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1.
ACh对人垂体腺瘤细胞内蛋白激酶C、胞内游离钙及cAMP/cGMP的影响 总被引:9,自引:2,他引:7
我们曾发现ACh可明显地抑制垂体腺瘤细胞的增殖代谢,为深入探讨ACh抑制垂体腺瘤细胞增殖作用的机制,观察了ACh作用后垂体腺瘤细胞内蛋白激酶C(PKC)、[Ca^2 ]i及cAMP/cGMP的变化。结果发现:(1)与空白处理组相比,使用PKC的激动剂PMA处理培养的人垂体腺瘤细胞时可使胞浆、胞膜和细胞总PKC活性浓度均升高,但ACh(10μmol/L)作用15min后,胞浆、胞膜和细胞总PKC活性均下降,且此作用可被阿托品阻断;(2)ACh(10μmol/L)作用于单个人垂体腺瘤细胞后,立即使垂体腺瘤细胞[Ca^2 ]i相对水平降低,但此作用可被阿托品阻断;(3)ACh作用于人垂体腺瘤细胞15min后,胞内cAMP水平均明显升高,而cGMP没有改变。该结果为探讨ACh抑制垂体腺瘤细胞增殖的分子机制提供了重要线索,同时提示,ACh对垂体瘤细胞增殖分化的调控作用是细胞内多信息系统相互整合的结果。 相似文献
2.
葡萄糖通过血脑屏障从血液中进入脑组织必须依赖葡萄糖转运蛋白(glucose transporter,GLUT)的帮助.GLUT1是血脑屏障上最主要的GLUT,也是脑毛细血管壁内皮细胞的分子标记.动物研究显示在急性脑缺血后脑内的GLUT1表达增加.检测了7例慢性微血管缺血性脑血管病变(ischemic cerebrovascular diseases,ICVD)的尸检脑组织中的GLUT1水平,并与11例同龄对照组比较.结果发现GLUT1水平在ICVD组中降低.其降低可能是由于低氧诱导因子-1α(hypoxia-induciblefactor-1α,HIF-1α)的下调所致.但是,在ICVD脑组织中的GLUT1水平降低不伴随有蛋白质O-GlcNAc糖基化水平的下降.上述结果为探讨脑缺血病变的机理提供了新线索. 相似文献
3.
菝葜属和肖菝葜属的核型变异和系统演化研究 总被引:1,自引:0,他引:1
基于体细胞染色体核型及花序特征对菝葜科Smilacaceae菝葜属Smilax和肖菝葜属Heterosmilax进行了系统演化研究,报道了国产菝葜科17个分类群的核型。根据已研究的部分形态学特征和已有的核型和分子序列资料,对它们的系统进化进行了分析。结果显示:(1)整个类群的核型变异表现在二型化、多倍化、染色体的微变异以及染色体基数递减(从16-15-13),16为菝葜类群的基本染色体基数。(2)草本菝葜的核型对称性在东亚到北美种类中,表现出从对称到不对称的变化,而木本菝葜的各组间并未表现出这种趋势。(3)先出叶(prophy11)是宿存的芽鳞,因此在菝葜组sect.China和土茯苓组sect.Coilanthus中具花序的分枝(该分枝基部具先出叶)与圆锥菝葜组sect.Macranthae和穗菝葜组sect.Smilax中着生叶腋的花序分枝或者具关节的单伞形花序是同源的;结合ITS资料,推测花序原始类型是具伞形花序无总花梗呈穗状排列的种类。从祖先类型,花序的分化朝两个方向:一为菝葜属的菝葜组和土茯苓组以及肖菝葜属的全部种类为代表的生于叶腋的单伞形花序,另一为菝葜属的圆锥菝葜组sect.Macranthae的全部种类构成的圆锥.伞形花序。(4)肖菝葜属的核型和ITS数据都表明其为非单系类群,与草本菝葜和土茯苓组成员为姐妹群,首次发现花被2/3联合的过渡类型——筐条菝葜S.corbularia,建议将肖菝葜属降为亚属,置于菝葜属。(5)核型特点支持草本菝葜是东亚起源,扩展到北美,与土茯苓组种类有共同祖先.来自于x=16的木本菝葜,赞同恢复草本组sect.Nemexia。(6)在广布种菝葜S.china中首次发现二倍体居群,已知其存在3种倍性(2x、4x和6x),发现不同倍性居群的分布规律,推测在第三纪至更新世中期日本、台湾岛与大陆分离之前,菝葜的叙居群已广泛分布,而目前广泛分布的缸居群是岛屿与大陆分离后形靠的。(7)我国西南是菝葜科现代分布和分化中心。 相似文献
4.
