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Camozzi M Rusnati M Bugatti A Bottazzi B Mantovani A Bastone A Inforzato A Vincenti S Bracci L Mastroianni D Presta M 《The Journal of biological chemistry》2006,281(32):22605-22613
Long-pentraxin 3 (PTX3) is a soluble pattern recognition receptor with non-redundant functions in inflammation and innate immunity. PTX3 comprises a pentraxin-like C-terminal domain involved in complement activation via C1q interaction and an N-terminal extension with unknown functions. PTX3 binds fibroblast growth factor-2 (FGF2), inhibiting its pro-angiogenic and pro-restenotic activity. Here, retroviral transduced endothelial cells (ECs) overexpressing the N-terminal fragment PTX3-(1-178) showed reduced mitogenic activity in response to FGF2. Accordingly, purified recombinant PTX3-(1-178) binds FGF2, prevents PTX3/FGF2 interaction, and inhibits FGF2 mitogenic activity in ECs. Also, the monoclonal antibody mAb-MNB4, which recognizes the PTX3-(87-99) epitope, prevents FGF2/PTX3 interaction and abolishes the FGF2 antagonist activity of PTX3. Consistently, the synthetic peptides PTX3-(82-110) and PTX3-(97-110) bind FGF2 and inhibit the interaction of FGF2 with PTX3 immobilized to a BIAcore sensor chip, FGF2-dependent EC proliferation, and angiogenesis in vivo. Thus, the data identify a FGF2-binding domain in the N-terminal extension of PTX3 spanning the PTX3-(97-110) region, pointing to a novel function for the N-terminal extension of PTX3 and underlining the complexity of the PTX3 molecule for modular humoral pattern recognition. 相似文献
108.
Lorenzi S Mattei F Sistigu A Bracci L Spadaro F Sanchez M Spada M Belardelli F Gabriele L Schiavoni G 《Journal of immunology (Baltimore, Md. : 1950)》2011,186(9):5142-5150
Cross-presentation is a crucial mechanism for generating CD8 T cell responses against exogenous Ags, such as dead cell-derived Ag, and is mainly fulfilled by CD8α(+) dendritic cells (DC). Apoptotic cell death occurring in steady-state conditions is largely tolerogenic, thus hampering the onset of effector CD8 T cell responses. Type I IFNs (IFN-I) have been shown to promote cross-priming of CD8 T cells against soluble or viral Ags, partly through stimulation of DC. By using UV-irradiated OVA-expressing mouse EG7 thymoma cells, we show that IFN-I promote intracellular Ag persistence in CD8α(+) DC that have engulfed apoptotic EG7 cells, regulating intracellular pH, thus enhancing cross-presentation of apoptotic EG7-derived OVA Ag by CD8α(+) DC. Notably, IFN-I also sustain the survival of Ag-bearing CD8α(+) DC by selective upmodulation of antiapoptotic genes and stimulate the activation of cross-presenting DC. The ensemble of these effects results in the induction of CD8 T cell effector response in vitro and in vivo. Overall, our data indicate that IFN-I cross-prime CD8 T cells against apoptotic cell-derived Ag both by licensing DC and by enhancing cross-presentation. 相似文献
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Jia?Nee Foo Karin?E. Smedby Nicholas?K. Akers Mattias Berglund Ishak?D. Irwan Xiaoming Jia Yi Li Lucia Conde Hatef Darabi Paige?M. Bracci Mads Melbye Hans-Olov Adami Bengt Glimelius Chiea?Chuen Khor Henrik Hjalgrim Leonid Padyukov Keith Humphreys Gunilla Enblad Christine?F. Skibola Paul?I.W. de?Bakker Jianjun Liu 《American journal of human genetics》2013,93(1):167-172
Non-Hodgkin lymphoma represents a diverse group of blood malignancies, of which follicular lymphoma (FL) is a common subtype. Previous genome-wide association studies (GWASs) have identified in the human leukocyte antigen (HLA) class II region multiple independent SNPs that are significantly associated with FL risk. To dissect these signals and determine whether coding variants in HLA genes are responsible for the associations, we conducted imputation, HLA typing, and sequencing in three independent populations for a total of 689 cases and 2,446 controls. We identified a hexa-allelic amino acid polymorphism at position 13 of the HLA-DR beta chain that showed the strongest association with FL within the major histocompatibility complex (MHC) region (multiallelic p = 2.3 × 10−15). Out of six possible amino acids that occurred at that position within the population, we classified two as high risk (Tyr and Phe), two as low risk (Ser and Arg), and two as moderate risk (His and Gly). There was a 4.2-fold difference in risk (95% confidence interval = 2.9–6.1) between subjects carrying two alleles encoding high-risk amino acids and those carrying two alleles encoding low-risk amino acids (p = 1.01 × 10−14). This coding variant might explain the complex SNP associations identified by GWASs and suggests a common HLA-DR antigen-driven mechanism for the pathogenesis of FL and rheumatoid arthritis. 相似文献
110.
Molecular evolution of mammalian aquaporin-2: further evidence that elephant shrew and aardvark join the paenungulate clade 总被引:1,自引:1,他引:0
Madsen O; Deen PM; Pesole G; Saccone C; de Jong WW 《Molecular biology and evolution》1997,14(4):363-371
A 328-bp sequence from exon 1 of the gene for aquaporin-2 (AQP2) was
compared in 12 mammalian species, representing as many eutherian orders.
This sequence encodes the N-terminal half of this kidney- specific water
channel protein. Most amino acid replacements, as well as an insertion,
have occurred in extracellular loops connecting the transmembrane helices,
in agreement with a lower functional importance of these loops.
Phylogenetic analyses were performed with parsimony, distance, and
maximum-likelihood methods. The AQP2 data set, alone as well as in
combination with previously published alpha A-crystallin protein sequences,
strongly supports a clade consisting of elephant, hyrax, aardvark, and
elephant shrew, reaching bootstrap values of 99%. This finding fully agrees
with the only other presently available sequence data sets that include
these taxa, those of von Willebrand factor and interphotoreceptor
retinoid-binding protein, and suggests that this extended paenungulate
clade is one of the most conspicuous superordinal groupings in eutherian
phylogeny. Some support was obtained for an artiodactyl/perissodactyl
clade, while the grouping of pholidotes with edentates was contradicted.
相似文献