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肯尼亚儿童疟原虫和 HIV-1 合并感染中血液学预测因子与严重贫血加重的关系。

Hematological predictors of increased severe anemia in Kenyan children coinfected with Plasmodium falciparum and HIV-1.

机构信息

Department of Infectious Diseases and Microbiology, University of Pittsburgh, Pittsburgh, PA, USA.

出版信息

Am J Hematol. 2010 Apr;85(4):227-33. doi: 10.1002/ajh.21653.

Abstract

Malaria and HIV-1 are coendemic in many developing countries, with anemia being the most common pediatric hematological manifestation of each disease. Anemia is also one of the primary causes of mortality in children monoinfected with either malaria or HIV-1. Although our previous results showed HIV-1(+) children with acute Plasmodium falciparum malaria [Pf(+)] have more profound anemia, potential causes of severe anemia in coinfected children remain unknown. As such, children with P. falciparum malaria (aged 3-36 months, n = 542) from a holoendemic malaria transmission area of western Kenya were stratified into three groups: HIV-1 negative [HIV-1(-)/Pf(+)]; HIV-1 exposed [HIV-1(exp)/Pf(+)]; and HIV-1 infected [HIV-1(+)/Pf(+)]. Comprehensive clinical, parasitological, and hematological measures were determined upon enrollment. Univariate, correlational, and hierarchical regression analyses were used to determine differences among the groups and to define predictors of worsening anemia. HIV-1(+)/Pf(+) children had significantly more malarial pigment-containing neutrophils (PCN), monocytosis, increased severe anemia (Hb < 6.0 g/dL), and nearly 10-fold greater mortality within 3 months of enrollment. Common causes of anemia in malaria-infected children, such as increased parasitemia or reduced erythropoiesis, did not account for worsening anemia in the HIV-1(+)/Pf(+) group nor did carriage of sickle cell trait or G6PD deficiency. Hierarchical multiple regression analysis revealed that more profound anemia was associated with elevated PCM, younger age, and increasing HIV-1 status ([HIV-1(-) --> HIV-1(exp) --> HIV-1(+)]. Thus, malaria/HIV-1 coinfection is characterized by more profound anemia and increased mortality, with acquisition of monocytic pigment having the most detrimental impact on Hb levels.

摘要

疟疾和 HIV-1 在许多发展中国家共同流行,贫血是这两种疾病在儿科中最常见的血液学表现。贫血也是疟疾或 HIV-1 单一感染儿童死亡的主要原因之一。尽管我们之前的研究结果表明,急性恶性疟原虫感染[Pf(+)]的 HIV-1(+)儿童贫血更为严重,但导致合并感染儿童严重贫血的潜在原因尚不清楚。因此,从肯尼亚西部一个全疟区采集了 3-36 个月龄的疟疾儿童(n = 542),根据 HIV-1 状态将其分为三组:HIV-1 阴性[HIV-1(-)/Pf(+)];HIV-1 暴露[HIV-1(exp)/Pf(+)];以及 HIV-1 感染[HIV-1(+)/Pf(+)]。在入组时确定了全面的临床、寄生虫学和血液学指标。使用单变量、相关性和分层回归分析来确定各组之间的差异,并确定导致贫血恶化的预测因素。HIV-1(+)/Pf(+)儿童的含疟色素中性粒细胞(PCN)、单核细胞增多症、严重贫血(Hb < 6.0 g/dL)和 3 个月内死亡率几乎增加了 10 倍。在疟疾感染儿童中,导致贫血的常见原因,如寄生虫增加或红细胞生成减少,不能解释 HIV-1(+)/Pf(+)组贫血恶化的原因,也不能解释携带镰状细胞特征或 G6PD 缺乏症的原因。分层多元回归分析显示,更严重的贫血与 PCM 升高、年龄较小和 HIV-1 状态增加有关[HIV-1(-) --> HIV-1(exp) --> HIV-1(+)。因此,疟疾/HIV-1 合并感染的特征是更严重的贫血和更高的死亡率,单核细胞色素的获得对 Hb 水平的影响最大。

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