒疗法之前和之后分别测量两次静息CD4+ T细胞感染情况。通过体外生长试验测量静息CD4+ T细胞感染频率。通过单拷贝血浆HIV RNA检测法定量低水平病毒血症。

结果

11名患者中只有4名观察到静息CD4+ T细胞感染减少。免疫激活水平和HIV特异性T细胞反应较低且稳定。在接近谷值时测量的丙戊酸水平范围为26至96微克/毫升。对9名患者进行了单拷贝检测。在三名丙戊酸治疗后静息CD4+ T细胞感染减少的患者中,单拷贝检测范围为每毫升少于1 - 5拷贝。在三名静息CD4+ T细胞感染稳定的患者(分别为24 - 87、8 - 87和1 - 7拷贝/毫升)中观察到持续低水平病毒血症,对其多个样本进行了分析。

结论

在稳定的抗逆转录病毒疗法中前瞻性添加丙戊酸可降低少数志愿者静息CD4+ T细胞感染的频率。在观察到静息CD4+ T细胞感染减少的患者中,单拷贝检测很少能检测到病毒血症。

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