4.7 Article

Queuine Is a Nutritional Regulator of Entamoeba histolytica Response to Oxidative Stress and a Virulence Attenuator

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MBIO
卷 12, 期 2, 页码 -

出版社

AMER SOC MICROBIOLOGY
DOI: 10.1128/mBio.03549-20

关键词

Entamoeba histolytica; oxidative stress; tRNA modification; virulence

资金

  1. Israel Ministry of Health within the framework European Research Area NETwork Infect-ERA (AMOEBAC project) [031L0004]
  2. Israel Science Foundation [260/16]
  3. ISF-NRF program [3208/19]
  4. National Research Foundation of Singapore through the Singapore-MIT Alliance for Research and Technology Antimicrobial Resistance IRG
  5. Rappaport Institute
  6. US-Israel Binational Science Foundation [2015211]
  7. Niedersachsen program

向作者/读者索取更多资源

Queuine has a dual role in promoting oxidative stress resistance and reducing virulence in the eukaryotic parasite Entamoeba histolytica. It is efficiently incorporated into the parasite's tRNAs and stimulates methylation, leading to protection against oxidative stress and downregulation of virulence-associated genes. Silencing of EhTGT prevents queuine incorporation, impairing parasite growth, oxidative stress resistance, and cytopathic activity.
Queuosine is a naturally occurring modified ribonucleoside found in the first position of the anticodon of the transfer RNAs for Asp, Asn, His, and Tyr. Eukaryotes lack pathways to synthesize queuine, the nucleobase precursor to queuosine, and must obtain it from diet or gut microbiota. Here, we describe the effects of queuine on the physiology of the eukaryotic parasite Entamoeba histolytica, the causative agent of amebic dysentery. Queuine is efficiently incorporated into E. histolytica tRNAs by a tRNA-guanine transglycosylase (EhTGT) and this incorporation stimulates the methylation of C38 in tRNA(GUC)(Asp). Queuine protects the parasite against oxidative stress (OS) and antagonizes the negative effect that oxidation has on translation by inducing the expression of genes involved in the OS response, such as heat shock protein 70 (Hsp70), antioxidant enzymes, and enzymes involved in DNA repair. On the other hand, queuine impairs E. histolytica virulence by downregulating the expression of genes previously associated with virulence, including cysteine proteases, cytoskeletal proteins, and small GTPases. Silencing of EhTGT prevents incorporation of queuine into tRNAs and strongly impairs methylation of C38 in tRNA(GUC)(Asp), parasite growth, resistance to OS, and cytopathic activity. Overall, our data reveal that queuine plays a dual role in promoting OS resistance and reducing parasite virulence. IMPORTANCE Entamoeba histolytica is a unicellular parasite that causes amebiasis. The parasite resides in the colon and feeds on the colonic microbiota. The gut flora is implicated in the onset of symptomatic amebiasis due to alterations in the composition of bacteria. These bacteria modulate the physiology of the parasite and affect the virulence of the parasite through unknown mechanisms. Queuine, a modified nucleobase of queuosine, is exclusively produced by the gut bacteria and leads to tRNA modification at the anticodon loops of specific tRNAs. We found that queuine induces mild oxidative stress resistance in the parasite and attenuates its virulence. Our study highlights the importance of bacterially derived products in shaping the physiology of the parasite. The fact that queuine inhibits the virulence of E. histolytica may lead to new strategies for preventing and/or treating amebiasis by providing to the host queuine directly or via probiotics.

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