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Fetal regional brain protein signature in FASD rat model

机译:FASD大鼠模型中的胎儿区域脑蛋白签名

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Fetal alcohol spectrum disorders (FASD) describe neurodevelopmental deficits in children exposed to alcohol in utero. We hypothesized that gestational alcohol significantly alters fetal brain regional protein signature. Pregnant rats were binge-treated with alcohol or pair-fed and nutritionally-controlled. Mass spectrometry identified 1806, 2077, and 1456 quantifiable proteins in the fetal hippocampus, cortex, and cerebellum, respectively. A stronger effect of alcohol exposure on the hippocampal proteome was noted: over 600 hippocampal proteins were significantly (P.05) altered, including annexin A2, nucleobindin-1, and glypican-4, regulators of cellular growth and developmental morphogenesis. In the cerebellum, cadherin-13, reticulocalbin-2, and ankyrin-2 (axonal growth regulators) were significantly (P.05) altered; altered cortical proteins were involved in autophagy (endophilin-B1, synaptotagmin-1). Ingenuity analysis identified proteins involved in protein homeostasis, oxidative stress, mitochondrial dysfunction, and mTOR as major pathways in the cortex and hippocampus significantly (P .05) affected by alcohol. Thus, neurodevelopmental protein changes may directly relate to FASD neuropathology. (C) 2018 Elsevier Inc. All rights reserved.
机译:胎儿酒精谱紊乱(FASD)描述在UTERO中暴露于酒精的儿童中的神经发育缺陷。我们假设妊娠酒精显着改变胎儿脑区域蛋白签名。怀孕的大鼠用酒精或配对喂养和营养控制的妊娠。质谱分别鉴定了胎儿海马,皮质和小脑中的1806,2077和1456个可量化的蛋白质。较强烈的酒精暴露对海马蛋白质组的影响:超过600个海马蛋白质显着(P <.05)改变,包括膜蛋白A2,核欠蛋白-1和糖尿病-4,细胞生长调节剂和发育形态发生。在小脑中,钙粘蛋白-13,稗素-13,reticulocalbin-2和Ankyrin-2(轴突生长调节剂)显着改变;改变的皮质蛋白涉及自噬(内皮蛋白-B1,Synaptotagmin-1)。 Ingenuity分析确定了蛋白质稳态,氧化应激,线粒体功能障碍和MTOR作为皮质和海马的主要途径的蛋白质显着(p <.05)受酒精的主要途径。因此,神经发育蛋白质的变化可能直接涉及FasD神经病理学。 (c)2018年Elsevier Inc.保留所有权利。

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