4-Ethylphenol-fluxes, metabolism and excretion of a gut microbiome derived neuromodulator implicated in autism

Francesca Day; Justin O'Sullivan; Chris Pook

doi:10.3389/fmolb.2023.1267754

4-Ethylphenol-fluxes, metabolism and excretion of a gut microbiome derived neuromodulator implicated in autism

Front Mol Biosci. 2023 Oct 12:10:1267754. doi: 10.3389/fmolb.2023.1267754. eCollection 2023.

Authors

Francesca Day¹, Justin O'Sullivan^{1

2

3

4

5}, Chris Pook¹

Affiliations

¹ Liggins Institute, Waipapa Taumata Rau-The University of Auckland, Auckland, New Zealand.
² The Maurice Wilkins Centre, The University of Auckland, Auckland, New Zealand.
³ MRC Lifecourse Epidemiology Unit, University of Southampton, Southampton, United Kingdom.
⁴ Australian Parkinson's Mission, Garvan Institute of Medical Research, Sydney, NSW, Australia.
⁵ A*STAR Singapore Institute for Clinical Sciences, Singapore, Singapore.

Abstract

Gut-microbiome-derived metabolites, such as 4-Ethylphenol [4EP], have been shown to modulate neurological health and function. Although the source of such metabolites is becoming better understood, knowledge gaps remain as to the mechanisms by which they enter host circulation, how they are transported in the body, how they are metabolised and excreted, and the way they exert their effects. High blood concentrations of host-modified 4EP, 4-ethylphenol sulfate [4EPS], are associated with an anxiety phenotype in autistic individuals. We have reviewed the existing literature and discuss mechanisms that are proposed to contribute influx from the gut microbiome, metabolism, and excretion of 4EP. We note that increased intestinal permeability is common in autistic individuals, potentially explaining increased flux of 4EP and/or 4EPS across the gut epithelium and the Blood Brain Barrier [BBB]. Similarly, kidney dysfunction, another complication observed in autistic individuals, impacts clearance of 4EP and its derivatives from circulation. Evidence indicates that accumulation of 4EPS in the brain of mice affects connectivity between subregions, particularly those linked to anxiety. However, we found no data on the presence or quantity of 4EP and/or 4EPS in human brains, irrespective of neurological status, likely due to challenges sampling this organ. We argue that the penetrative ability of 4EP is dependent on its form at the BBB and its physicochemical similarity to endogenous metabolites with dedicated active transport mechanisms across the BBB. We conclude that future research should focus on physical (e.g., ingestion of sorbents) or metabolic mechanisms (e.g., conversion to 4EP-glucuronide) that are capable of being used as interventions to reduce the flux of 4EP from the gut into the body, increase the efflux of 4EP and/or 4EPS from the brain, or increase excretion from the kidneys as a means of addressing the neurological impacts of 4EP.

Keywords: 4-ethylphenol; 4-ethylphenol sulfate; autism; gut microbiome; host microbiome modulation; membrane integrity; neuromodulators; uremic toxins.

Publication types

Review

Grants and funding

The author(s) declare financial support was received for the research, authorship, and/or publication of this article. FD was funded by the UoA Scholarship. CP Fellowship was funded by a donation from Shundi Group.