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Costs of molecular adaptation to the chemical exposome: a focus on xenobiotic metabolism pathways

Philosophical Transactions of the Royal Society B Biological Sciences 2024 11 citations ? Citation count from OpenAlex, updated daily. May differ slightly from the publisher's own count. Score: 60 ? 0–100 AI score estimating relevance to the microplastics field. Papers below 30 are filtered from public browse.
Xavier Coumoul, Céline Tomkiewicz, Céline Tomkiewicz, Xavier Coumoul, Xavier Coumoul, Pierre Nioche, Robert Barouki, Étienne Blanc Xavier Coumoul, Xavier Coumoul, Étienne Blanc

Summary

This review examines how the human body processes foreign chemicals through specialized metabolic pathways, and how the sheer number of chemicals we are exposed to can overwhelm these defense systems. The pathways designed to detoxify harmful substances can generate toxic byproducts when they are overloaded or when multiple chemicals compete for the same enzymes. This is relevant to microplastics because they carry absorbed chemicals into the body, adding to the overall chemical burden that these metabolic pathways must handle.

Body Systems

Organisms adapt to their environment through different pathways. In vertebrates, xenobiotics are detected, metabolized and eliminated through the inducible xenobiotic-metabolizing pathways (XMP) which can also generate reactive toxic intermediates. In this review, we will discuss the impacts of the chemical exposome complexity on the balance between detoxication and side effects. There is a large discrepancy between the limited number of proteins involved in these pathways (few dozens) and the diversity and complexity of the chemical exposome (tens of thousands of chemicals). Several XMP proteins have a low specificity which allows them to bind and/or metabolize a large number of chemicals. This leads to undesired consequences, such as cross-inhibition, inefficient metabolism, release of toxic intermediates, etc. Furthermore, several XMP proteins have endogenous functions that may be disrupted upon exposure to exogenous chemicals. The gut microbiome produces a very large number of metabolites that enter the body and are part of the chemical exposome. It can metabolize xenobiotics and either eliminate them or lead to toxic derivatives. The complex interactions between chemicals of different origins will be illustrated by the diverse roles of the aryl hydrocarbon receptor which binds and transduces the signals of a large number of xenobiotics, microbiome metabolites, dietary chemicals and endogenous compounds. This article is part of the theme issue 'Endocrine responses to environmental variation: conceptual approaches and recent developments'.

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