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991.
Lovastatin, an inhibitor of HMG-CoA reductase, lowers cholesterol saturation of bile. To determine the mechanism of this effect and further define the role of cholesterol synthesis in regulation of biliary lipid metabolism, we studied ten human volunteers in a control period and again after 5-6 weeks on lovastatin, 40 mg b.i.d. Mean sterol production from acetate in mononuclear leukocytes fell from 1.18 to 0.84 pmol/min per 10(6) cells on lovastatin (P less than 0.02). Concomitantly there was reduction in mean biliary secretion of cholesterol from 143 to 96 mumol/h (P less than 0.02). On lovastatin, mean pool size of bile acids by the Lindstedt method fell from 3193 to 2917 mumol (one-sided P = 0.05) and mean pool size by the one-sample method fell from 5158 to 4091 mumol (P less than 0.002). Lovastatin had no effect on mean fractional turnover rate of either cholic acid (0.77 vs. 0.74 day-1) or chenodeoxycholic acid (0.51 vs. 0.54 day-1). Mean total bile acid synthesis was lower on lovastatin (1443 vs. 1240 mumol/day), but the difference did not quite achieve statistical significance. In humans, inhibition of cholesterol synthesis by lovastatin lowers biliary cholesterol saturation by reducing cholesterol secretion into bile. Bile acid pool size, and perhaps bile acid synthesis, are also reduced by this inhibition. 相似文献
992.
Kentaro Kato Daijiro Konno Martin Berry Fumio Matsuzaki Ann Logan Alicia Hidalgo 《PloS one》2015,10(12)
Central nervous system injury induces a regenerative response in ensheathing glial cells comprising cell proliferation, spontaneous axonal remyelination, and limited functional recovery, but the molecular mechanisms are not fully understood. In Drosophila, this involves the genes prospero and Notch controlling the balance between glial proliferation and differentiation, and manipulating their levels in glia can switch the response to injury from prevention to promotion of repair. In the mouse, Notch1 maintains NG2 oligodendrocyte progenitor cells (OPCs) in a progenitor state, but what factor may enable oligodendrocyte (OL) differentiation and functional remyelination is not understood. Here, we asked whether the mammalian homologue of prospero, Prox1, is involved. Our data show that Prox1 is distributed in NG2+ OPCs and in OLs in primary cultured cells, and in the mouse spinal cord in vivo. siRNA prox1 knockdown in primary OPCs increased cell proliferation, increased NG2+ OPC cell number and decreased CC1+ OL number. Prox1 conditional knockout in the OL cell lineage in mice increased NG2+ OPC cell number, and decreased CC1+ OL number. Lysolecithin-induced demyelination injury caused a reduction in CC1+ OLs in homozygous Prox1-/- conditional knockout mice compared to controls. Remarkably, Prox1-/- conditional knockout mice had smaller lesions than controls. Altogether, these data show that Prox1 is required to inhibit OPC proliferation and for OL differentiation, and could be a relevant component of the regenerative glial response. Therapeutic uses of glia and stem cells to promote regeneration and repair after central nervous system injury would benefit from manipulating Prox1. 相似文献
993.
Gene-Jack Wang Dardo Tomasi Antonio Convit Jean Logan Christopher T. Wong Elena Shumay Joanna S. Fowler Nora D. Volkow 《PloS one》2014,9(7)
Objective
Dopamine mediates the rewarding effects of food that can lead to overeating and obesity, which then trigger metabolic neuroadaptations that further perpetuate excessive food consumption. We tested the hypothesis that the dopamine response to calorie intake (independent of palatability) in striatal brain regions is attenuated with increases in weight.Method
We used positron emission tomography with [11C]raclopride to measure dopamine changes triggered by calorie intake by contrasting the effects of an artificial sweetener (sucralose) devoid of calories to that of glucose to assess their association with body mass index (BMI) in nineteen healthy participants (BMI range 21–35).Results
Neither the measured blood glucose concentrations prior to the sucralose and the glucose challenge days, nor the glucose concentrations following the glucose challenge vary as a function of BMI. In contrast the dopamine changes in ventral striatum (assessed as changes in non-displaceable binding potential of [11C]raclopride) triggered by calorie intake (contrast glucose – sucralose) were significantly correlated with BMI (r = 0.68) indicating opposite responses in lean than in obese individuals. Specifically whereas in normal weight individuals (BMI <25) consumption of calories was associated with increases in dopamine in the ventral striatum in obese individuals it was associated with decreases in dopamine.Conclusion
These findings show reduced dopamine release in ventral striatum with calorie consumption in obese subjects, which might contribute to their excessive food intake to compensate for the deficit between the expected and the actual response to food consumption. 相似文献994.
