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71.
Davi Fernando Back Gelson Manzoni de Oliveira Marco Aurélio Ballin 《Inorganica chimica acta》2010,363(4):807-166
UO2(NO3)2·6H2O and VO(acac)2 react with 2-(2′-hydroxylphenyl)benzoxazole (Hpbx) in methanol to give [UO2(pbx)2(CH3OH)] (1) and [VO(pbx)2] (2). Complex 1 shows a distorted pentagonal bipyrimidal geometry, characteristic for the coordination number 7. Reciprocal OH?O interactions between neighbored molecules hold 1 in a pseudo-dimeric association with an inversion center. Complex 2 achieves a distorted octahedral geometry and the molecules “stack” along the b axis through secondary interactions. The molecule heaping is wholly linear, with Vn′−O(1)n′?V x′ angles of 180°. Luminescence properties of Hpbx, 1 and 2 are discussed. 相似文献
72.
Erika Garay Genaro Patiño‐López Socorro Islas Lourdes Alarcón Elsy Canche‐Pool Ricardo Valle‐Rios Oscar Medina‐Contreras Giovana Granados Bibiana Chávez‐Munguía Eusebio Juaristi Vianney Ortiz‐Navarrete Lorenza González‐Mariscal 《Journal of cellular biochemistry》2010,111(1):111-122
Class I‐restricted T cell associated molecule (CRTAM) is a member of the immunoglobulin superfamily that complies with the structural characteristics of the JAM family of proteins and is phylogenetically more closely related to nectin‐like proteins. Here we demonstrate for the first time, that CRTAM is expressed in epithelial cells along the lateral membrane and is important for early cell–cell contacts and cell–substrate interactions. CRTAM is sensitive to intermediate filament disruption and treatment of monolayers with soluble CRTAM enhances cell–cell dissociation and lowers transepithelial electrical resistance. Incubation of newly plated cells with anti‐CRTAM antibody decreases the formation of cell aggregates and promotes cell detachment. Co‐cultures of epithelial cells and fibroblasts that lack CRTAM expression and in vitro binding assays, demonstrate the participation of CRTAM in homotypic and heterotypic trans‐interactions. Hence we conclude that CRTAM is a molecule involved in epithelial cell adhesion. J. Cell. Biochem. 111: 111–122, 2010. © 2010 Wiley‐Liss, Inc. 相似文献
73.
74.
Manfredo Hörner Gelson Manzoni de Oliveira Leandro Bresolin Adriano Bof de Oliveira 《Inorganica chimica acta》2006,359(14):4631-4634
Deprotonated 1,3-bis(4-nitrophenyl)triazene reacts with an aqueous solution of TlNO3 to give dark-red crystals of {[TlI(RC6H4NNNC6H4R)]2}n [R = p-NO2], a symmetric-substituted triazenide complex “polymer” of TlI. The centrosymmetric tectons [TlI(RC6H4NNNC6H4R)]2 are related by translation and attain unidimensional chains along the c-axis through Tl?O bonding. The supramolecular bidimensional (2D) assembling of the dimeric tectons is achieved through weak secondary π-interactions of the type Tl-η2-arene between the unidimensional chains. 相似文献
75.
Barreiro Arcos ML Gorelik G Klecha A Genaro AM Cremaschi GA 《American journal of physiology. Cell physiology》2006,291(2):C327-C336
Regulation of cell proliferation by thyroid hormone (TH) has been demonstrated, but the effect of THs and the mechanisms involved in lymphocyte activity have not been elucidated. Differential expression of PKC isoenzymes and high nitric oxide synthase (NOS) activity have been described in tumor T lymphocytes. We have analyzed the direct actions of TH on normal T lymphocytes and BW5147 T lymphoma cells in relation to PKC and NOS activities. THs increased tumor and mitogen-induced normal T lymphocyte proliferation. PKC isoenzyme-selective blockers impaired these effects in both cell types, indicating the participation of Ca2+-dependent and -independent isoenzymes in normal and tumor cells, respectively. TH actions were blunted by extra- and intracellular Ca2+ blockers only in normal T lymphocytes, whereas NOS blockers impaired TH-induced proliferation in T lymphoma cells. Incubation for 24 h with TH induced a rise in total and membrane-associated PKC activities in both cell types and led to a rapid and transient effect only in tumor cells. THs increased atypical PKC-zeta expression in BW5147 cells and classical PKC isoenzymes in mitogen-stimulated normal T cells. TH augmented NOS activity and inducible NOS protein and gene expression only in tumor cells. Blockade of PKC and the atypical PKC-zeta isoform inhibited TH-mediated stimulation of inducible NOS and cell proliferation. These results show, for the first time, that differential intracellular signals are involved in TH modulation of lymphocyte physiology and pathophysiology. 相似文献
76.
de la Torre E Genaro AM Ribeiro ML Pagotto R Pignataro OP Sales ME 《Biochimica et biophysica acta》2008,1782(2):82-89
Macrophages (Mps) are essential cellular components of the innate immune system. They are released from the bone marrow as immature monocytes and after circulating in the blood stream, migrate into tissues to undergo final differentiation into resident Mps. In general terms Mps behavior in breast tumors, was described as being either for or against tumor growth. Under certain well defined circumstances Mps are able to kill cells in two ways: direct tumor cytotoxicity or antibody dependent cytotoxicity. We had previously demonstrated that peritoneal Mps from LMM3 mammary tumor bearing mice (TMps) enhanced in vivo the LMM3 induced angiogenesis, promoting tumor growth while Mps from normal BALB/c mice (NMps) did not. In this work, we demonstrate that Mps, expressing functional muscarinic acetylcholine receptors, are able to proliferate in vitro in response to the muscarinic agonist carbachol. These peritoneal cells use two distinct metabolic pathways: TMps are primed by tumor presence and they proliferate mainly by activating arginase pathway and by producing high levels of prostaglandin E(2) via M(1)-M(3) receptors activation. In NMps, carbachol stimulates M(2) receptors function, triggering protein kinase C activity and induces moderate prostaglandin E(2) liberation via M(1) receptor. 相似文献
77.
