In Utero Exposure to Caffeine and Acetaminophen, the Gut Microbiome, and Neurodevelopmental Outcomes: A Prospective Birth Cohort Study.

Pregnant individuals are exposed to acetaminophen and caffeine, but it is unknown how these exposures interact with the developing gut microbiome. We aimed to determine whether acetaminophen and/or caffeine relate to the childhood gut microbiome and whether features of the gut microbiome alter the relationship between acetaminophen/caffeine and neurodevelopment. Forty-nine and 85 participants provided meconium and stool samples at 6-7, respectively, for exposure and microbiome assessment. Fecal acetaminophen and caffeine concentrations were quantified, and fecal DNA underwent metagenomic sequencing. Caregivers and study staff assessed the participants' motor and cognitive development using standardized scales. Prenatal exposures had stronger associations with the childhood microbiome than concurrent exposures. Prenatal acetaminophen exposure was associated with a trend of lower gut bacterial diversity in childhood [ß = -0.17 Shannon Index, 95% CI: (-0.31, -0.04)] and was marginally associated with differences in the relative abundances of features of the gut microbiome at the phylum (Firmicutes, Actinobacteria) and gene pathway levels. Among the participants with a higher relative abundance of Proteobacteria, prenatal exposure to acetaminophen and caffeine was associated with lower scores on WISC-IV subscales. Acetaminophen during bacterial colonization of the naïve gut is associated with lasting alterations in childhood microbiome composition. Future studies may inform our understanding of downstream health effects.

Monitoring of prenatal exposure to organic and inorganic contaminants using meconium from an Eastern Canada cohort.

Evaluating in utero exposure to inorganic and multiclass organic contaminants is critical to better evaluate potential harmful effects on prenatal and postnatal development. The analysis of meconium, the first bowel discharge of the newborn, has been proposed as a non-invasive way to assess cumulative prenatal exposure. The aim of this study was to implement an analytical method for quantifying 72 targeted organic compounds, including pesticides, pharmaceutical compounds and daily life xenobiotics, in meconium in addition to selected elements (17 elements). We report initial monitoring results based on the analysis of 396 meconium samples from an Eastern Canada cohort (Quebec, Canada). Element contents in meconium were analysed by mass spectrometry after digestion in nitric acid and peroxide. Targeted organic compounds were extracted and purified from meconium samples by a solid-liquid extraction followed by a dispersive-SPE purification before tandem mass spectrometry analysis. Concentrations of targeted elements were within the range of concentration reported in European and US studies but were lower than concentrations found in a developing country cohort (i.e., Pb, Cd). Out of the 72 targeted organic compounds, 31 were detected at least once and 30 were quantified. Compounds with the highest frequency of detection were caffeine, detected in all samples (from 2.80 to 6186 ng g-1), followed by acetaminophen detected in 53% of the samples (up to ~402 µg g-1) and methyl paraben detected in 20% of the samples (up to ~10 µg g-1). Pesticides were detected in low frequencies (< 2%) and low concentration (< 35 ng g-1). Results show that meconium can be used to monitor prenatal exposure of foetus to a wide array of inorganic and organic contaminants.

Association Between Meconium Acetaminophen and Childhood Neurocognitive Development in GESTE, a Canadian Cohort Study.

Acetaminophen is the only over-the-counter pain reliever that is not contraindicated during pregnancy, but recent studies have questioned whether acetaminophen is safe for the fetus, particularly the developing brain. This prospective birth cohort study probed the previously observed association between in utero exposure to acetaminophen and neurodevelopment by using concentrations of acetaminophen measured in meconium, which more objectively captures exposure of the fetus than maternal report. Exposure, measured by liquid chromatography coupled with tandem mass spectrometry, was categorized into nondetection, low detection, and high detection levels. At age 6-8 years, children completed a set of subtests from the Wechsler Intelligence Scale for Children, 4th edition. Additionally, this study examined potential effect modification by child sex on the association between acetaminophen exposure and neurodevelopment. In fully adjusted models, in utero exposure to acetaminophen was not statistically significantly associated with decreased scores on any of the examined subtests in all children combined (n = 118). The effect of in utero acetaminophen exposure on the Coding subtest was marginally significantly different among boys and girls, with girls performing significantly better on the task with higher levels of acetaminophen compared with girls with undetectable levels of exposure (ßgirls, low = 2.83 [0.97, 4.70], ßgirls, high = 1.95 [-0.03, 3.93], ßboys, low = .02 [-1.78, 1.81], ßboys, high = -.39 [-2.09, 1.31], pinteraction = .06). Effect modification by child sex was not observed on other subtests. These results do not support prior reports of adverse neurodevelopmental effects of in utero exposure to acetaminophen.

Liquid chromatography-tandem mass spectrometry determination for multiclass pesticides from insect samples by microwave-assisted solvent extraction followed by a salt-out effect and micro-dispersion purification.

The effects of phyto-pharmaceutic compounds (PPCs), such as neonicotinoids, on wildlife reproduction and survival are a rising concern. Yet, understanding the biological consequences of PPC use is particularly complex given the large diversity of PPCs and their derivatives to which wildlife can be exposed. Here, we present a simple and sensitive method for the simultaneous detection and quantification of multiclass PPCs (54 molecules) in single insect boluses (<0.05 g dry mass) by ultra-high pressure liquid chromatography coupled to a tandem mass spectrometer (LC-MS/MS). A key part of this new method is the use of a two-step extraction method combining (i) the high efficiency of a microwave-assisted solvent extraction (MAE) for extracting analytes that might be tightly bound to environmental matrices and (ii) the versatility of a salt-out effect adapted from the QuEChERS methodology allowing the extraction and purification of a wide array of analytes. This microwave-assisted salt-out extraction (MASOE) approach was compared to classical extraction methods including matrix solid phase dispersion (MSPD), microwave-assisted extraction (MAE), and the QuEChERS method. Average recoveries for 54 analytes ranged from 49% to 106%, (relative standard deviations <22%). The limits of detection (LODs) and quantification (LOQs) were in the ranges of 0.10-3.00 ng g(-1) and 0.40-7.00 ng g(-1), respectively. We applied this method to analyse 881 insect boluses collected from Tree Swallow (Tachycineta bicolour) nestlings along an agricultural intensification gradient in southern Québec (Canada). We detected 25 PPCs out of the 54 considered. We detected at least one PPC in 30% of samples and were able to quantify at least one of them in 17% of samples. Our study shows that the MASOE method should prove to be a powerful tool for studying the fate and impacts of PPCs on wildlife.