Point-of-use filters containing granular activated carbon (GAC) are an effective method for removing certain chemicals from water, but their ability to remove bacteria and viruses has been relatively untested. Collision efficiencies (alpha) were determined using clean-bed filtration theory for two bacteria (Raoutella terrigena 33257 and Escherichia coli 25922), a bacteriophage (MS2), and latex microspheres for four GAC samples. These GAC samples had particle size distributions that were bimodal, but only a single particle diameter can be used in the filtration equation. Therefore, consistent with previous reports, we used a particle diameter based on the smallest diameter of the particles (derived from the projected areas of 10% of the smallest particles). The bacterial collision efficiencies calculated using the filtration model were high (0.8 < or = alpha < or = 4.9), indicating that GAC was an effective capture material. Collision efficiencies greater than unity reflect an underestimation of the collision frequency, likely as a result of particle roughness and wide GAC size distributions. The collision efficiencies for microspheres (0.7 < or = alpha < or = 3.5) were similar to those obtained for bacteria, suggesting that the microspheres were a reasonable surrogate for the bacteria. The bacteriophage collision efficiencies ranged from > or = 0.2 to < or = 0.4. The predicted levels of removal for 1-cm-thick carbon beds ranged from 0.8 to 3 log for the bacteria and from 0.3 to 1.0 log for the phage. These tests demonstrated that GAC can be an effective material for removal of bacteria and phage and that GAC particle size is a more important factor than relative stickiness for effective particle removal. 相似文献
995.
J. S. Fowler J. Logan Y.-S. Ding D. Franceschi G.J. Wang N. D. Volkow N. Pappas D. Schlyer S. J. Gatley D. Alexoff C. Felder A. Biegon† W. Zhu‡ 《Journal of neurochemistry》2001,79(5):1039-1046
Clorgyline is an irreversible inhibitor of monoamine oxidase (MAO A) which has been labeled with carbon-11 (C-11) and used to measure human brain MAO A with positron emission tomography (PET). In this study we compared [11C]clorgyline and deuterium-substituted [11C]clorgyline ([11C]clorgyline-D2) to better understand the molecular link between [11C]clorgyline binding and MAO A. In PET studies of five normal healthy volunteers scanned with [11C]clorgyline and [11C]clorgyline-D2 2 h apart, deuterium substitution generally produced the expected reductions in the brain uptake of [11C]clorgyline. However, the reduction was not uniform with the C-11 binding in white matter being significantly less sensitive to deuterium substitution than other brain regions. The percentages of the total binding attributable to MAO A is largest for the thalamus and smallest for the white matter and this is clearly seen in PET images with [11C]clorgyline-D2. Thus deuterium-substituted [11C]clorgyline selectively reduces the MAO A binding component of clorgyline in the human brain revealing non-MAO A binding which is most apparent in the white matter. The characterization of the non-MAO A binding component of this widely used MAO A inhibitor merits further investigation. 相似文献
996.
David P. Logan 《New Zealand journal of zoology.》2019,46(3):236-252
Larvae of the endemic dynastine scarabs Pericoptus truncatus and P. punctatus (Coleoptera: Scarabaeidae) occur in coastal sand dunes. Life cycles from egg to egg-laying adults were determined by rearing for the first time. They were 3–5 years (mean?±?SD?=?3.41?±?0.53 years, n?=?172) and 2–4 years (2.90?±?0.45 years, n?=?53) for P. truncatus and P. punctatus, respectively. The modal life cycle length was three years for both species. In the first year of development, survival of P. truncatus and P. punctatus was superior when larvae were provided with driftwood than with grass (Spinifex sericeus or Stenotaphrum secundatum). Head-capsule width could be used to reliably differentiate between instars of P. punctatus and P. truncatus except for second instar P. truncatus and third instar P. punctatus. These data may inform planning to protect sand scarabs and associated fauna of coastal sand dunes. 相似文献
997.
David Skelton Abbey Goodyear DaQun Ni Wendy J. Walton Myron Rolle Joan T. Hare Timothy M. Logan 《Journal of biomolecular NMR》2010,48(2):93-102
NMR studies of post-translationally modified proteins are complicated by the lack of an efficient method to produce isotope
enriched recombinant proteins in cultured mammalian cells. We show that reducing the glucose concentration and substituting
glutamate for glutamine in serum-free medium increased cell viability while simultaneously increasing recombinant protein
yield and the enrichment of non-essential amino acids compared to culture in unmodified, serum-free medium. Adding dichloroacetate,
a pyruvate dehydrogenase kinase inhibitor, further improves cell viability, recombinant protein yield, and isotope enrichment.
