Giardia duodenalis Virulence - "To Be, or Not To Be".

IF 3.6 Q2 INFECTIOUS DISEASES
Current Tropical Medicine Reports Pub Date : 2021-01-01 Epub Date: 2021-10-21 DOI:10.1007/s40475-021-00248-z
Raúl Argüello-García, M Guadalupe Ortega-Pierres
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引用次数: 13

Abstract

Purpose of review: Here, we review recent progress made on the genetic characterization of Giardia duodenalis assemblages and their relationship with virulence. We also discuss the implications of virulence factors in the pathogenesis of giardiasis, and advances in the development of vaccines and drugs based on knowledge of virulence markers.

Recent findings: The use of transcriptomic and proteomic technologies as well as whole genome sequencing (WGS) from single cysts has allowed the assembly of the draft genome sequences for assemblages C and D of G. duodenalis. These findings, along with the published genomes for assemblages A, B, and E, have allowed comparative genomic investigations. In addition, the use of these methodologies for the characterization of the secretomes of trophozoite-epithelial cell interactions for assemblages A/B has led to the identification of virulence markers including energy metabolism enzymes, proteinases, high-cysteine membrane proteins (HCMPs), and variant surface proteins (VSPs). Recently, some drugs and vaccines, targeting virulence factors have been developed, offering possible alternatives to current treatment and prevention options against giardiasis.

Summary: Among the nine recognized species of Giardia, G. duodenalis stands out because of its broad spectrum of hosts and its socio-economic importance. This species comprises eight genetic assemblages (A to H), of which A and B are zoonotic, and the other assemblages have narrow host specificities. Assemblages A and B may be considered as the most virulent ones, but the existence of asymptomatic carriers and considerable genetic variability within and among these assemblages hampers the definition of common virulence factors. The attachment of Giardia trophozoites to epithelial cells and structural cytoskeleton components of the adhesive disk, such as giardins or tubulins, is proposed to play key roles, but toxins have not yet been precisely defined. However, recent transcriptomic and proteomic analyses of the secretomes of trophozoites representing assemblages A and B and interacting with particular epithelial cell lines have defined a series of virulence factors, including glycolytic (e.g., enolase) and arginolytic (e.g., arginine deiminase) enzymes, cysteine proteases (e.g., giardipain-1) and VSPs (e.g., VSP9B10A). Other factors, such as HCMPs and tenascins, have been consistently found to be excreted/secreted, but their role(s) in the pathogenesis of giardiasis has not yet been elucidated. Interestingly, recent investigations of single cysts representing assemblages C and D using advanced sequencing and informatic methods have suggested that the transcription/expression profiles of virulence factors vary both within and between assemblages, thus assemblage-specific molecules might allow adaptation to the microenvironment within the host. Importantly, some drugs active against cysteine-rich proteins of Giardia, including giardipain-1, VSPs and arginine deiminase, have been shown to be targeted by cysteine-modifying compounds as disulfiram, L-canavanin and allicin. On the other hand, VSPs are presently considered as key vaccine candidates because they induce protection against Giardia in rodents and dogs. Overall, this review reveals that much more work is needed to identify, characterize, and understand the roles of virulence factors in Giardia and to assess their validity as drug and vaccine targets. Clear, advanced omics and informatic tools should assist in this future endeavor, with a focus on targeting virulence factors that are common and/or unique to distinct assemblages to develop new and effective interventions against Giardia.

Abstract Image

十二指肠贾第虫毒力-“生存,还是毁灭”。
综述目的:本文综述了十二指肠贾第鞭毛虫组合的遗传特征及其与毒力关系的最新进展。我们还讨论了毒力因素在贾第虫病发病机制中的意义,以及基于毒力标记物的疫苗和药物开发的进展。最近发现:利用转录组学和蛋白质组学技术以及单囊全基因组测序(WGS),可以组装十二指肠螺杆菌C和D组合的草图基因组序列。这些发现,连同已发表的组合A、B和E的基因组,使比较基因组研究成为可能。此外,利用这些方法表征滋养体-上皮细胞A/B组合相互作用的分泌组,已经鉴定出包括能量代谢酶、蛋白酶、高半胱氨酸膜蛋白(HCMPs)和变异表面蛋白(VSPs)在内的毒力标记。最近,已经开发了一些针对毒力因子的药物和疫苗,为目前针对贾第虫病的治疗和预防方案提供了可能的替代方案。摘要:在已知的九种贾第虫中,十二指肠贾第虫因其广泛的寄主范围和社会经济重要性而脱颖而出。该物种包括8个遗传组合(A至H),其中A和B是人畜共患的,其他组合具有狭窄的宿主特异性。组合A和B可能被认为是最具毒性的组合,但这些组合内部和之间存在无症状携带者和相当大的遗传变异性阻碍了共同毒力因子的定义。贾第鞭毛虫滋养体附着于上皮细胞和粘附盘的结构细胞骨架成分,如贾第鞭毛虫或微管蛋白,被认为起关键作用,但毒素尚未得到精确定义。然而,最近对代表A和B组合并与特定上皮细胞系相互作用的滋养体分泌组的转录组学和蛋白质组学分析已经确定了一系列毒力因子,包括糖酵解(如烯醇酶)和精氨酸分解(如精氨酸脱亚胺酶)酶、半胱氨酸蛋白酶(如鞭毛虫痛-1)和vsp(如VSP9B10A)。其他因素,如HCMPs和tenascin,一直被发现是排泄/分泌的,但它们在贾第虫病发病机制中的作用尚未阐明。有趣的是,最近使用先进的测序和信息学方法对代表组合C和D的单个包囊进行的研究表明,毒力因子的转录/表达谱在组合内部和组合之间都是不同的,因此组合特异性分子可能允许适应宿主内的微环境。重要的是,一些对贾第鞭虫富含半胱氨酸的蛋白质有活性的药物,包括贾第鞭虫痛-1、VSPs和精氨酸脱亚胺酶,已被证明是半胱氨酸修饰化合物如双硫胺、l -大麻素和大蒜素的靶标。另一方面,vsp目前被认为是关键的候选疫苗,因为它们在啮齿动物和狗身上引起对贾第鞭毛虫的保护。总的来说,这篇综述表明,需要做更多的工作来识别、表征和理解贾第鞭毛虫毒力因子的作用,并评估它们作为药物和疫苗靶点的有效性。明确的、先进的组学和信息学工具应该有助于这一未来的努力,重点是针对不同组合的常见和/或独特的毒力因子,以开发针对贾第鞭毛虫的新的有效干预措施。
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
Current Tropical Medicine Reports
Current Tropical Medicine Reports Medicine-Infectious Diseases
CiteScore
9.30
自引率
1.90%
发文量
23
期刊介绍: Current Tropical Medicine Reports provides expert views on recent advances in the field of tropical medicine in a clear and readable form. This journal offers reviews by domestic and international contributors that highlight the most important, recent papers and findings related to this specific field. We accomplish this by appointing renowned leaders in major tropical medicine subject areas to select topics addressing virology, bacteriology, parasitology, entomology, immunology, cell and molecular biology, epidemiology, ecology, behavioral science and clinical medicine for review by experts who assess the latest developments and highlight significant papers published over the last few years on their topics. These review articles also stress recently published papers of importance in the references, which are accompanied by annotations explaining their importance. In addition to these Section Editors, our international Editorial Board ensures our journal upholds its standards.
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