信号蛋白4c的断裂干扰了信号蛋白4c /丛蛋白B2通路对实验性脑出血大鼠的神经保护作用

IF 2.7 4区 医学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Journal of chemical neuroanatomy Pub Date : 2023-10-01 DOI:10.1016/j.jchemneu.2023.102318
Dong Li , Xiang Li Sr , Jiahe Wang , Haiying Li , Haitao Shen , Xiang Xu , Gang Chen
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引用次数: 0

摘要

Semaphorin 4C(SEMA4C)及其同源受体Plexin B2是轴突引导的重要调节因子,并参与许多神经系统疾病,其中SEMA4C不仅作为配体(“正向”模式),而且作为信号受体(“反向”模式)。然而,SEMA4C/Plexin B2在脑出血(ICH)中的作用尚不清楚。在本研究中,成年雄性Sprague-Dawley大鼠通过在右侧基底节注射自体血来诱导脑出血。在体外,培养的原代神经元接受OxyHb以模拟脑出血损伤。重组SEMA4C(rSEMA4C)和编码全长SEMA4C或分泌型SEMA4C的过表达慢病毒(sSEMA4C)通过脑室注射给大鼠。首先,我们发现临床患者脑脊液中sSEMA4C水平升高与预后不良有关。大鼠脑出血后血肿周围脑组织SEMA4C和sSEMA4C均升高。SEMA4C的过度表达减轻了脑出血后的神经元凋亡、神经症和神经损伤。然而,rSEMA4C或sSEMA4C过表达的治疗加重了神经元损伤。此外,当用SEMA4C过表达处理时,SEMA4C/Plexin B2信号传导的正向模式下游蛋白RhoA和反向模式下游ID1/3转录因子都被激活。然而,当暴露于rSEMA4C或sSEMA4C过表达时,只有正向模式被激活。因此,sSEMA4C可能是预测脑出血患者预后的一种新的分子生物标志物,预防SEMA4C切割有望成为一个有前途的治疗靶点。
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Cleavage of semaphorin 4 C interferes with the neuroprotective effect of the semaphorin 4 C/Plexin B2 pathway on experimental intracerebral hemorrhage in rats

Semaphorin 4 C (SEMA4C) and its cognate receptor Plexin B2 are important regulators of axon guidance and are involved in many neurological diseases, in which SEMA4C acts not only as a ligand ("forward" mode) but also as a signaling receptor ("reverse" mode). However, the role of SEMA4C/Plexin B2 in intracerebral hemorrhage (ICH) remains unclear. In this study, ICH in adult male Sprague-Dawley rats was induced by autologous blood injection in the right basal ganglia. In vitro, cultured primary neurons were subjected to OxyHb to imitate ICH injury. Recombinant SEMA4C (rSEMA4C) and overexpressing lentiviruses encoding full-length SEMA4C or secretory SEMA4C (sSEMA4C) were administered to rats by intraventricular injection. First, we found that elevated levels of sSEMA4C in the cerebrospinal fluid (CSF) of clinical patients were associated with poor prognosis. Both SEMA4C and sSEMA4C were increased in brain tissue around the hematoma after ICH in rats. Overexpression of SEMA4C attenuated neuronal apoptosis, neurosis, and neurologic impairment after ICH. However, treatment with rSEMA4C or sSEMA4C overexpression exacerbated neuronal injury. In addition, when treated with SEMA4C overexpression, the forward mode downstream protein RhoA and the reverse mode downstream ID1/3 transcriptional factors of SEMA4C/Plexin B2 signaling were all activated. Nevertheless, when exposed to rSEMA4C or sSEMA4C overexpression, only the forward mode was activated. Thus, sSEMA4C may be a novel molecular biomarker to predict the prognosis of patients with ICH, and the prevention of SEMA4C cleavage is expected to be a promising therapeutic target.

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来源期刊
Journal of chemical neuroanatomy
Journal of chemical neuroanatomy 医学-神经科学
CiteScore
4.50
自引率
3.60%
发文量
87
审稿时长
62 days
期刊介绍: The Journal of Chemical Neuroanatomy publishes scientific reports relating the functional and biochemical aspects of the nervous system with its microanatomical organization. The scope of the journal concentrates on reports which combine microanatomical, biochemical, pharmacological and behavioural approaches. Papers should offer original data correlating the morphology of the nervous system (the brain and spinal cord in particular) with its biochemistry. The Journal of Chemical Neuroanatomy is particularly interested in publishing important studies performed with up-to-date methodology utilizing sensitive chemical microassays, hybridoma technology, immunocytochemistry, in situ hybridization and receptor radioautography, to name a few examples. The Journal of Chemical Neuroanatomy is the natural vehicle for integrated studies utilizing these approaches. The articles will be selected by the editorial board and invited reviewers on the basis of their excellence and potential contribution to this field of neurosciences. Both in vivo and in vitro integrated studies in chemical neuroanatomy are appropriate subjects of interest to the journal. These studies should relate only to vertebrate species with particular emphasis on the mammalian and primate nervous systems.
期刊最新文献
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