Maternal Western diet exposure increases periportal fibrosis beginning in utero in nonhuman primate offspring
Michael J. Nash, … , Jacob E. Friedman, Stephanie R. Wesolowski
Michael J. Nash, … , Jacob E. Friedman, Stephanie R. Wesolowski
Published December 22, 2021
Citation Information: JCI Insight. 2021;6(24):e154093. https://doi.org/10.1172/jci.insight.154093.
View: Text | PDF
Research Article Gastroenterology

Maternal Western diet exposure increases periportal fibrosis beginning in utero in nonhuman primate offspring

Abstract

Maternal obesity affects nearly one-third of pregnancies and is a major risk factor for nonalcoholic fatty liver disease (NAFLD) in adolescent offspring, yet the mechanisms behind NAFLD remain poorly understood. Here, we demonstrate that nonhuman primate fetuses exposed to maternal Western-style diet (WSD) displayed increased fibrillar collagen deposition in the liver periportal region, with increased ACTA2 and TIMP1 staining, indicating localized hepatic stellate cell (HSC) and myofibroblast activation. This collagen deposition pattern persisted in 1-year-old offspring, despite weaning to a control diet (CD). Maternal WSD exposure increased the frequency of DCs and reduced memory CD4+ T cells in fetal liver without affecting systemic or hepatic inflammatory cytokines. Switching obese dams from WSD to CD before conception or supplementation of the WSD with resveratrol decreased fetal hepatic collagen deposition and reduced markers of portal triad fibrosis, oxidative stress, and fetal hypoxemia. These results demonstrate that HSCs and myofibroblasts are sensitive to maternal WSD-associated oxidative stress in the fetal liver, which is accompanied by increased periportal collagen deposition, indicative of early fibrogenesis beginning in utero. Alleviating maternal WSD-driven oxidative stress in the fetal liver holds promise for halting steatosis and fibrosis and preventing developmental programming of NAFLD.

Authors

Michael J. Nash, Evgenia Dobrinskikh, Sean A. Newsom, Ilhem Messaoudi, Rachel C. Janssen, Kjersti M. Aagaard, Carrie E. McCurdy, Maureen Gannon, Paul Kievit, Jacob E. Friedman, Stephanie R. Wesolowski

×

Figure 2

Evidence for increased collagen synthesis and stellate cell activation in NHP WSD-exposed fetal liver.

Options: View larger image (or click on image) Download as PowerPoint
Evidence for increased collagen synthesis and stellate cell activation i...
Expression of genes in CD (blue) and WSD (yellow) fetal liver tissue associated with collagen synthesis and stellate cell activation (A). ANOVA with fixed effect for maternal diet is significant for all variables shown (P < 0.1). Individual post test comparisons were performed between CD and WSD; n = 20 CD and n = 26 WSD. *P < 0.05. (B) Expression of genes associated with endothelial dysfunction, the YAP/TAZ pathway, and myeloid cell inflammation; n = 20 CD and n = 26 WSD. (C) Representative images and zooms of portal triads of CD- and WSD-exposed fetal livers via RNAscope. Red arrows indicate ACTA2+ cells; blue arrows indicate TIMP1+ cells; purple arrows indicate ACTA2 and TIMP1 double-positive cells. Scale bar: 60 μm (boxed areas are enlarged and cropped on the right). Average numbers of ACTA2+ cells (D), TIMP1+ cells (E), and ACTA2 and TIMP1 double-positive cells (F) per portal triad (PT) via RNAscope; n = 6 CD and n = 5 WSD. Unpaired 2-tailed Student’s t test was used to test significance. *P < 0.05, **P < 0.005, ****P < 0.0005.