Neural differentiation of human embryonic stem cells as an in vitro tool for the study of the expression patterns of the neuronal cytoskeleton during neurogenesis

The neural differentiation of human embryonic stem cells (ESCs) is a potential tool for elucidating the key mechanisms involved in human neurogenesis. Nestin and β-III-tubulin, which are cytoskeleton proteins, are marker proteins of neural stem cells (NSCs) and neurons, respectively. However, the expression patterns of nestin and β-III-tubulin in neural derivatives from human ESCs remain unclear. In this study, we found that neural progenitor cells (NPCs) derived from H9 cells express high levels of nestin and musashi-1. In contrast, β-III-tubulin was weakly expressed in a few NPCs. Moreover, in these cells, nestin formed filament networks, whereas β-III-tubulin was distributed randomly as small particles. As the differentiation proceeded, the nestin filament networks and the β-III-tubulin particles were found in both the cell soma and the cellular processes. Moreover, the colocalization of nestin and β-III-tubulin was found mainly in the cell processes and neurite-like structures and not in the cell soma. These results may aid our understanding of the expression patterns of nestin and β-III-tubulin during the neural differentiation of H9 cells.     

DNA repair mechanisms in dividing and non-dividing cells

DNA damage created by endogenous or exogenous genotoxic agents can exist in multiple forms, and if allowed to persist, can promote genome instability and directly lead to various human diseases, particularly cancer, neurological abnormalities, immunodeficiency and premature aging. To avoid such deleterious outcomes, cells have evolved an array of DNA repair pathways, which carry out what is typically a multiple-step process to resolve specific DNA lesions and maintain genome integrity. To fully appreciate the biological contributions of the different DNA repair systems, one must keep in mind the cellular context within which they operate. For example, the human body is composed of non-dividing and dividing cell types, including, in the brain, neurons and glial cells. We describe herein the molecular mechanisms of the different DNA repair pathways, and review their roles in non-dividing and dividing cells, with an eye toward how these pathways may regulate the development of neurological disease.     

5个温带树种冠层枝叶非结构性碳水化合物浓度的空间变异

非结构性碳水化合物(NSC)是树木存活和生长的重要能源物质。冠层NSC不但是全树NSC的来源,也是全树NSC的重要储存库。然而,冠层NSC空间变异的研究较少,因而影响了树木NSC分配的估算精度。以红松(Pinus koraiensis)、兴安落叶松(Larix gmelinii)、水曲柳(Fraxinus mandshurica)、蒙古栎(Quercus mongolica)和白桦(Betula platyphylla)5个温带树种为研究对象,测定了不同高度冠层叶和细枝(直径≤3 cm)NSC浓度,分析了粗枝(一级侧枝)枝皮、边材和心材NSC浓度轴向变化及其与枝径的关系。结果表明:(1)除了5月末兴安落叶松树冠中层叶淀粉浓度显著高于树冠下层,以及8月中旬树冠上层叶可溶性糖浓度显著高于树冠中层之外,其他树种冠层叶NSC浓度的垂直变化不显著。常绿树种红松叶龄对NSC浓度的影响在生长季中期显著,但在生长季末期和休眠季节的影响不显著。(2)除了5月末红松树冠上层细枝可溶性糖浓度显著高于树冠中层之外,其他树种不同高度冠层间细枝NSC浓度差异不显著。(3)在纵向上,阔叶树种蒙古栎、水曲柳和白桦粗枝的枝皮、边材和心材NSC浓度多随着距树枝基部距离的增加而升高;在径向上,NSC浓度(除了水曲柳边材淀粉和白桦枝皮淀粉之外)多随着枝径增加而降低,表明树枝中的NSC浓度随着远离碳源而降低。总体上,5个温带树种冠层叶、细枝NSC浓度的空间变异不显著,但枝径和叶龄对NSC浓度的影响因树种、组织和季节而异,这在未来研究中应予考虑。     

