Investigation of parasite genetic variation and systemic immune responses in patients presenting with different clinical presentations of cutaneous leishmaniasis caused by Leishmania aethiopica.

IF 8.1 1区 医学 Infectious Diseases of Poverty Pub Date : 2024-10-16 DOI:10.1186/s40249-024-01244-x
Endalew Yizengaw, Yegnasew Takele, Susanne Franssen, Bizuayehu Gashaw, Mulat Yimer, Emebet Adem, Endalkachew Nibret, Gizachew Yismaw, Edward Cruz Cervera, Kefale Ejigu, Dessalegn Tamiru, Abaineh Munshea, Ingrid Müller, Richard Weller, James A Cotton, Pascale Kropf
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Abstract

Background: Cutaneous leishmaniasis (CL) is a neglected tropical skin disease, caused by the protozoan parasite Leishmania. In Ethiopia, CL is mainly caused by Leishmania aethiopica and can present in different clinical forms. The aim of this study was to assess whether these different forms are associated with differences in parasite genetic and host systemic immune signatures.

Methods: Here we analysed the whole genome sequence data for 48 clinical parasite isolates and the systemic immune signature from a cohort of CL patients, who were recruited in Nefas Mewcha, Northern Ethiopia, from January 2019 to January 2022.

Results: Our results show that parasites from CL cases with different presentations in a single Ethiopian setting are from the same genetic population based on a permutation test of genome-wide similarity. Furthermore, a logistic regression test for genome wide association did not identify any individual genetic variants significantly associated with disease presentation. We also measured plasma chemokine and cytokine levels of 129 CL patients presenting with different forms of CL. None of the chemokine [eotaxin, eotaxin-3, interleukin (IL)-8, interferon (IFN)-γ-induced protein-10 (IP-10), monocyte chemoattractant protein (MCP)-1, MCP-4, macrophage-derived chemokines (MDC), macrophage inflammatory protein (MIP)-1α, MIP-1β and thymus- and activation-regulated chemokine (TARC)] or cytokine (IFN-γ, IL-1β, interleukin-2, IL-4, IL-6, IL-10, IL-12p70, IL-13, tumor necrosis factor-α) levels measured were significantly different between the different clinical presentations of CL, as measured by Kruskal-Wallis test. We also compared those with healthy nonendemic controls: our results show a chemokine (IP-10, MCP-1, MCP-4, MDC, MIP-1α, MIP-1β and TARC) but not a cytokine immune signature in patients with CL as compared to healthy nonendemic controls, as measured by Mann-Whitney test.

Conclusions: The results of our study did not identify a systemic immune signature or parasite genetic factors associated with different clinical presentation of CL.

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对不同临床表现的皮肤利什曼病患者寄生虫基因变异和全身免疫反应的调查。
背景:皮肤利什曼病(CL)是一种被忽视的热带皮肤病,由原生动物寄生虫利什曼原虫引起。在埃塞俄比亚,皮肤利什曼病主要由Leishmania aethiopica引起,可表现为不同的临床形式。本研究的目的是评估这些不同形式是否与寄生虫基因和宿主系统免疫特征的差异有关。方法:我们在此分析了 48 个临床寄生虫分离物的全基因组序列数据和来自一组 CL 患者的系统免疫特征,这些患者于 2019 年 1 月至 2022 年 1 月期间在埃塞俄比亚北部的 Nefas Mewcha 被招募:结果:我们的研究结果表明,根据全基因组相似性的置换检验,来自埃塞俄比亚单一环境中不同表现形式的CL病例的寄生虫来自同一遗传群体。此外,全基因组关联的逻辑回归测试并未发现任何与疾病表现显著相关的个体遗传变异。我们还测量了 129 名不同形式 CL 患者的血浆趋化因子和细胞因子水平。或细胞因子(IFN-γ、IL-1β、白细胞介素-2、IL-4、IL-6、IL-10、IL-12p70、IL-13、肿瘤坏死因子-α)水平,经 Kruskal-Wallis 检验,CL 不同临床表现之间存在显著差异。我们还将CL患者与健康的非流行病对照组进行了比较:结果显示,与健康的非流行病对照组相比,CL患者体内存在趋化因子(IP-10、MCP-1、MCP-4、MDC、MIP-1α、MIP-1β和TARC),但没有细胞因子免疫特征,这是由Mann-Whitney检验得出的:我们的研究结果没有发现与CL不同临床表现相关的全身免疫特征或寄生虫遗传因素。
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来源期刊
Infectious Diseases of Poverty
Infectious Diseases of Poverty INFECTIOUS DISEASES-
自引率
1.20%
发文量
368
期刊介绍: Infectious Diseases of Poverty is an open access, peer-reviewed journal that focuses on addressing essential public health questions related to infectious diseases of poverty. The journal covers a wide range of topics including the biology of pathogens and vectors, diagnosis and detection, treatment and case management, epidemiology and modeling, zoonotic hosts and animal reservoirs, control strategies and implementation, new technologies and application. It also considers the transdisciplinary or multisectoral effects on health systems, ecohealth, environmental management, and innovative technology. The journal aims to identify and assess research and information gaps that hinder progress towards new interventions for public health problems in the developing world. Additionally, it provides a platform for discussing these issues to advance research and evidence building for improved public health interventions in poor settings.
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