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人对氧磷酶 1 的表达降低了超氧化物水平,并改变了果蝇肠道中的细菌定植。

Expression of human paraoxonase 1 decreases superoxide levels and alters bacterial colonization in the gut of Drosophila melanogaster.

机构信息

Department of Internal Medicine, Carver College of Medicine, University of Iowa, Iowa City, Iowa, United States of America.

出版信息

PLoS One. 2012;7(8):e43777. doi: 10.1371/journal.pone.0043777. Epub 2012 Aug 30.

Abstract

Paraoxonases (PON) are a family of proteins (PON1, 2 and 3) with multiple enzymatic activities. PON1 interferes with homoserine lactone-mediated quorum sensing in bacteria and with reactive oxygen species (ROS) in humans and mice. PON1 gene mutations have been linked to multiple traits, including aging, and diseases of the cardiovascular, nervous and gastrointestinal system. The overlapping enzymatic activities in the PON family members and high linkage disequilibrium rates within their polymorphisms confound animal and human studies of PON1 function. In contrast, arthropods such as Drosophila melanogaster have no PON homologs, resulting in an ideal model to study interactions between PON genotype and host phenotypes. We hypothesized that expression of PON1 in D. melanogaster would alter ROS. We found that PON1 alters expression of multiple oxidative stress genes and decreases superoxide anion levels in normal and germ-free D. melanogaster. We also found differences in the composition of the gut microbiota, with a remarkable increase in levels of Lactobacillus plantarum and associated changes in expression of antimicrobial and cuticle-related genes. PON1 expression directly decreased superoxide anion levels and altered bacterial colonization of the gut and its gene expression profile, highlighting the complex nature of the interaction between host genotype and gut microbiota. We speculate that the interaction between some genotypes and human diseases may be mediated by the presence of certain gut bacteria that can induce specific immune responses in the gut and other host tissues.

摘要

对氧磷酶(PON)是具有多种酶活性的蛋白质家族(PON1、2 和 3)。PON1 干扰细菌中的同型半胱氨酸内酯介导的群体感应和人类及小鼠中的活性氧(ROS)。PON1 基因突变与多种特征相关,包括衰老以及心血管、神经和胃肠道系统疾病。PON 家族成员的重叠酶活性和其多态性中的高连锁不平衡率使 PON1 功能的动物和人类研究变得复杂。相比之下,像黑腹果蝇这样的节肢动物没有 PON 同源物,这使其成为研究 PON 基因型与宿主表型之间相互作用的理想模型。我们假设 PON1 在黑腹果蝇中的表达会改变 ROS。我们发现 PON1 改变了正常和无菌黑腹果蝇中多种氧化应激基因的表达,并降低了超氧阴离子水平。我们还发现肠道微生物组的组成存在差异,植物乳杆菌的水平显著增加,抗菌和角质层相关基因的表达也发生了变化。PON1 的表达直接降低了超氧阴离子水平,并改变了肠道的细菌定植及其基因表达谱,突出了宿主基因型和肠道微生物组之间相互作用的复杂性。我们推测,某些基因型与人类疾病之间的相互作用可能是由某些肠道细菌引起的,这些细菌可以在肠道和其他宿主组织中引发特定的免疫反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c50f/3431398/9a4e5b47dbbf/pone.0043777.g001.jpg

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