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Z. Yao A. Lattermann A. Volgger A. McNicholas G. Mueller-Eckhardt E. D. Albert 《Immunogenetics》1995,41(6):387-387
The name B
*4406 was officially assigned by the WHO Nomenclature Committee in February 1995. This follows the agreed policy that, subject to the conditions stated in the most recent Nomenclature Report (Bodmer et al. 1994), names will be assigned to new sequences as they are identified. Lists of such new names will be published in the following WHO Nomenclature Report. The nucleotide sequences reported in this Papers have been submitted to the EMBL nucleotide sequence database and have been assigned the accession numbers X83400 (HLA-B promoter region), X83401 (exon 1), X83402 (exon 2), and X83403 (exon 3) 相似文献
13.
Zych AJ Lam SQ Jenkins DM Herr RJ Ting PC Lee JF Kuang R Wu H Kim DW Aslanian RG Wainhaus S Black TA Cacciapuoti A McNicholas PM Xu Y Walker SS 《Bioorganic & medicinal chemistry letters》2012,22(14):4896-4899
The structure-activity relationship studies of a novel sulfonylurea series of piperazine pyridazine-based small molecule glucan synthase inhibitors is described. The optimization of PK profiles within the series led to the discovery of several compounds with improved pharmacokinetic profiles which demonstrated in vitro potency against clinically relevant strains. However, the advancement of compounds from this series into a non-lethal systemic fungal infection model failed to show in vivo efficacy. 相似文献
14.
R Kuang H Wu PC Ting RG Aslanian J Cao DW Kim JF Lee J Schwerdt G Zhou R Jason Herr AJ Zych J Yang SQ Lam DM Jenkins SA Sakwa S Wainhaus TA Black A Cacciapuoti PM McNicholas Y Xu SS Walker 《Bioorganic & medicinal chemistry letters》2012,22(16):5268-5271
A detailed structure-activity relationship study of a novel series of pyridazine-based small molecule glucan synthase inhibitors is described. The optimization of the PK profile of this series led to the discovery of compound 11g, which demonstrated in vivo potency ip in a lethal fungal infection model. 相似文献
15.
Anne S Rasmussen Henrik Lauridsen Christoffer Laustsen Bjarke G Jensen Steen F Pedersen Lars Uhrenholt Lene WT Boel Niels Uldbjerg Tobias Wang Michael Pedersen 《BMC physiology》2010,10(1):3
Background
In biomedical sciences, ex vivo angiography is a practical mean to elucidate vascular structures three-dimensionally with simultaneous estimation of intravascular volume. The objectives of this study were to develop a magnetic resonance (MR) method for ex vivo angiography and to compare the findings with computed tomography (CT). To demonstrate the usefulness of this method, examples are provided from four different tissues and species: the human placenta, a rice field eel, a porcine heart and a turtle. 相似文献16.
Paralogous origin of the red- and green-sensitive visual pigment genes in vertebrates 总被引:1,自引:0,他引:1
The nucleotide sequence of the red-sensitive visual pigment gene, R007Af,
in the fish Astyanax fasciatus, from the initiation codon to the stop codon
of this gene, including introns, is 1,592 bp, making it the shortest visual
pigment gene known in vertebrates. Analysis of this and other homologous
sequence data suggests that vertebrates initially had two duplicate genes
and that each ancestor of Astyanax, human, and chicken independently
duplicated the gene in the process of developing their red-green color
vision. Furthermore, many extant red-green colorblind organisms may be
explained simply by the failure of achieving very specific nucleotide
substitutions at the three codon positions 180, 277, and 285, rather than
by the lack of duplicate loci.
相似文献
17.
Unusual molecular evolution of an Adh pseudogene in Drosophila 总被引:2,自引:0,他引:2
Sullivan DT; Starmer WT; Curtiss SW; Menotti-Raymond M; Yum J 《Molecular biology and evolution》1994,11(3):443-458
18.
Supramolecular structures of peptide assemblies in membranes by neutron off-plane scattering: method of analysis 总被引:2,自引:1,他引:1 下载免费PDF全文
In a previous paper (Yang et al., Biophys. J. 75:641-645, 1998), we showed a simple, efficient method of recording the diffraction patterns of supramolecular peptide assemblies in membranes where the samples were prepared in the form of oriented multilayers. Here we develop a method of analysis based on the diffraction theory of two-dimensional liquids. Gramicidin was used as a prototype model because its pore structure in membrane in known. At full hydration, the diffraction patterns of alamethicin and magainin are similar to gramicidin except in the scale of q (the momentum transfer of scattering), clearly indicating that both alamethicin and magainin form pores in membranes but of different sizes. When the hydration of the multilayer samples was decreased while the bilayers were still fluid, the in-plane positions of the membrane pores became correlated from one bilayer to the next. We believe that this is a new manifestation of the hydration force. The effect is most prominent in magainin patterns, which are used to demonstrate the method of analysis. When magainin samples were further dehydrated or cooled, the liquid-like diffraction turned into crystal-like patterns. This discovery points to the possibility of investigating the supramolecular structures with high-order diffraction. 相似文献
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