Effects of Schistosoma haematobium infection and treatment on the systemic and mucosal immune phenotype, gene expression and microbiome: A systematic review

IF 3.8 2区医学 Q1 Medicine

PLoS Neglected Tropical Diseases Pub Date : 2024-09-09 DOI:10.1371/journal.pntd.0012456

Anna M. Mertelsmann, Sheridan F. Bowers, Drew Wright, Jane K. Maganga, Humphrey D. Mazigo, Lishomwa C. Ndhlovu, John M. Changalucha, Jennifer A. Downs

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引用次数: 0

Abstract

Background Urogenital schistosomiasis caused by Schistosoma haematobium affects approximately 110 million people globally, with the majority of cases in low- and middle-income countries. Schistosome infections have been shown to impact the host immune system, gene expression, and microbiome composition. Studies have demonstrated variations in pathology between schistosome subspecies. In the case of S. haematobium, infection has been associated with HIV acquisition and bladder cancer. However, the underlying pathophysiology has been understudied compared to other schistosome species. This systematic review comprehensively investigates and assimilates the effects of S. haematobium infection on systemic and local host mucosal immunity, cellular gene expression and microbiome. Methods We conducted a systematic review assessing the reported effects of S. haematobium infections and anthelmintic treatment on the immune system, gene expression and microbiome in humans and animal models. This review followed PRISMA guidelines and was registered prospectively in PROSPERO (CRD42022372607). Randomized clinical trials, cohort, cross-sectional, case-control, experimental ex vivo, and animal studies were included. Two reviewers performed screening independently. Results We screened 3,177 studies and included 94. S. haematobium was reported to lead to: (i) a mixed immune response with a predominant type 2 immune phenotype, increased T and B regulatory cells, and select pro-inflammatory cytokines; (ii) distinct molecular alterations that would compromise epithelial integrity, such as increased metalloproteinase expression, and promote immunological changes and cellular transformation, specifically upregulation of genes p53 and Bcl-2; and (iii) microbiome dysbiosis in the urinary, intestinal, and genital tracts. Conclusion S. haematobium induces distinct alterations in the host’s immune system, molecular profile, and microbiome. This leads to a diverse range of inflammatory and anti-inflammatory responses and impaired integrity of the local mucosal epithelial barrier, elevating the risks of secondary infections. Further, S. haematobium promotes cellular transformation with oncogenic potential and disrupts the microbiome, further influencing the immune system and genetic makeup. Understanding the pathophysiology of these interactions can improve outcomes for the sequelae of this devastating parasitic infection.

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血吸虫感染和治疗对全身和粘膜免疫表型、基因表达和微生物组的影响：系统综述

背景由血吸虫引起的尿路血吸虫病影响着全球约 1.1 亿人，其中大多数病例发生在中低收入国家。研究表明，血吸虫感染会影响宿主的免疫系统、基因表达和微生物组组成。研究表明，血吸虫亚种之间的病理学存在差异。就血吸虫而言，感染与艾滋病病毒感染和膀胱癌有关。然而，与其他血吸虫物种相比，人们对其潜在的病理生理学研究不足。本系统综述全面研究并吸收了血吸虫感染对全身和局部宿主粘膜免疫、细胞基因表达和微生物组的影响。方法我们进行了一项系统性综述，评估已报道的血吸虫感染和抗蠕虫药治疗对人类和动物模型的免疫系统、基因表达和微生物组的影响。该综述遵循了 PRISMA 指南，并在 PROSPERO（CRD42022372607）中进行了前瞻性注册。随机临床试验、队列研究、横断面研究、病例对照研究、实验性体内外研究和动物研究均被纳入其中。两名审稿人独立进行筛选。结果我们筛选了 3,177 项研究，并纳入了 94 项研究。据报道，血吸虫会导致(i) 混合免疫反应，主要是 2 型免疫表型、T 和 B 调节细胞增加以及选择性促炎细胞因子；(ii) 明显的分子改变，损害上皮完整性，如金属蛋白酶表达增加，促进免疫学改变和细胞转化，特别是 p53 和 Bcl-2 基因上调；以及 (iii) 泌尿道、肠道和生殖道微生物群失调。结论血吸虫会诱导宿主的免疫系统、分子特征和微生物组发生明显改变。这导致了多种多样的炎症和抗炎反应，并损害了局部粘膜上皮屏障的完整性，增加了二次感染的风险。此外，血孢子虫还会促进具有致癌潜力的细胞转化，并破坏微生物组，进一步影响免疫系统和基因构成。了解这些相互作用的病理生理学可以改善这种毁灭性寄生虫感染后遗症的治疗效果。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

PLoS Neglected Tropical Diseases Medicine-Infectious Diseases

CiteScore

7.40

自引率

10.50%

发文量

723

审稿时长

2-3 weeks

期刊介绍： PLOS Neglected Tropical Diseases publishes research devoted to the pathology, epidemiology, prevention, treatment and control of the neglected tropical diseases (NTDs), as well as relevant public policy. The NTDs are defined as a group of poverty-promoting chronic infectious diseases, which primarily occur in rural areas and poor urban areas of low-income and middle-income countries. Their impact on child health and development, pregnancy, and worker productivity, as well as their stigmatizing features limit economic stability. All aspects of these diseases are considered, including: Pathogenesis Clinical features Pharmacology and treatment Diagnosis Epidemiology Vector biology Vaccinology and prevention Demographic, ecological and social determinants Public health and policy aspects (including cost-effectiveness analyses).