Expression of GD2 and GD3 gangliosides in human embryonic neural stem cells

NSCs (neural stem cells) are undifferentiated neural cells endowed with a high potential for proliferation and a capacity for self-renewal with retention of multipotency to differentiate into neurons and glial cells. It has been recently reported that GD3, a b-series ganglioside, is a marker molecule for identifying and isolating mouse NSCs. However, the expression of gangliosides in human NSCs is largely unknown. In the present study, we analysed the expression of gangliosides, GD2 and GD3, in human NSCs that were isolated from human brains at gestational week 17 in the form of neurospheres, which are floating clonal aggregates formed by NSCs in vitro. Employing immunocytochemistry, we found that human NSCs were strongly reactive to anti-GD2 antibody and relatively weakly reactive to anti-GD3 antibody. Treatment of these cells with an organic solvent such as 100% methanol, which selectively removes glycolipids from plasma membrane, abolished the immunoreactivity with those antibodies, indicating that the reactivity was due to GD2 and GD3, but not to GD2-/GD3-like glycoproteins or proteoglycans. The immunoreactivity of human NSCs to antibody against SSEA-1 (stage-specific embryonic antigen-1), a well-known carbohydrate antigen of NSCs, was not decreased by the treatment with 100% methanol, indicating that SSEA-1 is mainly carried by glycoproteins and/or proteoglycans in human NSCs. Our study suggests that GD2 and GD3 can be marker gangliosides for identifying human NSCs.     

Activation of Autophagic Flux against Xenoestrogen Bisphenol-A-induced Hippocampal Neurodegeneration via AMP kinase (AMPK)/Mammalian Target of Rapamycin (mTOR) Pathways

The human health hazards related to persisting use of bisphenol-A (BPA) are well documented. BPA-induced neurotoxicity occurs with the generation of oxidative stress, neurodegeneration, and cognitive dysfunctions. However, the cellular and molecular mechanism(s) of the effects of BPA on autophagy and association with oxidative stress and apoptosis are still elusive. We observed that BPA exposure during the early postnatal period enhanced the expression and the levels of autophagy genes/proteins. BPA treatment in the presence of bafilomycin A₁ increased the levels of LC3-II and SQSTM1 and also potentiated GFP-LC3 puncta index in GFP-LC3-transfected hippocampal neural stem cell-derived neurons. BPA-induced generation of reactive oxygen species and apoptosis were mitigated by a pharmacological activator of autophagy (rapamycin). Pharmacological (wortmannin and bafilomycin A₁) and genetic (beclin siRNA) inhibition of autophagy aggravated BPA neurotoxicity. Activation of autophagy against BPA resulted in intracellular energy sensor AMP kinase (AMPK) activation, increased phosphorylation of raptor and acetyl-CoA carboxylase, and decreased phosphorylation of ULK1 (Ser-757), and silencing of AMPK exacerbated BPA neurotoxicity. Conversely, BPA exposure down-regulated the mammalian target of rapamycin (mTOR) pathway by phosphorylation of raptor as a transient cell''s compensatory mechanism to preserve cellular energy pool. Moreover, silencing of mTOR enhanced autophagy, which further alleviated BPA-induced reactive oxygen species generation and apoptosis. BPA-mediated neurotoxicity also resulted in mitochondrial loss, bioenergetic deficits, and increased PARKIN mitochondrial translocation, suggesting enhanced mitophagy. These results suggest implication of autophagy against BPA-mediated neurodegeneration through involvement of AMPK and mTOR pathways. Hence, autophagy, which arbitrates cell survival and demise during stress conditions, requires further assessment to be established as a biomarker of xenoestrogen exposure.     

氮肥对风箱果幼苗形态和生理特性的影响

采用盆栽实验的方法,设置4种水平氮肥处理,研究不同氮肥处理对风箱果1年生幼苗的生长表现、生物量积累和分配、光合生理特征、非结构性碳（NSC）积累等的影响。结果表明：施用氮肥促进了风箱果幼苗的地径、分枝数和冠幅的生长,促进了茎、叶和总生物量的积累（P<0.05）,提高了茎的生物量分配比例,减少了根生物量的分配比例;施用氮肥显著提高了净光合速率、叶氮含量、茎中的可溶性糖和NSC的积累（P<0.05）,但减少了根中的可溶性糖和NSC含量（P<0.05）。不同水平氮肥处理间（N1、N2、N3）的大部分指标差异并不显著,说明风箱果幼苗对土壤养分的变化并不敏感。