T细胞转录因子-4在大鼠脑缺血再灌注海马齿状回神经干细胞中的表达

目的:检测T细胞转录因子-4(Tcf-4)在大鼠脑缺血再灌注海马组织神经干细胞中的表达及其变化。探讨影响神经干细胞早期增殖分化的分子调控机制。方法:采用大脑中动脉栓塞(MCAO)制作大鼠脑缺血再灌注模型。用免疫组织化学SP法及RT-PCR法检测海马神经干细胞BrdU、Tcf-4中的表达。结果:随着脑缺血再灌注第3日齿状回神经元BrdU阳性细胞明显增多,第7日达高峰,然后逐渐减少。Tcf-4 mRNA反应产物随脑缺血再灌注时间延长逐渐增多,第21日表达最强,以后表达逐渐减少。结论:Tcf-4时间依赖性表达与神经干细胞增殖分化进程相吻合,说明其在神经干细胞晚期分化中起重要调控作用。     

Role of oxidative stress,angiogenesis and chemo-attractant cytokines in the pathogenesis of ischaemic protection induced by remote ischaemic conditioning: Study of a human model of ischaemia-reperfusion induced vascular injury

Aims

We explored the effect of remote ischaemic conditioning (RIC) on endothelial function and on circulating mediators.

Mucosal bromodomain-containing protein 4 mediates aeroallergen-induced inflammation and remodeling

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Malignant melanoma in effusions: a source of false-negative cytodiagnoses

Melanoma, a not uncommon tumor, is associated with variable cytomorphology and unpredictable metastatic potential. Although most cytologic diagnoses of malignant melanoma represent metastatic disease, the diagnosis is frequently unsuspected clinically. Three effusions in which cells from metastatic melanomas were not diagnosed are described. Clinical factors that may have contributed to the erroneous cytodiagnoses are illustrated. Cytologic features and adjunctive studies that are helpful in identifying melanoma cells are discussed.     

Ultrastructure du fuseau neuro-musculaire chez l'homme

Summary The ultrastructure of the muscle spindles has been studied in human lumbrical muscles. The findings have been compared with the morphology of muscle spindles of rat and sheep examined with light and electron microscopy. The study is based on cross and longitudinal sections of the entire muscle spindle obtained by dissection. The different components of the spindle are described with special reference to the nuclear bag and nuclear chain fibres. These nuclei have been examined in human adult and newborn material and compared to the animal ones. ADN measurements revealed that although there are morphological differences between the two kinds of nuclei in human newborn spindles, the amount of ADN is the same as well in the nuclear bag as in the nuclear chain nuclei. Special attention is also given to the sensory and motor endings in the muscle spindles and to the presence of Pacinian corpuscules in these receptors. Finally two kinds of leptomeric organelles are described in human material.

     

Absence of aluminium in neurofibrillary tangles in Alzheimer''s disease

Using the new technique of nuclear microscopy, aluminium is not detected in pyramidal neurons in brain tissue from Alzheimer's disease (AD) patients. The analytical technique of nuclear microscopy can simultaneously image and analyse features in unstained and untreated tissue sections. In tissue which had been previously subjected to conventional procedures such as fixation and osmication, aluminium was observed in both neurons and surrounding tissue. This result shows that the analysis of tissue prepared using conventional chemical techniques may produce contamination or elemental redistribution, and supports our previous investigations which implied that aluminium is not involved in the aetiology of AD. In addition, significant increases in iron, phosphorus and sulphur concentrations were noted between neurons from Alzheimer tissue and neurons from age-matched controls, and between the supporting Alzheimer tissue and supporting control tissue, implying an overall increase in these elements. No significant increase in calcium was observed between neurons from Alzheimer tissue and neurons from age-matched controls.     

核转录因子-κB在缺氧预处理抑制心肌细胞凋亡中的作用

目的 :研究缺氧预处理 (hypoxicpreconditioning ,HPC)对于心肌细胞蛋白激酶C(PKC)和核转录因子κB (NF κB)表达的影响 ,及其在缺氧复氧诱导心肌细胞凋亡中的作用。方法 :在培养的SD乳鼠心肌细胞制作缺氧 /复氧 (H/R)模型 ,以荧光素染料Hoechst3 3 2 5 8测定心肌细胞凋亡率 ;制备心肌细胞蛋白提取物 ,以新PKCε亚型 (nPKCε)特异性抗体测定nPKCε相对蛋白含量 ;以抗NF κB抗体检测NF κB的表达 ;并以PKC抑制剂H7与心肌细胞预孵育后 ,观察H7对于HPC诱导的PKC和NF κB表达上调以及心肌细胞保护作用的影响。结果 :缺氧复氧造成心肌细胞凋亡 ,HPC可以降低心肌细胞H/R后凋亡率 ,并诱导nPKCε和NF κB表达上调 ;PKC抑制剂H7可以消除HPC诱导的PKC、NF κB表达上调和心肌细胞保护作用。结论 :HPC可以提高乳鼠心肌细胞对于H/R的耐受性 ,其机制涉及PKC介导的NF κB表达上调。     

