Sex-Dependent Effects on Liver Inflammation and Gut Microbial Dysbiosis After Continuous Developmental Exposure to Trichloroethylene in Autoimmune-Prone Mice.

Sarah J Blossom,Kuppan Gokulan,Sangeeta Khare,Matthew Arnold

doi:10.3389/fphar.2020.569008

Abstract

Trichloroethylene (TCE) is a common environmental toxicant linked with hypersensitivity and autoimmune responses in humans and animal models. While autoimmune diseases are more common in females, mechanisms behind this disparity are not clear. Recent evidence suggests that autoimmunity may be increasing in males, and occupational studies have shown that TCE-mediated hypersensitivity responses occur just as often in males. Previous experimental studies in autoimmune-prone MRL+/+ mice have focused on responses in females. However, it is important to include both males and females in order to better understand sex-disparity in autoimmune disease. In addition, because of an alarming increase in autoimmunity in adolescents, developmental and/or early life exposures to immune-enhancing environmental pollutants should also be considered. Using MRL+/+ mice, we hypothesized that TCE would alter markers related to autoimmunity to a greater degree in female mice relative to male mice, and that TCE would enhance these effects. Mice were continuously exposed to either TCE or vehicle beginning at gestation, continuing during lactation, and directly in the drinking water. Both male and female offspring were evaluated at 7 weeks of age. Sex-specific effects were evident. Female mice were more likely than males to show enhanced CD4+ T cell cytokine responses (e.g., IL-4 and IFN-γ). Although none of the animals developed pathological or serological signs of autoimmune hepatitis-like disease, TCE-exposed female mice were more likely than males in either group to express higher levels of biomarkers in the liver related to regeneration/repair and proliferation. Levels of bacterial populations in the intestinal ileum were also altered by TCE exposure and were more prominent in females as compared to males. Thus, our expectations were correct in that young adult female mice developmentally exposed to TCE were more likely to exhibit alterations in immunological and gut/liver endpoints compared to male mice.

Highlights

Trichloroethylene (TCE) is a halocarbon best known for its use as an industrial solvent
The dose of TCE that was selected for the current study has been shown to induce autoimmune hepatitis (AIH)-like tissue pathology as well as early signs of liver inflammation in older adult mice after both adult-only and developmental exposure (Gilbert et al, 2009)
Statistically significant body weight differences were detected when mice were weaned at postnatal day 21 (PND21) (Figure 2)

Summary

Introduction

Trichloroethylene (TCE) is a halocarbon best known for its use as an industrial solvent. TCE is among the most frequently detected US EPA-regulated drinking water contaminants found in 4.5% of groundwater and 15% of surface water sources (ATSDR, 2014). TCE’s effects on human health have been studied extensively. TCE was classified as a human carcinogen (Guha et al, 2012). Among the myriad non-cancer outcomes associated with TCE exposure in humans is immunotoxicity. Chronic TCE exposure has been linked to autoimmune diseases including lupus, scleroderma, and autoimmune hepatitis (AIH) (Cooper et al, 2009; Parks and De Roos, 2014; Zhao et al, 2016)

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