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对需要输血的晚期HIV感染患者进行巨细胞病毒的定性和定量PCR检测。

Qualitative and quantitative PCR measures of cytomegalovirus in patients with advanced HIV infection who require transfusions.

作者信息

Para M F, Kalish L A, Collier A C, Pollard R B, Kumar P N, Mintz L, Wallach F R, Drew W L

机构信息

Department of Medicine, Ohio State University, Columbus, Ohio, USA.

出版信息

J Acquir Immune Defic Syndr. 2001 Apr 1;26(4):320-5. doi: 10.1097/00126334-200104010-00004.

Abstract

The Viral Activation Transfusion Study (VATS) was a randomized trial that compared leukocyte-reduced transfusions with unfiltered red blood cell transfusions in HIV and cytomegalovirus (CMV) antibody-positive patients with anemia who were undergoing their first blood transfusion. The relations of the baseline qualitative and quantitative polymerase chain reaction (PCR) measures of plasma CMV viremia, HIV RNA, CD4(+) cell counts, and quality of life in these study subjects were examined. The 511 study subjects had a median CD4(+) cell count equal to 15 cells/mm3, and 110 (21.5%) had CMV viremia by qualitative assay. In multivariate models, frequency of positive qualitative CMV increased with decreasing CD4(+) cell counts (p =.04 trend), higher HIV RNA (p <.001), and a history of CMV disease (p <.001). Quantitative CMV PCR were performed on the 110 qualitative assay-positive study subjects. Median CMV viral load was 1780 copies/ml. In multivariate regression models, lower CD4(+) cell count (p =.03), and a history of CMV disease (p <.001) correlated with the level of CMV load. HIV RNA load and CMV load were not correlated. A lower Karnofsky score was associated with both the presence and quantity of CMV DNA.

摘要

病毒激活输血研究(VATS)是一项随机试验,比较了在首次接受输血的贫血且人类免疫缺陷病毒(HIV)和巨细胞病毒(CMV)抗体阳性患者中,白细胞减少的输血与未过滤的红细胞输血。研究了这些受试者血浆CMV病毒血症、HIV RNA、CD4(+)细胞计数的基线定性和定量聚合酶链反应(PCR)测量值与生活质量之间的关系。511名研究受试者的CD4(+)细胞计数中位数等于15个细胞/mm3,110名(21.5%)通过定性检测有CMV病毒血症。在多变量模型中,定性CMV阳性频率随CD4(+)细胞计数减少(p = 0.04趋势)、HIV RNA水平升高(p < 0.001)以及有CMV疾病史(p < 0.001)而增加。对110名定性检测阳性的研究受试者进行了定量CMV PCR。CMV病毒载量中位数为1780拷贝/ml。在多变量回归模型中,较低的CD4(+)细胞计数(p = 0.03)和CMV疾病史(p < 0.001)与CMV载量水平相关。HIV RNA载量与CMV载量不相关。较低的卡诺夫斯基评分与CMV DNA的存在和数量均相关。

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