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雌激素增加单个突触前输入与多个突触后CA1锥体细胞之间的突触连接:一项连续电子显微镜研究。

Estrogen increases synaptic connectivity between single presynaptic inputs and multiple postsynaptic CA1 pyramidal cells: a serial electron-microscopic study.

作者信息

Yankova M, Hart S A, Woolley C S

机构信息

Department of Neurobiology and Physiology, Northwestern University, Evanston, IL 60208, USA.

出版信息

Proc Natl Acad Sci U S A. 2001 Mar 13;98(6):3525-30. doi: 10.1073/pnas.051624598. Epub 2001 Feb 20.

Abstract

Dendritic spines are sites of the vast majority of excitatory synaptic input to hippocampal CA1 pyramidal cells. Estrogen has been shown to increase the density of dendritic spines on CA1 pyramidal cell dendrites in adult female rats. In parallel with increased spine density, estrogen has been shown also to increase the number of spine synapses formed with multiple synapse boutons (MSBs). These findings suggest that estrogen-induced dendritic spines form synaptic contacts with preexisting presynaptic boutons, transforming some previously single synapse boutons (SSBs) into MSBs. The goal of the current study was to determine whether estrogen-induced MSBs form multiple synapses with the same or different postsynaptic cells. To quantify same-cell vs. different-cell MSBs, we filled individual CA1 pyramidal cells with biocytin and serially reconstructed dendrites and dendritic spines of the labeled cells, as well as presynaptic boutons in synaptic contact with labeled and unlabeled (i.e., different-cell) spines. We found that the overwhelming majority of MSBs in estrogen-treated animals form synapses with more than one postsynaptic cell. Thus, in addition to increasing the density of excitatory synaptic input to individual CA1 pyramidal cells, estrogen also increases the divergence of input from individual presynaptic boutons to multiple postsynaptic CA1 pyramidal cells. These findings suggest the formation of new synaptic connections between previously unconnected hippocampal neurons.

摘要

树突棘是海马体CA1锥体神经元绝大多数兴奋性突触输入的位点。雌激素已被证明可增加成年雌性大鼠CA1锥体神经元树突上的树突棘密度。与树突棘密度增加同时,雌激素还被证明可增加与多个突触终扣(MSB)形成的棘突触数量。这些发现表明,雌激素诱导形成的树突棘与预先存在的突触前终扣形成突触联系,将一些先前的单突触终扣(SSB)转变为MSB。本研究的目的是确定雌激素诱导的MSB是否与相同或不同的突触后细胞形成多个突触。为了量化同细胞与异细胞MSB,我们用生物素填充单个CA1锥体神经元,并对标记细胞的树突和树突棘以及与标记和未标记(即异细胞)棘突触接触的突触前终扣进行连续重建。我们发现,雌激素处理动物中的绝大多数MSB与不止一个突触后细胞形成突触。因此,除了增加单个CA1锥体神经元的兴奋性突触输入密度外,雌激素还增加了单个突触前终扣到多个突触后CA1锥体神经元的输入发散。这些发现表明在先前未连接的海马神经元之间形成了新的突触连接。

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