Spatial Lipid MetabolicRemodeling from Placenta toMultiple Suborgans during the Gestational Micro- or Nanoplastics Exposure

Guangquan Chen (7493930); Qianqian Sun (703509); Shiyi Xiong (5844731); Tianyou Cao (22653878); Bin Du (138774); Qingping Wang (1883716); Jing Li (10611); Qian Luo (610818); Chao Zhao (253684)

doi:10.1021/acsnano.5c13265.s001

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Spatial Lipid MetabolicRemodeling from Placenta toMultiple Suborgans during the Gestational Micro- or Nanoplastics Exposure

Figshare 2025

Guangquan Chen (7493930), Qianqian Sun (703509), Shiyi Xiong (5844731), Tianyou Cao (22653878), Bin Du (138774), Qingping Wang (1883716), Jing Li (10611), Qian Luo (610818), Chao Zhao (253684)

Summary

Using pregnant mice exposed to polystyrene micro- and nanoplastics from gestation day 1–18, researchers used MALDI mass spectrometry imaging to construct a comprehensive spatial map of lipid metabolism changes across placenta and multiple maternal and fetal organs, revealing widespread lipid metabolic remodeling.

Polymers

PE PS

Body Systems

Cardiovascular Hepatic Musculoskeletal Nervous Renal Reproductive

Models

Mouse

Study Type Environmental

Gestational exposure to micro- and/or nanoparticles (M/NPs) may be closely associated with adverse maternal and offspring outcomes involving multiple organ dysfunctions. Organ functional change is achieved through metabolic adaptation in response to changes in the external environment; yet, intricacies of these organ dysfunctions and underlying metabolic changes remain poorly understood, particularly at spatial suborgan level. Using a pregnant mouse model exposed to polystyrene (PS)-M/NPs (sizes: 100 nm, 5 μm, 10 mg/L in drinking water) from gestation day 1 to 18, we construct a comprehensive multisub-organ lipid metabolic landscape. This analysis integrates MALDI-mass spectrometry imaging with histological assessment to monitor changes in maternal suborgans-placenta-fetus unit. Our findings reveal distinct metabolic responses between maternal and fetal organs to gestational PS-M/NPs exposure. We identify potential targeted suborgans and spatial biomarkers associated with PS-M/NPs exposure according to histological damage and metabolic remodeling, including placental junctional and labyrinth zone (e.g., phosphatidylserine, phosphatidylethanolamine [PE]), renal cortex of maternal kidney (e.g., ceramide [Cer], PE, sphingomyelin [SM], phosphatidylglycerol [PG], phosphatidylserine), ventricular muscular layer and interventricular septum of maternal heart (e.g., PE, lysophosphatidylethanolamine [LPE], lysophosphatidic acid [LPA]), fetal brain and spinal cord (e.g., Cer), and fetal liver (e.g., Cer). Furthermore, phosphatidylserine synthesis and glycolipid metabolism pathways are found to be exclusively enriched following PS-NP and PS-MP exposure in the multiorgan network, respectively. We propose an M/NPs scale-exposed suborgan effect framework, which provides a molecular foundation and potential spatial biomarkers for elucidating intersub-organ interactions in response to M/NPs exposure and their role in mediating pregnancy state.

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