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基于 LCMS 的代谢组学和脂质组学方法鉴定人类钩虫感染期的小分子。

Identification of Small Molecules of the Infective Stage of Human Hookworm Using LCMS-Based Metabolomics and Lipidomics Protocols.

机构信息

Centre for Molecular Therapeutics, Australian Institute of Tropical Health and Medicine, James Cook University, Building E4, McGregor Road, Smithfield, Cairns, Queensland 4878, Australia.

Monash Institute of Pharmaceutical Sciences, Monash University, Royal Parade, Parkville, Victoria 3052, Australia.

出版信息

ACS Infect Dis. 2021 Dec 10;7(12):3264-3276. doi: 10.1021/acsinfecdis.1c00428. Epub 2021 Nov 12.

Abstract

Hookworm infections affect millions of people worldwide and are responsible for impaired mental and physical growth in children, and anemias. There is no vaccine, and increasing anthelmintic drug resistance in nematodes of domestic animals, and reduced drug cure rates in nematode infections of humans is alarming. Despite this looming health problem, there is a significant knowledge gap in terms of nonproteinaceous "excretory/secretory products" (ESPs) and how they orchestrate a parasitic existence. In the current study, we have conducted the first metabolomic and lipidomic analysis of the infective third-stage filariform larvae (L3) of the predominant human hookworm using liquid chromatography-mass spectrometry. Altogether, we have identified a total of 645 small molecules that were mainly produced through amino acid and glycerophospholipid metabolism. Putatively, 495 metabolites were unique to the somatic tissue extract, and 34 metabolites were present only in the ESP component. More than 21 novel mass features with nitrogen and sulfur functional groups were detected in the ESP component for the first time from helminths. While this study could not establish the biological functions of the metabolites identified, literature searches revealed that these metabolites possess various biological properties, including anti-inflammatory activities. These metabolites are likely used by the parasite upon exposure to a host to facilitate skin penetration, passage through different tissues, and immune regulation in the small bowel. Overall, the results presented herein offer significant insight into the metabolome of L3 and have the potential to instigate future work to establish biomarkers of infection. This area urgently needs attention, given the lack of sensitive point-of-care diagnostic tools.

摘要

钩虫感染影响着全球数百万人,导致儿童智力和身体发育受损以及贫血。目前尚无疫苗,家畜线虫的驱虫药物耐药性不断增加,人类线虫感染的药物治愈率下降,令人震惊。尽管存在这种迫在眉睫的健康问题,但对于非蛋白“排泄/分泌产物”(ESP)及其如何协调寄生生存方式,仍存在着显著的知识空白。在目前的研究中,我们首次对主要的人体钩虫的感染性第三期丝状幼虫(L3)进行了代谢组学和脂质组学分析,采用液相色谱-质谱法。总共鉴定出了 645 种小分子,这些小分子主要通过氨基酸和甘油磷脂代谢产生。推测 495 种代谢物是体细胞组织提取物所特有的,而 34 种代谢物仅存在于 ESP 成分中。在 ESP 成分中,首次从蠕虫中检测到超过 21 种具有氮和硫官能团的新型质量特征。虽然本研究尚不能确定所鉴定代谢物的生物学功能,但文献检索表明,这些代谢物具有多种生物学特性,包括抗炎活性。这些代谢物可能在寄生虫暴露于宿主时被寄生虫利用,以促进皮肤穿透、通过不同组织以及在小肠中的免疫调节。总的来说,本研究结果为 L3 的代谢组学提供了重要的见解,并有可能引发未来的工作,以确定感染的生物标志物。鉴于缺乏敏感的即时诊断工具,这一领域急需关注。

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