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儿童疾病综合管理(IMCI)策略下的疟疾诊断与治疗:ICT疟疾P.f/P.v快速免疫层析检测和OptiMal实验室支持的相关性

Malaria diagnosis and treatment under the strategy of the integrated management of childhood illness (IMCI): relevance of laboratory support from the rapid immunochromatographic tests of ICT Malaria P.f/P.v and OptiMal.

作者信息

Tarimo D S, Minjas J N, Bygbjerg I C

机构信息

Department of Parasitology and Medical Entomology, Institute of Public Health, Muhimbili University College of Health Sciences, University of Dar es Salaam, P.O. Box 65001, Dar es Salaam, Tanzania.

出版信息

Ann Trop Med Parasitol. 2001 Jul;95(5):437-44. doi: 10.1080/13648590120068971.

Abstract

The algorithm developed for the integrated management of childhood illness (IMCI) provides guidelines for the treatment of paediatric malaria. In areas where malaria is endemic, for example, the IMCI strategy may indicate that children who present with fever, a recent history of fever and/or pallor should receive antimalarial chemotherapy. In many holo-endemic areas, it is unclear whether laboratory tests to confirm that such signs are the result of malaria would be very relevant or useful. Children from a holo-endemic region of Tanzania were therefore checked for malarial parasites by microscopy and by using two rapid immunochromatographic tests (RIT) for the diagnosis of malaria (ICT Malaria P.f/P.v and OptiMal. At the time they were tested, each of these children had been targeted for antimalarial treatment (following the IMCI strategy) because of fever and/or pallor. Only 70% of the 395 children classified to receive antimalarial drugs by the IMCI algorithm had malarial parasitaemias (68.4% had Plasmodium falciparum trophozoites, 1.3% only P. falciparum gametocytes, 0.3% P. ovale and 0.3% P. malariae). As indicators of P. falciparum trophozoites in the peripheral blood, fever had a sensitivity of 93.0% and a specificity of 15.5% whereas pallor had a sensitivity of 72.2% and a specificity of 50.8%. The RIT both had very high corresponding sensitivities (of 100.0% for the ICT and 94.0% for OptiMal) but the specificity of the ICT (74.0%) was significantly lower than that for OptiMal (100.0%). Fever and pallor were significantly associated with the P. falciparum asexual parasitaemias that equalled or exceeded the threshold intensity (2000/microl) that has the optimum sensitivity and specificity for the definition of a malarial episode. Diagnostic likelihood ratios (DLR) showed that a positive result in the OptiMal test (DLR = infinity) was a better indication of malaria than a positive result in the ICT (DLR = 3.85). In fact, OptiMal had diagnostic reliability (0.93) which approached that of an ideal test and, since it only detects live parasites, OptiMal is superior to the ICT in monitoring therapeutic responses. Although the RIT may seem attractive for use in primary health facilities because relatively inexperienced staff can perform them, the high cost of these tests is prohibitive. In holo-endemic areas, use of RIT or microscopical examination of bloodsmears may only be relevant when malaria needs to be excluded as a cause of illness (e.g. prior to treatment with toxic or expensive drugs, or during malaria epidemics). Wherever the effective drugs for the first-line treatment of malaria are cheap (e.g. chloroquine and Fansidar), treatment based on clinical diagnosis alone should prove cost-saving in health facilities without microscopy.

摘要

为儿童疾病综合管理(IMCI)制定的算法为小儿疟疾治疗提供了指导方针。例如,在疟疾流行地区,IMCI策略可能表明,出现发热、近期有发热病史和/或面色苍白的儿童应接受抗疟化疗。在许多高度流行地区,尚不清楚通过实验室检测来确认这些症状是否由疟疾导致是否具有相关性或实用性。因此,对来自坦桑尼亚高度流行地区的儿童进行了显微镜检查,并使用两种快速免疫色谱检测法(RIT)来诊断疟疾(ICT疟原虫/间日疟原虫检测试剂和OptiMal检测试剂)。在接受检测时,这些儿童中的每一个都因发热和/或面色苍白而被列为抗疟治疗对象(遵循IMCI策略)。在IMCI算法判定应接受抗疟药物治疗的395名儿童中,只有70%患有疟原虫血症(68.4%有恶性疟原虫滋养体,1.3%仅有恶性疟原虫配子体,0.3%有卵形疟原虫,0.3%有三日疟原虫)。作为外周血中恶性疟原虫滋养体的指标,发热的敏感度为93.0%,特异度为15.5%;而面色苍白的敏感度为72.2%,特异度为50.8%。两种RIT检测法的相应敏感度都非常高(ICT检测试剂为100.0%,OptiMal检测试剂为94.0%),但ICT检测试剂的特异度(74.0%)显著低于OptiMal检测试剂(100.0%)。发热和面色苍白与恶性疟原虫无性体血症显著相关,该血症等于或超过阈值强度(2000/微升),此阈值强度对疟疾病例的定义具有最佳的敏感度和特异度。诊断似然比(DLR)表明,OptiMal检测法的阳性结果(DLR = 无穷大)比ICT检测法的阳性结果(DLR = 3.85)更能表明患有疟疾。事实上,OptiMal检测法的诊断可靠性(0.93)接近理想检测法,而且由于它只检测活寄生虫,OptiMal在监测治疗反应方面优于ICT检测试剂。尽管RIT检测法可能因相对缺乏经验的工作人员也能操作而在基层卫生机构中颇具吸引力,但这些检测法成本高昂,令人望而却步。在高度流行地区,只有在需要排除疟疾作为病因时(例如在使用有毒或昂贵药物治疗之前,或在疟疾流行期间),使用RIT检测法或对血涂片进行显微镜检查才可能具有相关性。只要用于疟疾一线治疗的有效药物价格低廉(例如氯喹和Fansidar),在没有显微镜检查设备的卫生机构中,仅基于临床诊断进行治疗应能节省成本。

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