基于利什曼原虫感染标志物对埃塞俄比亚一个高度暴露的艾滋病毒队列中内脏利什曼病发展的预测：PreLeisH研究结果

Prediction of visceral leishmaniasis development in a highly exposed HIV cohort in Ethiopia based on Leishmania infection markers: results from the PreLeisH study.

作者信息

van Griensven Johan, van Henten Saskia, Kibret Aderajew, Kassa Mekibib, Beyene Hailemariam, Abdellati Saïd, Mersha Dagnew, Sisay Kasaye, Seyum Hailemicheal, Eshetie Hamid, Kassa Fikadu, Bogale Tadfe, Melkamu Roma, Yeshanew Arega, Smekens Bart, Burm Christophe, Landuyt Hanne, de Hondt Annelies, Van den Bossche Dorien, Mohammed Rezika, Pareyn Myrthe, Vogt Florian, Adriaensen Wim, Ritmeijer Koert, Diro Ermias

机构信息

Institute of Tropical Medicine, Antwerp, Belgium.

出版信息

EBioMedicine. 2024 Dec;110:105474. doi: 10.1016/j.ebiom.2024.105474. Epub 2024 Nov 29.

DOI:10.1016/j.ebiom.2024.105474

PMID:39612653

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11647465/

Abstract

BACKGROUND

Targeted preventive strategies in persons living with HIV (PLWH) require markers to predict visceral leishmaniasis (VL). We conducted a longitudinal study in a HIV-cohort in VL-endemic North-West Ethiopia to 1) describe the pattern of Leishmania markers preceding VL; 2) identify Leishmania markers predictive of VL; 3) develop a clinical management algorithm according to predicted VL risk levels.

METHODS

The PreLeisH study followed 490 adult PLWH free of VL at enrolment for up to two years (2017-2021). Blood RT-PCR targeting Leishmania kDNA, Leishmania serology and Leishmania urine antigen test (KAtex) were performed every 3-6 months. We calculated the sensitivity/specificity of the Leishmania markers for predicting VL and developed an algorithm for distinct clinical management strategies, with VL risk categories defined based on VL history, CD4 count and Leishmania markers (rK39 RDT & RT-PCR).

FINDINGS

At enrolment, 485 (99%) study participants were on antiretroviral treatment; 360/490 (73.5%) were male; the median baseline CD4 count was 392 (IQR 259-586) cells/μL; 135 (27.5%) had previous VL. Incident VL was diagnosed in 34 (6.9%), with 32 (94%) displaying positive Leishmania markers before VL. In those without VL history, baseline rK39 RDT had 60% sensitivity and 84% specificity to predict VL; in patients with previous VL, RT-PCR had 71% sensitivity and 95% specificity. The algorithm defined 442 (92.3%) individuals at low VL risk (routine follow-up), 31 (6.5%) as moderate risk (secondary prophylaxis) and six (1.2%) as high risk (early treatment).

INTERPRETATION

Leishmania infection markers can predict VL risk in PLWH. Interventional studies targeting those at high risk are needed.

FUNDING

The PreLeisH study was supported by grants from the Department of Economy, Science and Innovation of the Flemish Government, Belgium (757013) and the Directorate-General for Development Cooperation and Humanitarian Aid (DGD), Belgium (BE-BCE_KBO-0410057701-prg2022-5-ET).

摘要

背景

针对艾滋病病毒感染者（PLWH）的针对性预防策略需要标志物来预测内脏利什曼病（VL）。我们在埃塞俄比亚西北部VL流行地区的一个艾滋病队列中进行了一项纵向研究，以1）描述VL之前利什曼原虫标志物的模式；2）识别预测VL的利什曼原虫标志物；3）根据预测的VL风险水平制定临床管理算法。

方法

PreLeisH研究对490名入组时无VL的成年PLWH进行了长达两年（2017 - 2021年）的随访。每3 - 6个月进行一次针对利什曼原虫kDNA的血液RT-PCR、利什曼原虫血清学检测和利什曼原虫尿液抗原检测（KAtex）。我们计算了利什曼原虫标志物预测VL的敏感性/特异性，并制定了不同临床管理策略的算法，根据VL病史、CD4细胞计数和利什曼原虫标志物（rK39快速诊断试验和RT-PCR）定义VL风险类别。

研究结果

入组时，485名（99%）研究参与者正在接受抗逆转录病毒治疗；360/490名（73.5%）为男性；基线CD4细胞计数中位数为392（四分位间距259 - 586）个/μL；135名（27.5%）有既往VL病史。34名（6.9%）被诊断为新发VL，其中32名（94%）在VL出现前利什曼原虫标志物呈阳性。在无VL病史的人群中，基线rK39快速诊断试验预测VL的敏感性为60%，特异性为84%；在有既往VL病史的患者中，RT-PCR的敏感性为71%，特异性为95%。该算法将442名（92.3%）个体定义为低VL风险（常规随访），31名（6.5%）为中度风险（二级预防），6名（1.2%）为高风险（早期治疗）。

解读

利什曼原虫感染标志物可预测PLWH的VL风险。需要针对高风险人群开展干预性研究。

资助

PreLeisH研究得到了比利时弗拉芒政府经济、科学和创新部（757013）以及比利时发展合作与人道主义援助总局（DGD）（BE - BCE_KBO - 0410057701 - prg2022 - 5 - ET）的资助。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d10/11647465/c0a6308c7d30/gr1.jpg

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基于利什曼原虫感染标志物对埃塞俄比亚一个高度暴露的艾滋病毒队列中内脏利什曼病发展的预测：PreLeisH研究结果

Prediction of visceral leishmaniasis development in a highly exposed HIV cohort in Ethiopia based on Leishmania infection markers: results from the PreLeisH study.

作者信息

机构信息

出版信息

BACKGROUND

METHODS

FINDINGS

INTERPRETATION

FUNDING

背景

方法

研究结果

解读

资助

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