We demonstrate the method by producing partially enriched recombinant Thy1 glycoprotein from Lec1 Chinese hamster ovary (CHO)
cells using U-13C-glucose and 15N-glutamate as labeled precursors. This study suggests that uniformly 15N,13C-labeled recombinant proteins may be produced in cultured mammalian cells starting from a mixture of labeled essential amino
acids, glucose, and glutamate. 相似文献
998.
An evaluation of the concept of living at moderate altitude and training at sea level 总被引:7,自引:0,他引:7
Hahn AG Gore CJ Martin DT Ashenden MJ Roberts AD Logan PA 《Comparative biochemistry and physiology. Part A, Molecular & integrative physiology》2001,128(4):777-789
Despite equivocal findings about the benefit of altitude training, current theory dictates that the best approach is to spend several weeks living at > or =2500 m but training near sea level. This paper summarizes six studies in which we used simulated altitude (normobaric hypoxia) to examine: (i) the assumption that moderate hypoxia compromises training intensity (two studies); and (ii) the nature of physiological adaptations to sleeping in moderate hypoxia (four studies). When submaximal exercise was >55% of sea level maximum oxygen uptake (VO2max), 1800 m simulated altitude significantly increased heart rate, blood lactate and perceived exertion of skiers. In addition, cyclists self-selected lower workloads during high-intensity exercise in hypoxia (2100 m) than in normoxia. Consequently, our findings partially confirm the rationale for 'living high, training low'. In the remaining four studies, serum erythropoietin increased 80% in the early stages of hypoxic exposure, but the reticulocyte response did not significantly exceed that of control subjects. There was no significant increase in haemoglobin mass (Hb(mass)) and VO2max tended to decrease. Performance in exercise tasks lasting approximately 4 min showed a non-significant trend toward improvement (1.0+/-0.4% vs. 0.1+/-0.4% for a control group; P=0.13 for group x time interaction). We conclude that sleeping in moderate hypoxia (2650-3000 m) for up to 23 days may offer practical benefit to elite athletes, but that any effect is not likely due to increased Hb(mass) or VO2max. 相似文献
999.
Abstract. Effects of future fire regimes on boreal tree species and plant functional types were studied in W Canada using a simulation approach. Present (1975–1990) and future (2080–2100) fire regimes were simulated using data from the Canadian Global Coupled Model (CGCM1). The long‐term effects of these fire regimes were simulated using a stand level, boreal fire effects model (BORFIRE) developed for this study. Changes in forest composition and biomass storage due to future altered fire regimes were determined by comparing the effects of present and future fire regimes on forest stands over a 400‐yr period. Differences in the two scenarios after 400 yr indicate shifting trends in forest composition and biomass that can be expected as a result of future changes in the fire regime. The ecological impacts of altered fire regimes are discussed in terms of general plant functional types. The Canadian Global Coupled Model showed more severe burning conditions under future fire regimes including fires with greater intensity, greater depth of burn and greater total fuel consumption. Shorter fire cycles estimated for the future generally favoured species which resprout (fire endurers) or store seed (fire evaders). Species with no direct fire survival traits (fire avoiders) declined under shorter fire cycles. The moderately thick barked trait of fire resisters provided little additional advantage in crown fire dominated boreal forests. Many species represent PFTs with multiple fire survival traits. The fire evader and avoider PFT was adaptable to the widest range of fire cycles. There was a general increase in biomass storage under the simulated future fire regimes caused by a shift in species composition towards fast‐growing re‐sprouting species. Long‐term biomass storage was lower in fire exclusion simulations because some stands were unable to reproduce in the absence of fire. 相似文献
1000.
Logan DC 《Journal of experimental botany》2007,58(1):1225-1243
Mitochondria are vital organelles that perform a variety of fundamental functions ranging from the synthesis of ATP through to being intimately involved in programmed cell death. Comprised of at least six compartments: outer membrane, inner boundary membrane, intermembrane space, cristal membranes, intracristal space, and matrix, mitochondria have a complex, dynamic internal structure. This internal dynamism is reflected in the pleomorphy and motility of mitochondria. Mitochondria contain their own DNA (mtDNA), encoding a small number of vital genes, but this role as a genetic vault is not compatible with the role of mitochondria in bioenergetics since electron transport results in the generation of reactive oxygen species (ROS) that induce lesions in the mtDNA. It is hypothesized that ROS shape the morphological organization of the higher plant cell mitochondrial population into a discontinuous whole, and that ROS are a selective pressure affecting the organization of the mitochondrial genome. This review describes how inter- and intra-mitochondrial compartmentalization underpins the biology of this complex organelle. 相似文献