Estrogen and glucocorticoid receptors co-regulate acrolein-induced respiratory and systemic homeostatic stress responses.

IF 4.1 3区医学 Q2 TOXICOLOGY

Toxicological Sciences Pub Date : 2025-09-01 DOI:10.1093/toxsci/kfaf084

Devin I Alewel, Katherine M Rentschler, Mette C Schladweiler, Colette N Miller, Stephen H Gavett, Paul A Evansky, Rachel Grindstaff, Wanda C Williams, Urmila P Kodavanti

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Abstract

The contribution of neuroendocrine mechanisms of air pollution health effects in females and the extent to which such effects are related to estrogen signaling are unclear. To examine the interactive roles of estrogen (ER) and glucocorticoid receptors (GR) in acrolein-induced respiratory and systemic effects, female Wistar-Kyoto rats were treated daily for 9 days with corn oil (vehicle, 1 ml/kg), fulvestrant (ER-antagonist/degrader, 20 mg/kg), mifepristone (GR antagonist, 30 mg/kg) or fulvestrant + mifepristone, and on days 8 and 9 post-drug-treatment start, rats were exposed nose-only to 0 or 3.2 ppm acrolein for ∼4 h/day. Glucose-tolerance testing was performed following the first exposure. Nasal and lung lavages and blood samples were collected following the second exposure. Fulvestrant and mifepristone pretreatments decreased serum estrogen and progesterone, respectively, and each drug increased adrenocorticotropic hormone in acrolein-exposed rats. Although acrolein-induced nasal and lung protein leakage was reduced in fulvestrant-treated rats, neutrophilic inflammation and pro-inflammatory cytokine increases were exacerbated. However, acrolein-induced airway inflammation was not observed in mifepristone or co-treated rats. Regarding systemic markers of hypothalamic-pituitary-adrenal (HPA) activity, fulvestrant and mifepristone each increased circulating basal leukocytes regardless of exposure, especially total white blood cells and neutrophils. Fulvestrant-induced neutrophilia was slightly dampened in acrolein-exposed females. Fulvestrant also primed multiple adverse acrolein-induced metabolic alterations. Importantly, systemic markers of acrolein-induced HPA activity were not impacted in mifepristone or fulvestrant + mifepristone co-treated rats. These data demonstrate that neuroendocrine co-regulation by ER and GR might explain acrolein susceptibility differences, contributing novel mechanistic information to the growing recognition of gonadal hormone influence in air pollution health effects susceptibility.

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雌激素和糖皮质激素受体共同调节丙烯醛诱导的呼吸和全身稳态应激反应。

空气污染对女性健康影响的神经内分泌机制的贡献以及这种影响与雌激素信号的关系程度尚不清楚。为了研究雌激素（ER）和糖皮质激素受体（GR）在丙烯醛诱导的呼吸和全身效应中的相互作用，雌性Wistar-Kyoto大鼠每天用玉米油（对照物，1 ml /kg）、氟维司汀（ER拮抗剂/降解剂，20 mg/kg）、米非司酮（GR拮抗剂，30 mg/kg）或氟维司汀+米非司酮治疗9天，在药物治疗后第8天和第9天，大鼠仅鼻子暴露于0或3.2 ppm丙烯醛中4小时/天。首次暴露后进行葡萄糖耐量试验。第二次接触后采集鼻腔和肺部灌洗液和血液样本。氟维司汀和米非司酮预处理分别降低丙烯醛暴露大鼠血清雌激素和孕酮水平，提高促肾上腺皮质激素水平。虽然丙烯醛诱导的大鼠鼻和肺蛋白渗漏减少，但中性粒细胞炎症和促炎细胞因子的增加加剧。然而，在米非司酮或共处理大鼠中未观察到丙烯醛诱导的气道炎症。关于HPA活性的全身标志物，氟维司汀和米非司酮均增加了循环基础白细胞，尤其是总白细胞和中性粒细胞。丙烯醛暴露的雌性富维司汀诱导的中性粒细胞略有减弱。氟维司汀还引发了多种不良丙烯醛诱导的代谢改变。重要的是，在米非司酮或氟维司酮+米非司酮联合治疗的大鼠中，丙烯醛诱导的HPA活性的全身标志物没有受到影响。这些数据表明，ER和GR的神经内分泌协同调节可能解释了丙烯醛易感性的差异，为越来越多的人认识到性激素对空气污染健康影响易感性的影响提供了新的机制信息。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Toxicological Sciences 医学-毒理学

CiteScore

7.70

自引率

7.90%

发文量

118

审稿时长

1.5 months

期刊介绍： The mission of Toxicological Sciences, the official journal of the Society of Toxicology, is to publish a broad spectrum of impactful research in the field of toxicology. The primary focus of Toxicological Sciences is on original research articles. The journal also provides expert insight via contemporary and systematic reviews, as well as forum articles and editorial content that addresses important topics in the field. The scope of Toxicological Sciences is focused on a broad spectrum of impactful toxicological research that will advance the multidisciplinary field of toxicology ranging from basic research to model development and application, and decision making. Submissions will include diverse technologies and approaches including, but not limited to: bioinformatics and computational biology, biochemistry, exposure science, histopathology, mass spectrometry, molecular biology, population-based sciences, tissue and cell-based systems, and whole-animal studies. Integrative approaches that combine realistic exposure scenarios with impactful analyses that move the field forward are encouraged.