The organotin triphenyltin disrupts cholesterol signaling in mammalian ovarian steroidogenic cells through a combination of LXR and RXR modulation

Yong Pu; Elvis Ticiani; Sarah Pearl; Denny Martin; Almudena Veiga-Lopez

doi:10.1016/j.taap.2022.116209

The organotin triphenyltin disrupts cholesterol signaling in mammalian ovarian steroidogenic cells through a combination of LXR and RXR modulation

Toxicol Appl Pharmacol. 2022 Oct 15:453:116209. doi: 10.1016/j.taap.2022.116209. Epub 2022 Aug 23.

Authors

Yong Pu¹, Elvis Ticiani¹, Sarah Pearl², Denny Martin², Almudena Veiga-Lopez³

Affiliations

¹ Department of Pathology, University of Illinois at Chicago, IL, USA.
² Department of Obstetrics and Gynecology, Sparrow Health System, Lansing, MI, USA.
³ Department of Pathology, University of Illinois at Chicago, IL, USA; The Chicago Center for Health and Environment, University of Illinois at Chicago, Chicago, IL, USA. Electronic address: veiga@uic.edu.

Abstract

Organotins, a chemical family with over 30 congeners to which humans are directly exposed to through food consumption, are a chemical class widely used as stabilizers in polyvinyl chloride, and biocides in antifouling products. Aside from tributyltin (TBT), toxicological information on other organotin congeners, such as triphenyltin (TPT), remains scarce. Our previous work has demonstrated that TBT can interfere with cholesterol trafficking in steroidogenic cells. Given their structural similarities, we hypothesized that TPT, similar to TBT, disrupts intracellular cholesterol transport and impairs steroidogenesis in ovarian theca cells. To test this, human and ovine primary ovarian theca cells were isolated, purified and exposed to TPT at environmentally relevant doses (1 or 10 ng/ml) in pre-luteinized (48 h exposure) or luteinizing cells (72 h exposure). Intracellular cholesterol levels, progesterone, and testosterone secretion and gene expression of nuclear receptors, cholesterol transporters, and steroidogenic enzymes were evaluated. In ovine cells, TPT upregulated StAR, ABCA1, and SREBF1 mRNA and ABCA1 protein in both pre-luteinized and luteinized stages. TPT did not alter intracellular cholesterol or testosterone synthesis, but upregulated progesterone production. Inhibitor and shRNA knockdown approaches were then used to evaluate the role of retinoid X receptor (RXR) and liver X receptor (LXR) on TPT's effects. TPT upregulated ABCA1 and StAR expression was blocked by both LXR and RXR antagonists. TPT's effect on ABCA1 expression was reduced in LXRβ and RXRβ knockdown theca cells. Similar findings were obtained with primary human theca cells. No synergistic effect of TBT and TPT was observed. In conclusion, at an environmentally relevant dose, TPT upregulates theca cell cholesterol transporter ABCA1 expression via RXR and LXR pathways. Similar effects of TPT on human and sheep theca cells supports its conserved mechanism across mammalian theca cells.

Keywords: Ovary; Steroidogenesis; Triphenyltin; theca cells.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Cholesterol / metabolism
Female
Humans
Liver X Receptors
Mammals / metabolism
Organotin Compounds
Progesterone* / metabolism
Retinoid X Receptors
Sheep
Testosterone / metabolism
Trialkyltin Compounds* / toxicity

Substances

Liver X Receptors
Organotin Compounds
Retinoid X Receptors
Trialkyltin Compounds
Testosterone
Progesterone
tributyltin
triphenyltin
Cholesterol

Grants and funding

R01 ES027863/ES/NIEHS NIH HHS/United States