淀粉样β蛋白_(1-42)和thiorphan对恒河猴海马结构的影响

目的观察淀粉样β蛋白1-42(Aβ1-42)和thiorphan对恒河猴大脑海马神经元淀粉样蛋白、乙酰胆碱转移酶(ChAT)以及胶质纤维酸性蛋白(GFAP)表达的影响,为注射thior-phan和Aβ1-42建立恒河猴AD模型提供数据准备。方法开颅后先注射thiorphan到猕猴的大脑皮质和基底核,消耗已存在的Neprilysin,然后再缓慢的注射孵育好的纤丝状Aβ1-42,后植入含有thiorphan的微渗透泵到基底核。HE染色观察海马结构病理改变。免疫组化的方法检测猴子海马Aβ1-42、乙酰胆碱转移酶(ChAT)、胶质纤维酸性蛋白(GFAP)阳性细胞的表达。结果HE染色显示海马CA1、CA2等区神经元萎缩,海马齿状回局部颗粒细胞丢失被胶质细胞取代;免疫组化结果显示模型组海马各区Aβ1-42、ChAT、GFAP阳性细胞吸光度(OD值)分别为0.59±0.05、0.21±0.04、0.19±0.04,与对照组比较P<0.01,差异具有统计学意义。结论Aβ1-42和thiorphan联合颅内给药导致恒河猴海马产生类似AD患者的病理改变。     

Growing axons in fish optic nerve are accompanied by astrocytes interconnected by tight junctions

Mammalian astrocytes are in general interconnected by gap but not by tight junctions and play an ambiguous and controversially discussed role in central nervous system regeneration. At different neuroanatomical sites, fish astrocytes are interconnected by tight junctions and desmosomes and are involved in the successful regeneration of lesioned fiber tracts. In fish, newly generated retinal ganglion cells continuously grow new axons to the optic tectum but the interrelationship between glial tight junctions and axonal growth is undefined so far. We therefore investigated the occurrence of tight junctional structures and molecules within the ribbon-shaped optic nerve of a teleost fish (Astatotilapia burtoni) and found a predominant expression of zonula occludens protein-1 and claudin-1 in astrocytes where axons of new ganglion cells are assembled retinotopically within the optic nerve. This may support a previously formulated hypothesis according to that different properties of astrocytic membranes could be responsible for different glio-neuronal interactions which in turn may determine the micro-environmental conditions of growing axons.     

Impact of 17beta-estradiol on cytokine-mediated apoptotic effects in primary hippocampal and neocortical cell cultures

Estrogens are developmental regulators of mitochondrial apoptotic pathway in the central nervous system, but little is known about their involvement in cytokine-induced apoptosis. In the present study, we evaluated effects of 17beta-estradiol on pro-inflammatory cytokine- and staurosporine-mediated activation of caspase-3 and LDH-release in primary neuronal/glial cell cultures of mouse hippocampal and neocortical cells at different stages of their development in vitro. Enzyme activities were determined with colorimetric methods 6 h, 14 h, 24 h, and 48 h after exposure to the apoptotic agents. Biochemical data were supported at the cellular level by Hoechst 33342 and MAP-2 stainings, which were carried out 48 h after the treatment. Cytokines (co-treatment with Il-1beta and TNFalpha; 1 ng/ml) increased caspase-3 activity in the hippocampal and neocortical cells up to over 200% of control values, and these effects were mostly observed on 2 and 7 days in vitro (DIV). Moderate, but significant cytokine-mediated increase in LDH-release was demonstrated in both tissues, especially on 7 and 12 DIV. Estradiol (100 nM) inhibited the activation of caspase-3 at early stage of development (2 DIV) in the hippocampal, but not in the neocortical cultures. The cytokine-induced activation of caspase-3 and LDH-release was inhibited by estradiol in estrogen receptor-independent way. These data point to a possible role of estrogens as non-estrogen receptor-related inhibitors of cytokine-activated apoptotic pathway in the developing central nervous system.     

Musashi1 antigen expression in human fetal germinal matrix development

Musashi1 is a highly conserved protein found in neural progenitor cells. We examined the expression dynamics of Musashi1 in conjunction with other representative neural progenitor antigenic determinants (Ki-67 and nestin) during 8 different stages of the developing human fetal germinal matrix. Our results indicate that Musashi1 is a useful marker for immature cells in periventricular areas inhabited by stem cells, progenitor cells, and differentiating cells.     

Inflammatory responses of the substantia nigra after acute hypoxia in neonatal rats

The neocortex and the striatum are the brain regions most known to be particularly vulnerable to acute insults like hypoxia or ischemia. In this work, we assess the possibility of cellular damage to the substantia nigra (SN) after hypoxia-reoxygenation in the new born rat. The aim of the present paper was to evaluate the expression of growth factor IGF-I, and growth factor binding proteins IGFBP-3 and IGFBP-5 genes and induction of NOS family members (nNOS, eNOS and iNOS) and TNF-alpha genes together with glia activation, in the SN at 5 and 48 h after severe hypoxia in the 7 day-old rat, a model for the term human fetus. At early time, while IGFs remain unchanged, we found a transient increase in eNOS and nNOS. Two days after the injury, nNOS expression remained high, iNOS and TNF-alpha increased and also GFAP protein expression was observed together with a profusion of reactive astrocytes distributed throughout the SN. This study on the acute effects of hypoxia on the developing brain provides additional insights into the vulnerability of the SN, a brain region involved in neurodegenerative pathologies.     

