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在感染的早期阶段,克氏锥虫会在其载体丽蝇的前中肠内重新编程线粒体代谢。

Trypanosoma cruzi reprograms mitochondrial metabolism within the anterior midgut of its vector Rhodnius prolixus during the early stages of infection.

机构信息

Laboratory of Vector-Pathogen Biology, Proteomic Platform, Department of Molecular Biology, Université Libre de Bruxelles, 6041, Gosselies, Belgium.

Institute of Medical Biochemistry Leopoldo de Meis, Centro de Ciências e da Saúde, Federal University of Rio de Janeiro, Rio de Janeiro, 21941-902, Brazil.

出版信息

Parasit Vectors. 2024 Sep 6;17(1):381. doi: 10.1186/s13071-024-06415-1.

Abstract

BACKGROUND

Trypanosoma cruzi is transmitted to humans by hematophagous bugs belonging to the Triatominae subfamily. Its intra-vectorial cycle is complex and occurs exclusively in the insect's midgut. Dissecting the elements involved in the cross-talk between the parasite and its vector within the digestive tract should provide novel targets for interrupting the parasitic life cycle and affecting vectorial competence. These interactions are shaped by the strategies that parasites use to infect and exploit their hosts, and the host's responses that are designed to detect and eliminate parasites. The objective of the current study is to characterize the impact of T. cruzi establishment within its vector on the dynamics of its midgut.

METHODS

In this study, we evaluated the impact of T. cruzi infection on protein expression within the anterior midgut of the model insect Rhodnius prolixus at 6 and 24 h post-infection (hpi) using high-throughput quantitative proteomics.

RESULTS

Shortly after its ingestion, the parasite modulates the proteome of the digestive epithelium by upregulating 218 proteins and negatively affecting the expression of 11 proteins involved in a wide array of cellular functions, many of which are pivotal due to their instrumental roles in cellular metabolism and homeostasis. This swift response underscores the intricate manipulation of the vector's cellular machinery by the parasite. Moreover, a more in-depth analysis of proteins immediately induced by the parasite reveals a pronounced predominance of mitochondrial proteins, thereby altering the sub-proteomic landscape of this organelle. This includes various complexes of the respiratory chain involved in ATP generation. In addition to mitochondrial metabolic dysregulation, a significant number of detoxifying proteins, such as antioxidant enzymes and P450 cytochromes, were immediately induced by the parasite, highlighting a stress response.

CONCLUSIONS

This study is the first to illustrate the response of the digestive epithelium upon contact with T. cruzi, as well as the alteration of mitochondrial sub-proteome by the parasite. This manipulation of the vector's physiology is attributable to the cascade activation of a signaling pathway by the parasite. Understanding the elements of this response, as well as its triggers, could be the foundation for innovative strategies to control the transmission of American trypanosomiasis, such as the development of targeted interventions aimed at disrupting parasite proliferation and transmission within the triatomine vector.

摘要

背景

克氏锥虫通过属于锥蝽亚科的吸血昆虫传播给人类。其在媒介内的周期很复杂,只发生在昆虫的中肠。解析寄生虫与其在消化道内的媒介之间的串扰涉及的元素,应为阻断寄生虫生命周期和影响媒介能力提供新的靶点。这些相互作用是由寄生虫用来感染和利用宿主的策略以及宿主旨在检测和消除寄生虫的反应形成的。本研究的目的是描述克氏锥虫在其媒介体内建立对其中肠动态的影响。

方法

在这项研究中,我们使用高通量定量蛋白质组学评估了在感染后 6 和 24 小时(hpi)时,克氏锥虫感染对模型昆虫 Rhodnius prolixus 前中肠内蛋白质表达的影响。

结果

在摄入后不久,寄生虫通过上调 218 种蛋白质并下调 11 种参与广泛细胞功能的蛋白质的表达来调节消化上皮的蛋白质组,其中许多蛋白质因其在细胞代谢和动态平衡中的重要作用而至关重要。这种快速反应突显了寄生虫对媒介细胞机制的复杂操纵。此外,对寄生虫立即诱导的蛋白质进行更深入的分析表明,线粒体蛋白质明显占主导地位,从而改变了该细胞器的亚蛋白质组景观。这包括参与 ATP 生成的呼吸链的各种复合物。除了线粒体代谢失调外,寄生虫还立即诱导了大量解毒蛋白,如抗氧化酶和 P450 细胞色素,从而强调了应激反应。

结论

本研究首次说明了接触克氏锥虫时消化上皮的反应以及寄生虫对线粒体亚蛋白质组的改变。这种对媒介生理学的操纵归因于寄生虫激活信号通路的级联反应。了解这种反应的元素及其触发因素可能为控制美洲锥虫病的传播提供创新策略的基础,例如开发旨在破坏寄生虫在三锥虫媒介内增殖和传播的靶向干预措施。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fb4d/11380418/6a9638767495/13071_2024_6415_Fig1_HTML.jpg

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