Reference Gene Validation in the Embryonic and Postnatal Brain in the Rat Hyperhomocysteinemia Model.

IF 2.9 3区 医学 Q2 NEUROSCIENCES
Anna A Kovalenko, Alexander P Schwarz, Anastasiia D Shcherbitskaia, Anastasiia V Mikhel, Dmitrii S Vasilev, Alexander V Arutjunyan
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引用次数: 0

Abstract

Maternal hyperhomocysteinemia (HCY) induced by genetic defects in methionine cycle enzymes or vitamin imbalance is known to be a pathologic factor that can impair embryonal brain development and cause long-term consequences in the postnatal brain development as well as changes in the expression of neuronal genes. Studies of the gene expression on this model requires the selection of optimal housekeeping genes. This work aimed to analyze the expression stability of housekeeping genes in offspring brain. Pregnant female Wistar rats were treated daily with a 0.15% L-methionine solution in the period starting on the 4th day of pregnancy until delivery, to cause the increase in the homocysteine level in fetus blood and brain. Housekeeping gene expression was assessed by RT-qPCR on whole embryonic brain and selected rat brain areas at P20 and P90. The amplification curves were analyzed, and raw means Cq data were imported to the RefFinder online tool to assess the reference genes stability. Most of the analyzed genes showed high stability of mRNA expression in the fetal brain at both periods of analysis (E14 and E20). However, the most stably expressed genes at different age points differed. Actb, Ppia, Rpl13a are the most stably expressed on E14, Ywhaz, Pgk1, Hprt1 - on E20 and P20, Hprt1, Actb, and Pgk1 - on P90. Gapdh gene used as a reference in various studies demonstrates high stability only in the hippocampus and cannot be recommended as the optimal reference gene on HCY model. Hprt1 and Pgk1 genes were found to be the most stably expressed in the brain of rat subjected to HCY. These two genes showed high stability in the brain on E20 and in various areas of the brain on the P20 and P90. On E14, the preferred genes for normalization are Actb, Ppia, Rpl13a.

Abstract Image

大鼠高同型半胱氨酸血症模型胚胎和出生后大脑中参考基因的验证。
众所周知,由蛋氨酸循环酶遗传缺陷或维生素失衡诱发的母体高同型半胱氨酸血症(HCY)是一种病理因素,可损害胚胎大脑发育,对出生后大脑发育造成长期影响,并导致神经元基因表达发生变化。研究该模型的基因表达需要选择最佳的管家基因。本研究旨在分析子代脑中看门基因的表达稳定性。从怀孕第 4 天起至分娩前,每天用 0.15% L-蛋氨酸溶液处理怀孕雌性 Wistar 大鼠,以引起胎儿血液和大脑中同型半胱氨酸水平的升高。用 RT-qPCR 方法评估了整个胚胎大脑和 P20 和 P90 大鼠选定脑区的看家基因表达。对扩增曲线进行分析,并将原始平均 Cq 数据导入 RefFinder 在线工具,以评估参考基因的稳定性。在两个分析时期(E14 和 E20),大多数分析基因在胎儿大脑中的 mRNA 表达都表现出较高的稳定性。然而,在不同的年龄点,表达最稳定的基因却各不相同。Actb、Ppia和Rpl13a在E14时表达最稳定,Ywhaz、Pgk1和Hprt1在E20和P20时表达最稳定,Hprt1、Actb和Pgk1在P90时表达最稳定。在多项研究中作为参考基因的 Gapdh 基因仅在海马中表现出高度稳定性,因此不能推荐作为 HCY 模型的最佳参考基因。研究发现,Hprt1 和 Pgk1 基因在 HCY 大鼠大脑中的表达最为稳定。这两个基因在 E20 大鼠大脑中以及在 P20 和 P90 大鼠大脑的不同区域均表现出高度稳定性。在 E14 期,Actb、Ppia 和 Rpl13a 是首选的正常化基因。
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来源期刊
Neurotoxicity Research
Neurotoxicity Research 医学-神经科学
CiteScore
7.70
自引率
5.40%
发文量
164
审稿时长
6-12 weeks
期刊介绍: Neurotoxicity Research is an international, interdisciplinary broad-based journal for reporting both basic and clinical research on classical neurotoxicity effects and mechanisms associated with neurodegeneration, necrosis, neuronal apoptosis, nerve regeneration, neurotrophin mechanisms, and topics related to these themes. Published papers have focused on: NEURODEGENERATION and INJURY Neuropathologies Neuronal apoptosis Neuronal necrosis Neural death processes (anatomical, histochemical, neurochemical) Neurodegenerative Disorders Neural Effects of Substances of Abuse NERVE REGENERATION and RESPONSES TO INJURY Neural Adaptations Neurotrophin mechanisms and actions NEURO(CYTO)TOXICITY PROCESSES and NEUROPROTECTION Excitatory amino acids Neurotoxins, endogenous and synthetic Reactive oxygen (nitrogen) species Neuroprotection by endogenous and exogenous agents Papers on related themes are welcome.
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