EGF联合HGF诱导BMSCs向神经元样细胞分化

目的:通过观察HGF在诱导BMSCs向神经元样细胞分化过程中的作用,尝试寻找一种高效的诱导BMSCs分化途径。方法:从成年大鼠股骨内获取骨髓,分离BMSCs,细胞培养并鉴定,然后加入不同的诱导因子诱导BMSCs分化,利用免疫荧光染色技术、RT-PCR技术及免疫印迹技术检测BMSCs向神经元样细胞的分化情况。结果:形态学观察及流式细胞检测技术结果显示成功的获得了BMSCs,加入诱导因子HGF或EGF联合HGF后,RT-PCR检测结果及免疫印迹检测结果均显示,BMSCs可向神经元样细胞分化。结论:EGF联合HGF可诱导BMSCs向神经元样细胞分化。     

Taurine: The comeback of a neutraceutical in the prevention of retinal degenerations

Taurine is the most abundant amino acid in the retina. In the 1970s, it was thought to be involved in retinal diseases with photoreceptor degeneration, because cats on a taurine-free diet presented photoreceptor loss. However, with the exception of its introduction into baby milk and parenteral nutrition, taurine has not yet been incorporated into any commercial treatment with the aim of slowing photoreceptor degeneration. Our recent discovery that taurine depletion is involved in the retinal toxicity of the antiepileptic drug vigabatrin has returned taurine to the limelight in the field of neuroprotection. However, although the retinal toxicity of vigabatrin principally involves a deleterious effect on photoreceptors, retinal ganglion cells (RGCs) are also affected. These findings led us to investigate the possible role of taurine depletion in retinal diseases with RGC degeneration, such as glaucoma and diabetic retinopathy. The major antioxidant properties of taurine may influence disease processes. In addition, the efficacy of taurine is dependent on its uptake into retinal cells, microvascular endothelial cells and the retinal pigment epithelium. Disturbances of retinal vascular perfusion in these retinal diseases may therefore affect the retinal uptake of taurine, resulting in local depletion. The low plasma taurine concentrations observed in diabetic patients may further enhance such local decreases in taurine concentration. We here review the evidence for a role of taurine in retinal ganglion cell survival and studies suggesting that this compound may be involved in the pathophysiology of glaucoma or diabetic retinopathy. Along with other antioxidant molecules, taurine should therefore be seriously reconsidered as a potential treatment for such retinal diseases.     

P3a and P3b components associated to the neurocognitive evaluation of invalidly cued targets

The present report focuses on evaluating the neurocognitive consequences of the correct or incorrect spatial prediction induced by a spatial cue. Positions in the vertical meridian were cued in order to evaluate the cognitive consequences in the processing of the validly (VC) or invalidly cued (IC) targets. The behavioural responses and the 64 EEG channel were recorded. The late endogenous event-related potential (ERP) induced by target stimuli in VC and IC targets were compared in voltage amplitude, voltage and current source density topographies. The P3a and a late positive complex, possibly P3b were increased in a statistically significant manner in the IC targets with regard to the VC targets. The previous result suggests that subjects prepare to accomplish the task upon specification of the cue, and when the IC target appeared it is treated as a low probability stimulus in a similar manner to deviant stimuli in odd-ball paradigms.     

Cell-cell interaction modulates neuroectodermal specification of embryonic stem cells

The controlled differentiation of embryonic stem (ES) cells is of utmost interest to their clinical, biotechnological, and basic science use. Many investigators have combinatorially assessed the role of specific soluble factors and extracellular matrices in guiding ES cell fate, yet the interaction between neighboring cells in these heterogeneous cultures has been poorly defined due to a lack of conventional tools to specifically uncouple these variables. Herein, we explored the role of cell-cell interactions during neuroectodermal specification of ES cells using a microfabricated cell pair array. We tracked differentiation events in situ, using an ES cell line expressing green fluorescent protein (GFP) under the regulation of the Sox1 gene promoter, an early marker of neuroectodermal germ cell commitment in the adult forebrain. We observed that a previously specified Sox1-GFP+ cell could induce the specification of an undifferentiated ES cell. This induction was modulated by the two cells being in contact and was dependent on the age of previously specified cell prior to coculture. A screen of candidate cell adhesion molecules revealed that the expression of connexin (Cx)-43 correlated with the age-dependent effect of cell contact in cell pair experiments. ES cells deficient in Cx-43 showed aberrant neuroectodermal specification and lineage commitment, highlighting the importance of gap junctional signaling in the development of this germ layer. Moreover, this study demonstrates the integration of microscale culture techniques to explore the biology of ES cells and gain insight into relevant developmental processes otherwise undefined due to bulk culture methods.