直立百部的一个新异名 总被引:1,自引:0,他引:1
根据对直立百部Stemona sessilifolia(Miq.)Miq.大量标本的研究和野外调查及引种栽培观察,结合对山东百部Stemona shandongensis D.K.Zang模式标本产地的调查,发现直立百部的形态性状是多变的。研究表明它的习性受生境影响而多变,从直立半灌木到蔓生都有;叶型多变;花通常出自叶腋,而花梗有时与叶柄,甚至主脉合生;内轮花被片大多明显大于外轮。山东百部的形态性状处于直立百部的变异范围内,因此作为独立的种是难以成立的,应处理为直立百部的新异名。 相似文献
5.
菝葜科种皮微结构特征及其分类学意义 总被引:6,自引:0,他引:6
在光学显微镜和扫描电镜下对菝葜科Smilacaceae3个属(菝葜属Smilax、肖菝葜属Heterosmilax和Ripogonum属)共53种5变种植物的种子形态及种皮微形态特征进行了研究。结果表明其种子形状为球形、半球形或钝三角形。在扫描电镜下种子表皮纹饰可分为7种类型,即脑纹型、粗脑纹型、网纹型、细网纹型、孔穴型、密孔穴型和细条纹型。根据种皮微形态的特征,对菝葜科内属间和属内组间的关系进行了探讨。种皮形态分析结果支持将Ripogonum属从菝葜科中分离、独立成科,支持将肖菝葜属与菝葜属合并的观点,这与孢粉学和分子证据的分析结果一致;推测肖菝葜属和菝葜属的土茯苓组sect.Coilanthus及草本组sect.Coprosmanthus的多数种类之间亲缘关系较近,菝葜组sect.China和圆锥组sect.Macranthae的大多数种类之间的亲缘关系较为密切,但种皮形态证据不支持Koyama将菝葜属分为6个组的观点。 相似文献
6.
Gong CX Liu F Wu G Rossie S Wegiel J Li L Grundke-Iqbal I Iqbal K 《Journal of neurochemistry》2004,88(2):298-310
Protein phosphatase 5 (PP5) is a 58-kDa novel phosphoseryl/phosphothreonyl protein phosphatase. It is ubiquitously expressed in all mammalian tissues examined, with a high level in the brain, but little is known about its physiological substrates. We found that this phosphatase dephosphorylated recombinant tau phosphorylated with cAMP-dependent protein kinase and glycogen synthase kinase-3beta, as well as abnormally hyperphosphorylated tau isolated from brains of patients with Alzheimer's disease. The specific activity of PP5 toward tau was comparable to those reported with other protein substrates examined to date. The PP5 activity toward tau was stimulated by arachidonic acid by 30- to 45-fold. Immunostaining demonstrated that PP5 was primarily cytoplasmic in PC12 cells and in neurons of postmortem human brain tissue. A small pool of PP5 associated with microtubules. Expression of active PP5 in PC12 cells resulted in reduced phosphorylation of tau, suggesting that PP5 can also dephosphorylate tau in cells. These results suggest that PP5 plays a role in the dephosphorylation of tau and might be involved in the molecular pathogenesis of Alzheimer's disease. 相似文献
7.
