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Sandmann J  Schwedhelm KS  Tsikas D 《FEBS letters》2005,579(19):4119-4124
The transport of various S-nitrosothiols, NO and NO donors in human red blood cells (RBC) and the formation of erythrocytic S-nitrosoglutathione were investigated. Of the NO species tested only S-nitrosocysteine was found to form S-nitrosoglutathione in the RBC cytosol. L-Serine, L-cysteine and L-lysine inhibited formation of S-nitrosoglutathione. Incubation of RBC pre-incubated with S-[15N]nitroso-L-cysteine with native plasma or platelet-rich plasma led to formation of S-[15N]nitrosoalbumin and inhibited platelet aggregation, respectively. The specific transporter system of S-nitroso-L-cysteine in the RBC membrane may have implications for formation of S-nitrosoalbumin and S-nitrosohemoglobin and for transport of NO bioactivity within the vasculature.  相似文献   
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Plants rely on different immune receptors to recognize pathogens and defend against pathogen attacks. Nucleotide‐binding domain and leucine‐rich repeat (NLR) proteins play a major role as intracellular immune receptors. Their homeostasis must be maintained at optimal levels in order to effectively recognize pathogens without causing autoimmunity. Previous studies have shown that the activity of the ubiquitin‐proteasome system is essential to prevent excessive accumulation of NLR proteins such as Suppressor of NPR1, Constitutive 1 (SNC1). Attenuation of the ubiquitin E3 ligase SCFCPR1 (Constitutive expressor of Pathogenesis Related genes 1) or the E4 protein MUSE3 (Mutant, SNC1‐Enhancing 3) leads to NLR accumulation and autoimmunity. In the current study, we report the identification of AtCDC48A as a negative regulator of NLR‐mediated immunity. Plants carrying Atcdc48A‐4, a partial loss‐of‐function allele of AtCDC48A, exhibit dwarf morphology and enhanced disease resistance to the oomycete pathogen Hyaloperonospora arabidopsidis (H.a.) Noco2. The SNC1 level is increased in Atcdc48A‐4 plants and AtCDC48A interacts with MUSE3 in co‐immunoprecipitation experiments, supporting a role for AtCDC48A in NLR turnover. While Arabidopsis contains four other paralogs of AtCDC48A, knockout mutants of these genes do not show obvious immunity‐related phenotypes, suggesting functional divergence within this family. As an AAA‐ATPase, AtCDC48A likely serves to process the poly‐ubiquitinated NLR substrate for final protein degradation by the 26S proteasome.  相似文献   
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The Rhodopsin family is a class of integral membrane proteins belonging to G protein-coupled receptors (GPCRs). To date, several orphan GPCRs are still uncharacterized and in this study we present an anatomical characterization of the GPR162 protein and an attempt to describe its functional role. Our results show that GPR162 is widely expressed in GABAergic as well as other neurons within the mouse hippocampus, whereas extensive expression is observed in areas related to energy homeostasis and hedonic feeding such as hypothalamus, amygdala and ventral tegmental area, regions known to be involved in the regulation of palatable food consumption.  相似文献   
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Lin YY  Wu DM  Liu L  Liu QH  Yan ZY  Wu BW 《生理学报》2008,60(1):38-42
本研究采用全细胞膜片钳技术观察了SNCl62(一种选择性δ阿片受体激动剂)对人鼠心室肌细胞L型钙电流(L-type Ca2 current,ICa-L)和瞬时外向钾电流(transient outward K current,Ito)的影响.结果显示,SNCl62明显抑制大鼠心室肌细胞,Ica L和Ica L,对Ica L.和k的最大抑制率分别为(46.13±4.12)%和(36.53±10.57)%.1x10-4mol/L SNCl62使,Ica L的甲均电流密度从(8.98±0.40)pA/pF下降到(4.84±0.44)pA/pF(P<0.01,n=5),Ito的平均电流密度从(18.69±2.42)pA/pF降低到(11.73±1.67)pA/pF(P<0.01,n=5).单独应用naltrindole(一种选择性δ阿片受体拮抗剂)对大鼠心室肌细胞Ica L和Ito无显著作用,但预先应用naltrindole可以消除SNCl62对Ica L和Ito的抑制作用.结果表明,通过δ阿片受体,SNCl62(1x10-6~1x10-4mol/L)浓度依赖性地抑制人鼠心室肌细胞Ica L和Ito这可能是激动δ阿片受体产生抗心律失常效应的重要机制.  相似文献   
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Heat shock proteins (HSPs) serve as molecular chaperones for diverse client proteins in many biological processes. In plant immunity, cytosolic HSP90s participate in the assembly, stability control and/or activation of immune receptor complexes. In this paper we report that in addition to the well‐established positive roles that HSP90 isoforms play in plant immunity, they are also involved in the negative regulation of immune receptor accumulation. Point mutations in two HSP90 genes, HSP90.2 and HSP90.3, were identified from a forward genetic screen designed to isolate mutants with enhanced disease resistance. We found that specific mutations in HSP90.2 and HSP90.3 lead to heightened accumulation of immune receptors, including SNC1, RPS2 and RPS4. HSP90s may assist SGT1 in the formation of SCF E3 ubiquitin ligase complexes that target immune receptors for degradation. Such regulation is critical for maintaining appropriate levels of immune receptor proteins to avoid autoimmunity.  相似文献   
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Heavy Metals Modulate Glutamatergic System in Human Platelets   总被引:3,自引:0,他引:3  
Research strategies have been developed to characterize parameters in peripheral tissues that might easily be measured in humans as surrogate markers of damage, dysfunction or interactions involving neural targets of toxicants. The similarities between platelet and neuron may even be clinically important, as a number of biochemical markers show parallel changes in the central nervous system (CNS) and platelets. The purpose of our research was to investigate the effect of Hg2+, Pb2+ and Cd2+ on the [3H]-glutamate binding and [3H]-glutamate uptake in human platelets. The involvement of oxidative stress in the modulation of glutamatergic system induced by heavy metals was also investigated. The present study clearly demonstrates that Hg2+, Cd2+, and Pb2+ inhibited [3H]-glutamate uptake in human platelets. Hg2+ inhibited [3H]-glutamate binding, while Cd2+ and Pb2+ stimulated [3H]-glutamate binding in human platelets. Hg2+, Cd2+ and Pb2+ increased lipid peroxidation levels and reactive oxygen species (ROS) measurement in platelets. The present limited results could suggest that glutamatergic system may be used as a potential biomarker for neurotoxic action of heavy metals in humans.  相似文献   
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