Gelson Manzoni de Oliveira Manfredo Hörner Aline Machado Jorge H.S.K. Monteiro 《Inorganica chimica acta》2011,366(1):203-859
Deprotonated 3-(4-nitrophenyl)-1-phenyltriazene N-oxide reacts with YCl3·6H2O and LnCl3·6H2O (Ln = Eu, Ho, Yb) to give the monoclinic chelate complexes [Y{O2N(C6H4)NNN(O)Ph}4](Et3NH)·H2O (1) (Ph = C6H5; Et = C2H5) and [LnIII{O2N(C6H4)NNN(O)Ph}4](Et3NH)·H2O·{CH3OH∗} {LnIII = Eu (2), Ho (3), Yb∗ (4), in which the metal centers present a square antiprismatic configuration. As already observed for hydrated ammonium complexes of triazene-oxides ligands with (C6H4)−NO2 groups, multiple, effective O···H and N···H interactions hold the species in supramolecular 3D assemblies. The optical and the luminescent properties of the triazene-oxide europium complex 2 are also presented and fully discussed. 相似文献
78.
Paola Llanos Ariel Contreras-Ferrat Genaro Barrientos Marco Valencia David Mears Cecilia Hidalgo 《PloS one》2015,10(6)
Glucose-stimulated insulin secretion (GSIS) from pancreatic β-cells requires an increase in intracellular free Ca2+ concentration ([Ca2+]). Glucose uptake into β-cells promotes Ca2+ influx and reactive oxygen species (ROS) generation. In other cell types, Ca2+ and ROS jointly induce Ca2+ release mediated by ryanodine receptor (RyR) channels. Therefore, we explored here if RyR-mediated Ca2+ release contributes to GSIS in β-cell islets isolated from male rats. Stimulatory glucose increased islet insulin secretion, and promoted ROS generation in islets and dissociated β-cells. Conventional PCR assays and immunostaining confirmed that β-cells express RyR2, the cardiac RyR isoform. Extended incubation of β-cell islets with inhibitory ryanodine suppressed GSIS; so did the antioxidant N-acetyl cysteine (NAC), which also decreased insulin secretion induced by glucose plus caffeine. Inhibitory ryanodine or NAC did not affect insulin secretion induced by glucose plus carbachol, which engages inositol 1,4,5-trisphosphate receptors. Incubation of islets with H2O2 in basal glucose increased insulin secretion 2-fold. Inhibitory ryanodine significantly decreased H2O2-stimulated insulin secretion and prevented the 4.5-fold increase of cytoplasmic [Ca2+] produced by incubation of dissociated β-cells with H2O2. Addition of stimulatory glucose or H2O2 (in basal glucose) to β-cells disaggregated from islets increased RyR2 S-glutathionylation to similar levels, measured by a proximity ligation assay; in contrast, NAC significantly reduced the RyR2 S-glutathionylation increase produced by stimulatory glucose. We propose that RyR2-mediated Ca2+ release, induced by the concomitant increases in [Ca2+] and ROS produced by stimulatory glucose, is an essential step in GSIS. 相似文献
79.
Zorrilla Zubilete MA Guelman LR Maur DG Caceres LG Rios H Zieher LM Genaro AM 《Neurochemistry international》2011,58(3):273-280
Acute and long-term complications can occur in patients receiving radiation therapy. It has been suggested that cytoprotection might decrease the incidence and severity of therapy-related toxicity in these patients. Developing cerebellum is highly radiosensitive and for that reason it is a useful structure to test potential neuroprotective substances to prevent radiation induced abnormalities. Recent studies have shown that estrogen can rapidly modulate intracellular signalling pathways involved in cell survival. Thus, it has been demonstrated that estrogens mediate neuroprotection by promoting growth, cell survival and by preventing axonal pruning. The aim of this work was to evaluate the effect of the treatment with 17-β-estradiol on the motor, structural and biochemical changes induced by neonatal ionizing radiation exposure, and to investigate the participation of nitric oxide and protein kinase C, two important intracellular messengers involved in neuronal activity. Our results show that perinatal chronic 17-β-estradiol treatment partially protects against radiation-induced cerebellar disorganization and motor abnormalities. PKC and NOS activities could be implicated in its neuroprotective mechanisms. These data provide new evidence about the mechanisms underlying estrogen neuroprotection, which could have therapeutic relevance for patients treated with radiotherapy. 相似文献
80.
The modular nature of repeat proteins makes them a versatile platform for the design of smart materials with predetermined properties. Here, we present a general strategy for combining protein modules with specified stability and function into arrays for the assembly of stimuli-responsive gels. We have designed tetratricopeptide repeat (TPR) arrays which contain peptide-binding modules that specify the strength and reversibility of network crosslinking in combination with spacer modules that specify crosslinking geometry and overall stability of the array. By combining such arrays with multivalent peptide ligands, self-supporting stimuli-responsive gels are formed. Using microrheology, we characterized the kinetics of gelation as a function of concentration and stoichiometry of the components. We also show that such gels are effective in encapsulating and releasing small molecules. Moreover, TPR gels alone are fully compatible with cell growth, whereas gels loaded with an anticancer compound release the compound, resulting in cell death. Thus, we have demonstrated that this new class of tunable biomaterials is ripe for further development as tissue engineering and drug delivery platform. 相似文献