Tau蛋白过度磷酸化是Alzheimer病(Alzheimer disease, AD)的一个重要病理特征.采用 I 型糖尿病大鼠模型,研究胰岛素信号传导途径及葡萄糖代谢失调对tau蛋白过度磷酸化的形成机制进行探讨.以同龄Wistar大鼠做对照(CTL),胰腺大部分切除造低胰岛素组(PX),STZ较大剂量一次性注射造1型糖尿病模型即低胰岛素高血糖组(T1DM).葡萄糖氧化酶法检测血浆血糖,放免法检测血浆胰岛素,蛋白质印迹分析海马内总tau蛋白及tau蛋白上部分位点(Ser199、Thr212、Ser214、Ser396及Ser422)的磷酸化及神经细胞膜上葡萄糖转运子3(Glucose transport 3,GLUT3)水平.γ-32P-ATP和特异性底物肽检测海马内胰岛素信号传导系统中的关键酶糖原合成酶激酶-3β(Glycogen synthase kinase-3β, GSK-3β)活性.发现3组大鼠海马回总tau蛋白水平无显著差异,但以高血糖、低胰岛素血症为特征的T1DM组在tau蛋白Ser199、Thr212、Ser214、Ser396及Ser422位点上,呈现过度磷酸化状态,以低胰岛素血症为特征而血糖正常的PX组在位点Ser199、Thr212及Ser396上磷酸化程度比CTL组显著上升, 在位点Ser214及 Ser422上的磷酸化程度的改变不显著;T1DM及PX组大鼠海马 GSK-3β活性显著高于CTL组, 而GLUT3水平在T1DM和PX组均降低, 尤以T1DM组降低更显著.研究结果显示,胰岛素水平低下可能通过激活GSK-3β和下调细胞内葡萄糖代谢的双重作用引起脑内tau蛋白过度磷酸化. 相似文献
8.
? Premise of the study: Microsatellite primers were developed for the endangered Davidia involucrata to assess the population genetics and infer its evolutionary history. ? Methods and Results: Using both the modified magnetic bead hybridization method and the dual-suppression PCR method, we isolated and characterized 12 polymorphic microsatellite loci using 134 individuals from five populations in southwestern China. The number of alleles per locus ranged from six to 21 (mean = 10.8). The expected heterozygosity per locus ranged from 0.404 to 0.918 and observed heterozygosity ranged from 0.015 to 0.821. ? Conclusions: All of the 12 microsatellite markers developed for D. involucrata are polymorphic, and lay a solid foundation for further studies of the population genetics of this famous tree. 相似文献
9.
Shi J Zhang T Zhou C Chohan MO Gu X Wegiel J Zhou J Hwang YW Iqbal K Grundke-Iqbal I Gong CX Liu F 《The Journal of biological chemistry》2008,283(42):28660-28669
Two groups of tau, 3R- and 4R-tau, are generated by alternative splicing of tau exon 10. Normal adult human brain expresses equal levels of them. Disruption of the physiological balance is a common feature of several tauopathies. Very early in their life, individuals with Down syndrome (DS) develop Alzheimer-type tau pathology, the molecular basis for which is not fully understood. Here, we demonstrate that Dyrk1A, a kinase encoded by a gene in the DS critical region, phosphorylates alternative splicing factor (ASF) at Ser-227, Ser-234, and Ser-238, driving it into nuclear speckles and preventing it from facilitating tau exon 10 inclusion. The increased dosage of Dyrk1A in DS brain due to trisomy of chromosome 21 correlates to an increase in 3R-tau level, which on abnormal hyperphosphorylation and aggregation of tau results in neurofibrillary degeneration. Imbalance of 3R- and 4R-tau in DS brain by Dyrk1A-induced dysregulation of alternative splicing factor-mediated alternative splicing of tau exon 10 represents a novel mechanism of neurofibrillary degeneration and may help explain early onset tauopathy in individuals with DS. 相似文献
10.
微管相关蛋白MAP1b的生物学活性受其磷酸化修饰的调节,后者则受相应的蛋白激酶和蛋白磷酸酯酶(PP)调控.为研究蛋白磷酸酯酶在脑内对MAP1b磷酸化的调控作用,采用有代谢活性的大鼠脑片作为模型,分别应用冈田酸(okadaic acid)和cyclosporin A选择性地抑制PP2A 和PP2B活性,来研究其对脑内蛋白磷酸酯酶MAP1b磷酸化的调控.采用特异性的MAP1bⅠ型磷酸化依赖性抗体522和免疫印迹技术检测MAP1bⅠ型磷酸化.结果表明,当PP2A被okadaic acid选择性抑制后,MAP1bⅠ型磷酸化明显增加.而PP2B被选择性地抑制后,MAP1b磷酸化的变化不大.免疫组化染色显示,MAP1b广泛分布于鼠大脑神经元和突起中,与对照组相比,在PP2A抑制的脑片中抗体522的免疫活性在神经元中明显升高.上述结果表明,PP2A是脑中调控MAP1bⅠ型磷酸化的主要蛋白磷酸酯酶. 相似文献