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首页> 外文期刊>JAIDS: Journal of acquired immune deficiency syndromes >Performance of clinical algorithms for HIV-1 diagnosis and antiretroviral initiation among HIV-1-exposed children aged less than 18 months in Kenya.
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Performance of clinical algorithms for HIV-1 diagnosis and antiretroviral initiation among HIV-1-exposed children aged less than 18 months in Kenya.

机译:在肯尼亚,年龄小于18个月的HIV-1暴露儿童的HIV-1诊断和抗逆转录病毒起始临床算法的性能。

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BACKGROUND: Ninety percent of HIV-1-infected children live in sub-Saharan Africa. In the absence of diagnosis and antiretroviral therapy, approximately 50% die before 2 years. METHODS: We evaluated sensitivity and specificity of clinical algorithms for diagnosis of HIV-1 infection and antiretroviral therapy initiation among HIV-1-exposed children aged less than 18 months. Children were identified with routine HIV-1 testing and assessed using 3 sets of criteria: (1) Integrated Management of Childhood Illnesses (IMCI), (2) World Health Organization Presumptive Diagnosis (WHO-PD) for HIV-1 infection, and (3) CD4 T-lymphocyte cell subsets. HIV-1 infection status was determined using DNA polymerase chain reaction testing. FINDINGS: A total of 1418 children (median age 5.4 months) were screened for HIV-1 antibodies, of whom 144 (10.2%) were seropositive. Of these, 134 (93%) underwent HIV-1 DNA testing and 80 (60%) were found to be HIV-1 infected. Compared with HIV-1 DNA testing, sensitivity and specificity of the IMCI criteria were 19% and 96% and for WHO-PD criteria 43% and 88%, respectively. Inclusion of severe immune deficiency determined by CD4% improved sensitivity of IMCI and WHO-PD criteria to 74% and 84%, respectively; however, specificity declined to 43% and 41%, respectively. INTERPRETATION: Diagnosis of HIV-1 infection among exposed children less than 18 months in a high-prevalence resource-limited setting remains a challenge, and current recommended algorithms have low sensitivity. This underscores the need for rapid scale-up of viral assays for early infant diagnosis.
机译:背景:HIV-1感染儿童的百分之九十生活在撒哈拉以南非洲。在没有诊断和抗逆转录病毒疗法的情况下,大约50%的患者在2年之前死亡。方法:我们评估了在年龄小于18个月的HIV-1暴露儿童中诊断HIV-1感染和开始抗逆转录病毒治疗的临床算法的敏感性和特异性。对儿童进行了常规HIV-1检测,并使用3套标准进行了评估:(1)儿童疾病综合管理(IMCI),(2)世界卫生组织HIV-1感染的假定诊断(WHO-PD)和( 3)CD4 T淋巴细胞亚群。使用DNA聚合酶链反应测试确定HIV-1感染状况。结果:总共对1418名儿童(中位年龄5.4个月)进行了HIV-1抗体筛查,其中144名(10.2%)血清阳性。其中134(93%)人接受了HIV-1 DNA检测,发现80(60%)人感染了HIV-1。与HIV-1 DNA检测相比,IMCI标准的敏感性和特异性分别为19%和96%,而WHO-PD标准的敏感性和特异性分别为43%和88%。通过CD4%确定的严重免疫缺陷纳入将IMCI和WHO-PD标准的敏感性分别提高至74%和84%;然而,特异性分别下降至43%和41%。解释:在资源有限的高流行地区,对少于18个月的暴露儿童进行HIV-1感染的诊断仍然是一个挑战,目前推荐的算法敏感性较低。这突显了需要快速扩大用于婴儿早期诊断的病毒检测的规模。

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