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组成型Ras活性诱导synRas小鼠海马体肥大和锥体神经元重塑。

Constitutive Ras activity induces hippocampal hypertrophy and remodeling of pyramidal neurons in synRas mice.

作者信息

Gärtner Ulrich, Alpár Alán, Reimann Frank, Seeger Gudrun, Heumann Rolf, Arendt Thomas

机构信息

Department of Neuroanatomy, Paul Flechsig Institute for Brain Research, University of Leipzig, Leipzig, Germany.

出版信息

J Neurosci Res. 2004 Sep 1;77(5):630-41. doi: 10.1002/jnr.20194.

Abstract

The small G protein Ras, which is involved critically in neurotrophic signal transduction, has been implicated in neuronal plasticity of both the developing and the adult nervous systems. In the present study, the cumulative effects of constitutive Ras activity from early in postnatal development into the adult upon the morphology of hippocampal pyramidal neurons were investigated in synRas mice overexpressing Val12-Ha-Ras postmitotically under the control of the rat synapsin I promoter. In synRas mice, stereologic investigations revealed hypertrophy of the hippocampus associated with an increase in perikaryal size of pyramidal neurons within the CA2/CA3 region and the gyrus dentatus. Morphometric analyses of Lucifer Yellow-filled CA1 pyramidal neurons, in addition, demonstrated considerable expansion of dendritic arbors. The increase in basal dendritic size was caused primarily by alterations of intermediate and distal segments and was associated with an enlarged dendritic surface. Apical dendrites showed similar but more moderate changes, which were attributed mainly to elongation of terminal segments. Sholl analyses illustrated higher complexity of both basal and apical trees. Despite significant morphologic alterations, dendritic arbors preserve their major design principles. The synaptic density within the stratum radiatum of CA1 remained unchanged; however, increases in the total hippocampal volume and in apical dendritic size imply an increment in the absolute number of synaptic contacts. The data presented here suggest a critical involvement of Ras dependent signaling in morphoregulatory processes during the maturation and in the maintenance of hippocampal pyramidal neurons.

摘要

小G蛋白Ras在神经营养信号转导中起关键作用,已被证明与发育中和成年神经系统的神经元可塑性有关。在本研究中,我们在大鼠突触素I启动子控制下,对有丝分裂后过表达Val12-Ha-Ras的synRas小鼠,研究了从出生后早期到成年期组成型Ras活性对海马锥体细胞形态的累积影响。在synRas小鼠中,体视学研究显示海马肥大,伴有CA2/CA3区和齿状回锥体细胞胞体大小增加。此外,对用路西法黄填充的CA1锥体细胞进行形态计量分析,结果显示树突分支有显著扩展。基底树突大小增加主要是由中间段和远端段的改变引起的,并伴有树突表面增大。顶树突表现出类似但更适度的变化,主要归因于末端段的延长。Sholl分析表明基底树突和顶树突的复杂性更高。尽管有明显的形态学改变,但树突分支仍保留其主要设计原则。CA1辐射层内的突触密度保持不变;然而,海马总体积和顶树突大小的增加意味着突触接触的绝对数量增加。本文提供的数据表明,Ras依赖性信号在海马锥体细胞成熟和维持过程中的形态调节过程中起关键作用。

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