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首页> 外文期刊>Journal of Clinical Microbiology >Persistent ICT Malaria P.f/P.v Panmalarial and HRP2 Antigen Reactivity after Treatment of Plasmodium falciparumMalaria Is Associated with Gametocytemia and Results in False-Positive Diagnoses of Plasmodium vivax in Convalescence
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Persistent ICT Malaria P.f/P.v Panmalarial and HRP2 Antigen Reactivity after Treatment of Plasmodium falciparumMalaria Is Associated with Gametocytemia and Results in False-Positive Diagnoses of Plasmodium vivax in Convalescence

机译:恶性疟原虫治疗后持续性ICT疟疾P.f / P.v疟疾和HRP2抗原反应性疟疾与配子细胞症相关,导致假阳性的间日疟原虫假阳性诊断

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A problem with rapid Plasmodium falciparum-specific antigen histidine-rich protein 2 (HRP2) detection tests for malaria is the persistence of antigen in blood after the disappearance of asexual-stage parasitemia and clinical symptoms, resulting in false-positive (FP) test results following treatment. The ICT P.f/P.v immunochromatographic test detects both HRP2 and a panmalarial antigen (PMA) found in both P. falciparum and Plasmodium vivax. To examine posttreatment antigen persistence with this test and whether persistent sexual-stage forms (gametocytes) are a cause of FP tests after treatment, we compared serial antigen test results with microscopy results from patients symptomatic with P. falciparum malaria in Indonesia for 28 days following treatment with chloroquine (CQ; n = 66), sulfadoxine-pyrimethamine (SP; n = 36), and artesunate plus sulfadoxine-pyrimethamine (ART + SP;n = 15). Persistent FP antigenemia following SP treatment occurred in 29% (HRP2) and 42% (PMA) of the patients on day 7 and in 10% (HRP2) and 23% (PMA) on day 14. The high rates of persistent HRP2 and PMA antigenemia following CQ and SP treatment were strongly associated with the presence of gametocytemia, with the proportion with gametocytes on day 7 posttreatment being significantly greater in those with FP results than in those with true-negative PMA and HRP2 results. Gametocyte frequency on day 14 post-SP treatment was also greater in those with FP PMA results. Following SP treatment, PMA persisted longer than HRP2, giving an FP diagnosis of P. vivax in up to 16% of patients on day 14, with all FP P. vivax diagnoses having gametocytemia. In contrast, PMA was rapidly cleared following ART + SP treatment in association with rapid clearance of gametocytemia. Gametocytes appear to be an important cause of persistent posttreatment panmalarial antigenemia in areas of endemicity and may also contribute in part to persistent HRP2 antigenemia following treatment.
机译:快速的恶性疟原虫特异性抗原组氨酸富集蛋白2(HRP2)检测测试的一个问题是无性阶段寄生虫病和临床症状消失后血液中的抗原持续存在,导致假治疗后的阳性(FP)测试结果。 ICT P.f / P.v免疫色谱测试可检测HRP2和在两个 P中发现的泛疟抗原(PMA)。恶性疟原虫和间日疟原虫。为了通过此测试检查治疗后抗原的持久性以及治疗后持久性阶段形式(配子细胞)是否是FP测试的原因,我们将连续抗原测试结果与有症状的患者的显微镜检查结果进行了比较。氯喹(CQ; n = 66),磺胺多辛-乙胺嘧啶(SP; n = 36)和青蒿琥酯治疗后,印度尼西亚的恶性疟原虫持续28天加上磺胺多辛-乙胺嘧啶(ART + SP; n = 15)。 SP治疗后持久性FP抗原血症在第7天发生在29%(HRP2)和42%(PMA)的患者中,在第14天发生在10%(HRP2)和23%(PMA)的患者中。持久性HRP2和PMA的高发生率CQ和SP治疗后的抗原血症与配子细胞减少症的存在密切相关,FP结果的患者中配子细胞比例在治疗后第7天明显高于真阴性PMA和HRP2结果的患者。 FP PMA结果的患者,SP治疗后第14天的配子细胞频率也更高。在进行SP治疗后,PMA的持续时间比HRP2长,因此FP诊断为 P。在第14天,多达16%的患者使用vivax ,所有FP P。 vivax 诊断患有配子细胞减少症。相反,ART + SP治疗后与配子细胞瘤的快速清除相关联,PMA迅速清除。配子细胞似乎是在流行地区持续治疗后泛疟抗原血症的重要原因,也可能部分导致治疗后持续HRP2抗原血症。

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