Molecular and Metabolic Analysis of Arsenic-Exposed Humanized AS3MT Mice

Jenna Todero; Christelle Douillet; Alexandria J Shumway; Beverly H Koller; Matt Kanke; Daryl J Phuong; Miroslav Stýblo; Praveen Sethupathy

doi:10.1289/EHP12785

Molecular and Metabolic Analysis of Arsenic-Exposed Humanized AS3MT Mice

Environ Health Perspect. 2023 Dec;131(12):127021. doi: 10.1289/EHP12785. Epub 2023 Dec 27.

Authors

Jenna Todero¹, Christelle Douillet², Alexandria J Shumway¹, Beverly H Koller³, Matt Kanke¹, Daryl J Phuong¹, Miroslav Stýblo², Praveen Sethupathy¹

Affiliations

¹ Department of Biomedical Sciences, College of Veterinary Medicine, Cornell University, Ithaca, New York, USA.
² Department of Nutrition, Gillings School of Global Public Health, University of North Carolina, Chapel Hill, North Carolina, USA.
³ Department of Genetics, School of Medicine, University of North Carolina, Chapel Hill, North Carolina, USA.

Abstract

Background: Chronic exposure to inorganic arsenic (iAs) has been associated with type 2 diabetes (T2D). However, potential sex divergence and the underlying mechanisms remain understudied. iAs is not metabolized uniformly across species, which is a limitation of typical exposure studies in rodent models. The development of a new "humanized" mouse model overcomes this limitation. In this study, we leveraged this model to study sex differences in the context of iAs exposure.

Objectives: The aim of this study was to determine if males and females exhibit different liver and adipose molecular profiles and metabolic phenotypes in the context of iAs exposure.

Methods: Our study was performed on wild-type (WT) 129S6/SvEvTac and humanized arsenic $+ 3$ methyl transferase (human AS3MT) 129S6/SvEvTac mice treated with $400 ppb$ of iAs via drinking water ad libitum. After 1 month, mice were sacrificed and the liver and gonadal adipose depots were harvested for iAs quantification and sequencing-based microRNA and gene expression analysis. Serum blood was collected for fasting blood glucose, fasting plasma insulin, and homeostatic model assessment for insulin resistance (HOMA-IR).

Results: We detected sex divergence in liver and adipose markers of diabetes (e.g., miR-34a, insulin signaling pathways, fasting blood glucose, fasting plasma insulin, and HOMA-IR) only in humanized (not WT) mice. In humanized female mice, numerous genes that promote insulin sensitivity and glucose tolerance in both the liver and adipose are elevated compared to humanized male mice. We also identified Klf11 as a putative master regulator of the sex divergence in gene expression in humanized mice.

Discussion: Our study underscored the importance of future studies leveraging the humanized mouse model to study iAs-associated metabolic disease. The findings suggested that humanized males are at increased risk for metabolic dysfunction relative to humanized females in the context of iAs exposure. Future investigations should focus on the detailed mechanisms that underlie the sex divergence. https://doi.org/10.1289/EHP12785.

MeSH terms

Animals
Arsenic* / analysis
Arsenicals*
Blood Glucose / analysis
Diabetes Mellitus, Type 2* / chemically induced
Female
Humans
Insulin
Insulin Resistance*
Male
Methyltransferases / genetics
Mice
Obesity

Substances

Arsenic
Blood Glucose
Arsenicals
Insulin
AS3MT protein, human
Methyltransferases
AS3MT protein, mouse

Grants and funding

P42 ES031007/ES/NIEHS NIH HHS/United States