The queen's gut refines with age: longevity phenotypes in a social insect model.
Author
Anderson, Kirk ERicigliano, Vincent A
Mott, Brendon M
Copeland, Duan C
Floyd, Amy S
Maes, Patrick
Affiliation
Univ Arizona, Sch Anim & Comparat Biomed Sci, Dept MicrobiolUniv Arizona, Dept Entomol
Univ Arizona, Ctr Insect Sci
Issue Date
2018-06-18Keywords
AcetobacteracaeaeAging
Bacteria
Bifidobacterium
Core microbiota
Honey bees
Ileum
Lactobacillus kunkeei
Oxidative stress
Parasaccharibacter apium
Metadata
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BIOMED CENTRAL LTDCitation
Anderson, K. E. et al. The queen’s gut refines with age: longevity phenotypes in a social insect model. Microbiome 6, 287 (2018).Journal
MICROBIOMERights
© The Author(s). 2018. This article is distributed under the terms of the Creative Commons Attribution 4.0 International License.Collection Information
This item from the UA Faculty Publications collection is made available by the University of Arizona with support from the University of Arizona Libraries. If you have questions, please contact us at repository@u.library.arizona.edu.Abstract
In social insects, identical genotypes can show extreme lifespan variation providing a unique perspective on age-associated microbial succession. In honey bees, short- and long-lived host phenotypes are polarized by a suite of age-associated factors including hormones, nutrition, immune senescence, and oxidative stress. Similar to other model organisms, the aging gut microbiota of short-lived (worker) honey bees accrue Proteobacteria and are depleted of Lactobacillus and Bifidobacterium, consistent with a suite of host senescence markers. In contrast, long-lived (queen) honey bees maintain youthful cellular function with much lower expression of oxidative stress genes, suggesting a very different host environment for age-associated microbial succession. We sequenced the microbiota of 63 honey bee queens exploring two chronological ages and four alimentary tract niches. To control for genetic and environmental variation, we quantified carbonyl accumulation in queen fat body tissue as a proxy for biological aging. We compared our results to the age-specific microbial succession of worker guts. Accounting for queen source variation, two or more bacterial species per niche differed significantly by queen age. Biological aging in queens was correlated with microbiota composition highlighting the relationship of microbiota with oxidative stress. Queens and workers shared many major gut bacterial species, but differ markedly in community structure and age succession. In stark contrast to aging workers, carbonyl accumulation in queens was significantly associated with increased Lactobacillus and Bifidobacterium and depletion of various Proteobacteria. We present a model system linking changes in gut microbiota to diet and longevity, two of the most confounding variables in human microbiota research. The pattern of age-associated succession in the queen microbiota is largely the reverse of that demonstrated for workers. The guts of short-lived worker phenotypes are progressively dominated by three major Proteobacteria, but these same species were sparse or significantly depleted in long-lived queen phenotypes. More broadly, age-related changes in the honey bee microbiota reflect the regulatory anatomy of reproductive host metabolism. Our synthesis suggests that the evolution of colony-level reproductive physiology formed the context for host-microbial interactions and age-related succession of honey bee microbiota.ISSN
2049-2618PubMed ID
29914555Version
Final published versionSponsors
ARS-USDA [501-2022-050 017]ae974a485f413a2113503eed53cd6c53
10.1186/s40168-018-0489-1
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Except where otherwise noted, this item's license is described as © The Author(s). 2018. This article is distributed under the terms of the Creative Commons Attribution 4.0 International License.
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