Fetal Neuroprotective Mechanism of Maternal Magnesium Sulfate: Proteomic Analysis

被引:0
|
作者
Lee Reicher
Hanin Dabaja
Yuval Ginsberg
Nizar Khatib
Yuval Fouks
Emmanuel Attali
Michael G. Ross
Zeev Weiner
Ron Beloosesky
机构
[1] Lis Maternity and Women’s Hospital,(affiliated with Sackler Faculty of Medicine)
[2] Tel Aviv Sourasky Medical Center,Department of Obstetrics and Gynecology
[3] Tel Aviv University,Bruce Rappaport Faculty of Medicine
[4] Rambam Health Care Campus,Department of Obstetrics and Gynecology
[5] Technion-Israel Institute of Technology,undefined
[6] UCLA Medical Center,undefined
[7] Biomedical Research Institute at Harbor-UCLA,undefined
[8] David Geffen School of Medicine at UCLA,undefined
来源
Journal of Molecular Neuroscience | 2022年 / 72卷
关键词
Magnesium sulfate; Preterm; Asphyxia; Infection; Neuroprotection;
D O I
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中图分类号
学科分类号
摘要
Mg supplementation has been shown to protect preterm fetuses from white and gray matter damage, but the mechanism is unclear. The purpose of this study was to study the effect of maternal inflammation on the overall protein panel of the fetal rat brain, as well as the neuroprotective effect of magnesium-sulfate (MG). Pregnant rats at e20 (n = 6, 18 total) received injections of i.p. lipopolysaccharide (LPS) 500 ug/kg or control saline (SAL) at time 0. Dams were randomized to treatment with s.c. MG (270 mg/kg loading followed by 27 mg/kg q20 min) or saline (SAL) from −2 to +2 h, followed by an additional injection of MG (270 mg/kg) at +2 h. At 4 h after LPS administration, fetal brains were collected from the 3 treatment groups (LPS/SAL, LPS/MG, SAL/SAL) and analyzed by proteomic technique. LPS significantly decreased fetal brain complement C3, alpha-1-antiproteinase, metallothionein-3, alpha-2-macroglobulin, neurosecretory protein VGF, glutathione S-transferase mu 2, fam91a1, cnot7, mitogen-activated protein kinase levels, and significantly increased fetal brain Hbg1, while MG treatment normalized these measures to normal values. Maternal inflammation may cause brain injury via pathways other than the activation of neurotoxic cytokines; this effect could be due to increased/decreased production of certain proteins associated with securing oligodendrocytes, encouraging neuronal growth in the brain, or protecting against cerebral ischemia. MG’s neuroprotective activity may be achieved by modifying the effect of LPS on proteins involved in early brain development.
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页码:626 / 632
页数:6
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