低氧诱导因子1α诱导卵巢癌细胞周期阻滞的研究

目的：探讨低氧诱导因子1α（HIF-1α）对卵巢癌细胞周期的阻滞作用。方法: 采用化学性低氧诱导剂氯化钴（CoCl2）和物理性低氧培养箱两种方法对体外培养的卵巢癌SW626细胞诱导低氧，用诱骗法（decoy）阻断HIF-1α功能，Western blotting、RT-PCR和流式细胞术分别检测HIF-1α蛋白、mRNA的表达水平和细胞周期比率。结果： B1组(3.75±1.31)和C1组(3.48±1.01) HIF-1α蛋白表达水平明显高于A1组(0.97±0.31)（P<0.05), decoy法对HIF-1α蛋白表达没有明显影响(P>0.05)；A1组（0.65±0.32）和B1组（0.64±0.34）HIF-1α mRNA表达水平明显低于C1组（1.28±0.62）（P<0.05），decoy法对HIF-1α mRNA 表达没有明显影响（P>0.05）；流式细胞术检测发现B1组（81.78±24.33）和C1组（77.62±22.76）G0/G1期细胞比率显著高于A1组（49.49±18.54）（P<0.05）；B2组（61.54±20.84）明显低于B1组（P<0.05），C2组明显低于C1组（56.03±21.42），而A1组和A2组之间无明显差异（P>0.05）。结论：CoCl2或物理性低氧均能明显诱导卵巢癌细胞SW626 G0/G1期细胞周期阻滞和HIF-1α的表达，HIF-1α在低氧引起的卵巢癌细胞SW626的细胞周期阻滞中起重要作用。     

Loss of heterozygosity on chromosome 9q22.3 in microdissected basal cell carcinomas around the Semipalatinsk Nuclear Testing Site, Kazakhstan

A high incidence of skin cancers has been noted around the Semipalatinsk Nuclear Testing Site (SNTS) in Kazakhstan. Recently, basal cell carcinoma (BCC) susceptibility genes, human homolog of the Drosophila pathed gene (PTCH), and the xeroderma pigmentosa group A-complementing gene (XPA), have been cloned and localized on chromosome 9q22.3. To clarify the effect of low-dose irradiation on the occurrence of BCC, we used microdissection and polymerase chain reaction to identify loss of heterozygosity (LOH) at 9q22.3 using BCC samples obtained from this region. Ten Japanese samples were analyzed as controls. LOH with at least 1 marker was identified in 5 of 14 cases from around SNTS, whereas only 1 case with 1 marker was identified among the 10 Nagasaki cases. The total number of LOH alleles from SNTS (8 of 45) was significantly higher than the number from Nagasaki (1 of 26) (P = 0.03). The higher incidence of LOH on 9q22.3 in BCC from around SNTS suggests involvement of chronic low-dose irradiation by fallout from the test site as a factor in the cancers.     

C and V proteins of Sendai virus target signaling pathways leading to IRF-3 activation for the negative regulation of interferon-beta production

We here report a molecular basis for downregulation of interferon (IFN)-beta production by V and C proteins of Sendai virus (SeV). The infection of HeLa cells with SeV poorly induced IFN-beta even if the expression of C/C' was disrupted. In contrast, when the expression of C/C'/Y1/Y2 or V/W was disrupted, SeV infection strongly induced IFN-beta production and significantly activated the interferon regulatory factor (IRF)-3 pathway. The independent expression of C or V inhibited the double-stranded (ds) RNA- or Newcastle disease virus (NDV)-induced activation of IRF-3 and NF-kappa B, as well as the IFN-beta promoter. This inhibitory effect was also observed when Y1, Y2, or a C-terminal half fragment (aa 85-204) of C was independently expressed. Phosphorylation and homodimer formation of IRF-3 were suppressed not only in cells infected with SeV capable of expressing both C/C'/Y1/Y2 (or Y1/Y2) and V/W, but also in HeLa cells constitutively expressing Y1. These results suggest that C, Y1, Y2, and V block signaling pathways leading to IRF-3 activation to downregulate IFN-beta production.