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Download fileMALDI-MS Imaging Reveals Asymmetric Spatial Distribution of Lipid Metabolites from Bisphenol S‑Induced Nephrotoxicity
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posted on 2018-02-12, 00:00 authored by Chao Zhao, Peisi Xie, Ting Yong, Hailin Wang, Arthur Chi Kong Chung, Zongwei CaiWith the continuous
exposure of environmental pollutants in organisms,
determination of abundance variation and spatial distribution of lipids
might expand our understanding of toxicological mechanisms occurring
in the kidney. Herein, an integrated method involving mass spectrometry
(MS)-based lipidomics and matrix-assisted laser desorption/ionization-MS
imaging (MALDI-MSI) was developed for the study of nephrotoxicity
in mice exposed to 10 and 100 μg bisphenol S (BPS)/kg body weight/day.
The BPS exposure remarkable perturbed abundances of 91 potential markers
that mainly involved in five metabolic pathways. We elucidated the
lipids spatial heterogeneity by using morphological analysis, probabilistic
latent semantic analysis, and coregistered multimodal three-dimensional
(3D)-MSI. In morphological analysis, both 10 and 100 μg BPS
induced significant nephrotoxicity to mice, including glomerular necrosis
in renal cortex, cloudy swelling in renal medulla, and interstitial
collapsing in renal pelvis. Significant differential signaling lipids
such as sphingomyelin (SM) (d22:0/20:4), ceramide (Cer) (d18:2/24:1),
and sphingosine (d18:0) related to inflammation were found to be up-regulated
and colocalized in the renal cortex, medulla, and pelvis, respectively.
Also, seven significant differential lipids, which are considered
to be involved in membrane homeostasis and cellular function, were
found to be colocalized in the renal cortex. The observed significant
variations of morphology, lipid accumulation, and metabolism in the
renal cortex implicated that lipids in the renal cortex were more
sensitive to BPS exposure than those in the renal medulla and pelvis.
Moreover, we reconstructed a 3D-MSI model of kidney and identified
two heterogeneous-related substructures in the renal cortex and pelvis
upon 100 μg BPS exposure. It might be used in novel specificity
evaluation and early diagnosis for environmental pollutant-induced
kidney diseases.